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    Thread: Dinitrophenol (DNP)

    1. #1
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      Dinitrophenol (DNP)

      Here is some info to read if you are even remotely considering running DNP or just want some info.



      This is an educational article covering different aspects of DNP and is intended only to educate the reader about DNP. This article is far from comprehensive, but it should provide a good background to get the reader started on learning about DNP.

      In this article I will attempt to cover the following topics regarding DNP:

      History
      Mechanism of Action
      Dose and Cycle Recommendations
      Dietary Recommendations
      Side effects/ risks
      Prevention/ Contraindications
      Recommended supplements with DNP

      HISTORY:

      DNP stands for 2,4-dinitrophenol. This is a chemical that was once used in the early 20th century to ignite dynamite and cast a yellow dye on wood and other handcrafts. A few years later demographical statistics showed that employees who worked with DNP everyday tended to lose weight, often rapidly. One fall out from this was a study conducted by Stanford University in 1920 showing that the ingestion of DNP does in fact cause weight loss. This prompted physicians to prescribe DNP to obese patients of that era. DNP was on the market for 2 decades as a weight loss drug and was eventually taken off the market and banned for human consumption by the FDA because there was a report of cataract formation among female users of this drug which turned out to be false. This chemical is still deemed too dangerous by the FDA to allow it to come back to the pharmaceutical marketplace. Over the decades of research on DNP, scientists have never shown it to have the ability to cause cancer or any other mutations despite the fact that it�s a phenol and that most phenolic compounds are carcinogenic. DNP is now only used as a research chemical and as a pesticide in a few states that still approve of its use. It is not illegal to own DNP, but it is illegal to market it for personal consumption.

      MECHANISM OF ACTION:

      DNP exerts its effects within the cell, more specifically within the membrane of the mitochondria. The advantage of intracellular mechanisms of action such as this is that a tolerance to DNP cannot develop. To make a long story short, DNP makes the process of ATP formation very inefficient. Why is this important? Because ATP is the energy unit needed to drive all our biochemical reactions in our body that is necessary to keep us alive. The cells in our body constantly need energy (ATP) to stay alive. The amount of ATP needed to keep a person alive depends on his/her basal metabolic rate. By making ATP formation inefficient, a person�s basal metabolic rate can increase indefinitely, but for practical uses, basal metabolic rate can safely increase by 30-50% without putting one�s life in danger. It is not unheard of for people to lose up to one pound of pure fat per day while on DNP.

      If you�re not familiar with ATP, it�s what the Calories that are stored in carbs, fats, and proteins are eventually turned into. In other words, the energy that is stored in the macromolecules are transferred to the ATP molecule, but DNP disrupts this process. Instead of making ATP from macromolecules in the presence of DNP, the potential energy is just turned into heat. This is very significant because ATP levels in the body will quickly diminish and cells want to replenish that storage by breaking down more fats, carbs, etc. As you can see, a patter quickly develops where ATP levels will constantly be below normal and the body will always be trying to burn more fats, carbs, and proteins to help replenish the ATP levels. This is no different than doing aerobic exercises such as jogging, biking, etc, except while on DNP, the body is doing the aerobic exercise non stop 24 hours a day.


      DOSES AND CYCLE RECOMMENDATIONS:

      DNP is not a drug for everyone, definitely not the beginner who just wants to lose a couple of pounds to look better with the shirt off� Without proper education on its use, DNP can be deadly.

      There are 2 forms of DNP currently on the market, pure crystalline (100% dry) DNP, and powdered DNP (usually 5-10% moisture). The crystalline version is stronger and more effective, but more caution needs to be used while using it. It acts much faster, and the side effects also subside faster as well.


      I recommend between 2-6mg/kg-bw per day for crystalline DNP and 4-10mg/kg-bw for powdered DNP. A beginner should always start off at the low end to assess tolerance. Trying this for the first time 2 weeks before a competition can be disastrous. A 220lb man is 100kg exactly. This means that if he is a first time user of crystalline DNP then he should take 200mg per day. I suggest staying with this dose for at least 3 days to keep it safe, then slowly increase the dosage. 400mg/day can be used, but never take it all at once. Always split up the doses as far as possible, so for 400mg/day that would mean taking 1 200mg capsule every 12 hours. Only on rare occasions should someone attempt 600mg/day with the crystalline capsules unless it�s used by a very experienced user and all the vital signs are closely monitored.

      Cycle length depends largely on the individual. At first it was thought that a DNP cycle should be limited to 10 days at the most because the thyroids shuts down and t4 to t3 conversion in the liver becomes nil, however, this is not the case. 10 days is a very arbitrary number. A person taking 200mg/day would have almost completely normal thyroid function at day 10 whereas if s/he took 600mg/day, t3 would be non existent after 3 days. While the t3 hormone plays a very large role in determining fat loss, it should not be a big concern while on DNP because the fat burning capabilities of DNP will more than compensate for the suppressed t3 levels. An advantage to suppressed t3 levels is that the body will burn much less muscle while still burning fat on DNP. Normal t3 and thyroid function is restored within a week of stopping DNP.

      Ok, so how long should you do it? I suggest playing around with it and just go by how your body feels. It is not a bad idea to just take 2-3mg/kg-bw for 3-4 weeks. This causes less side effects and will have the same overall effect, but it will just take a bit longer. After you get used to 2-3mg/kg-bw, then another option is to up the dose by 1 cap and carrying that out for as long as your body can handle it because fatigue and a host of other side effects will eventually overtake you. If 2 caps/day is still too mild then repeat the above step with 3 caps per day spread out into 8-hour intervals.

      Because of some water retention caused by DNP, users typically find that they look their best 4-7 days after finishing their cycle when the water has normalized.

      For competitors:

      Take the last DNP capsule 8 days prior to the competition date. Carb deplete after 3 days after the last cap. Carb load immediately 2 days prior to competition and stop fluid intake. This should allow for excellent glycogen super compensation within the muscles for a fuller look.


      DIETARY RECOMMENDATIONS:

      1. Carb deplete for 3 days prior to DNP because DNP will take a good 2-3 days to deplete the body's glycogen stores before it can efficiently burn stored fat.

      2. Once on DNP eat an isocaloric diet (33% prot, 33% fat, 33% carbs) and keep the calories at around maintenance level. Restricting carbs will put the body in a state of hypoglycemia and can be dangerous to the health and also the mental well being. DNP also mimics insulin in that it shuttles glucose into the cells in the absence of glucose. This is great for fat burning, but when carb intake is too low the blood glucose can be at dangerously low levels as well. a more experienced user can switch up this ratio a bit. Either way it won't make a huge difference because it's mostly about the total calorie consumption.

      This is what I�m proposing to be the optimal DNP diet (for a high dose short cycle(s) and the end of a low dose extended cycle only):

      50% carbs, 35% protein, 15% fat. It�s not a misprint; carbs are essential for DNP to work properly. Keep in mind that it�s only the percentage that changes and not the total calories. From this point it will get a bit complicated, but read over it a few times and you will get the gist of it. I�ll also try to keep it as simple as possible.

      When fatty acids are broken down they need to be fed into an energy cycle for a complete break down so that more can be broken down later. The beginning of this cycle is called the citric acid cycle. Fats enter the citric acid cycle as a 2-carbon molecule called acetate and to start off this cycle it needs to bind to another 2-carbon molecule called oxaloacetate. Without enough oxaloacetate this cycle cannot proceed. With little oxaloacetate this cycle is slowed down, thus fat burning is slowed down. Where does oxaloacetate come from? Several sources, but the main one is from pyruvate, the end product of the first step of glucose (carbohydrate) metabolism. Without enough glucose in the blood, fat burning becomes very inefficient.

      This is not to say the more carbs we eat the more pyruvate we can generate, therefore the more fat is burned. We only need adequate levels of pyruvate to supply the citric acid cycle of the necessary starting material for fat to enter, and then it will eventually proceed to be completely oxidized in the electron transport chain.

      Don�t worry about eating too many carbs while on DNP because these carbs cannot be stored and are immediately used for fuel to try to replenish cellular ATP. While keeping the calorie level at maintenance level, it would be most beneficial to eat about 55% calories from carbs, 35% protein and 10% fat (mostly unsaturated). It may be optimal for fat burning to raise the carbs a bit more, but the protein should be high enough so that muscle catabolism is kept at a minimum when DNP creates the huge calorie deficit in the body.


      SIDE EFFECTS:

      Heat- you will feel very hot while taking this. It is very similar to jogging a slow pace all day long, so be prepared to sweat a little. In some people a lot of sweat is not too uncommon. Body temperature will rise to about 101 degrees and sustain there. This is not too out of the ordinary. This increase in core body temperature causes a vasodilation effect throughout the body to help cool you off. However, evaporative cooling with the aid of vasodilation will not be effective when the surrounding environment does not allow for proper cooling. For example, being out in the summer sun when it�s 90 degrees and high humidity can cause you to rapidly overheat to dangerous levels. Avoid hot environments at all costs. Stay indoors if you choose to use it in the summer and only go outside briefly when it�s absolutely necessary. Dehydration can cause the body to not regulate temperature properly and rapidly overheat as well. Drink 1-3 gallons of water daily depending on DNP dose.

      Water retention- this is very closely associated with heat. When the vasodilation occurs due to the rise in body temperature, blood vessels expand, causing an increase in blood volume and subsequent water retention. Also, an increased blood volume leads to decreased pressure, which would lead the body to try to store more sodium and cause even more water retention. All the water retention will subside within a week after stopping the DNP dosage, but often sooner than that. Popular diuretics are not very effective against DNP induced water retention because these diuretics mainly focus on one aspect of diuresis and that is suppression of the anti diuretic hormone (ADH), but the cause of water retention from DNP is independent of ADH. While diuretics will get rid of some naturally stored water, it isn�t getting rid of enough water that would make a competitor presentable on stage and would put the user in jeopardy of death or serious health complications due to potassium depletion.

      Lethargy- This is the biggest problem associated with DNP and is somewhat associated with the insomnia that I will cover later. As you have learned DNP depletes the body of ATP and without ATP you have no energy. It literally feels like you�re jogging a marathon all day long without a break. Of course the extent of the lethargy will depend on the dose, but it is not uncommon for people to be almost bed ridden. Walking to the kitchen to get food will be a chore. Even eating the food can become very laborious. This will subside within 24-36 hours of stopping the doses.

      Insomnia- sleeping will be very difficult for some people, not because of the familiar central nervous stimulation experienced with ephedrine and caffeine supplementation, but because it gets so damned hot. Many people including myself find it very difficult to sleep when we�re sweating in our beds. The best way to combat this is to sleep with 2 fans from both sides of the bed and the air conditioner cranked up. Obviously if you have a significant other that you sleep with then it would be wise to sleep in separate beds for parts of the cycle.

      Shortness of breath/ rapid breathing- this is common when the dose is at the upper limits. The breathing will seem like you�re jogging even while you�re sitting down and doing nothing. It will seem like you can never catch your breath. Doing anything active will make you even more out of breath and this can become dangerous. When breathing becomes irregular, you should avoid doing any aerobic or strenuous activities. This means no working out (not like you�ll have any energy to do so anyway).

      Dehydration- a very serious side effect. If hydration levels are not adequate it can predispose the body to severe overheating and possibly death. Water needs to be replenished on the order of 1-3 gallons per day.

      Electrolyte depletion- this is caused by excessive water and salt loss through sweating. Drinking water will replace fluids, but not electrolytes. Best way to replenish salts is to drink v8 juice. This can lead to a host of other problems if not remedied including excessive lethargy, low blood pressure, poor cardiac function, nausea, diarrhea�

      Nausea- This is a common side effect that afflicts roughly around 30% of the users. There could be several causes to this: dehydration, electrolyte imbalance, low blood pH, and other unknown (by me) mechanisms.

      Diarrhea- possibly due to electrolyte imbalance and undissolved DNP that passes onto the large intestine causing osmotic imbalances. If this becomes too problematic the only thing to do is just to decrease the dosage or stop completely.

      Headache- largely due to dehydration. In most people, forcing down a liter of fluids will alleviate the headaches.

      Dry/ sore throat- I don�t know the cause of this one, but it is pretty common among users and seems to manifest itself the most during sleep and may contribute to the insomnia.

      Allergies/ dermatitis- this is relatively rare. I�ve been in contact with nearly 500 people who have used DNP and I would estimate about 30-40 of them have experienced allergic reactions to DNP. The allergies manifest themselves first as phantom itches (itching without any rashes or redness) around the torso in some people. It will later develop into rashes and or hives around the body and possibly spread to the face, neck, lips, and scalp area in severe cases. Any over the counter or prescription allergy medication (anti histamine) will cure the allergies. Also if you�re allergic to DNP it doesn�t mean you can�t use it in the future. Allergies to DNP seem to have a tolerance factor. It first gets worse, then better with successive cycles. So if you are allergic, stop immediately and start again 7-10 days later and repeat until you are no longer allergic to DNP anymore. Allergies are also dose and length dependent.

      Yellow vision- This is even more rare than allergies. I�ve only known about 15 people who have experienced this out of all the people I have come in contact with who have used DNP in the past. It seems to be most apparent when you look at a white surface and yellow spots will appear on the white that you see. I�m not sure what exactly causes this, but it doesn�t seem to harm anything and goes away within 1-2 days of stopping the doses.

      PREVENTION/ CONTRAINDICATIONS:

      1. Never start your first cycle with an optimal dose. Always play it safe and start low.

      2. Never use DNP if you�re going to be in a hot environment for an extended period of time.

      3. Never take any diuretics while on DNP. This includes excessive alcohol. While mild diuretics like alcohol will make you much more uncomfortable and hotter, a harsh diuretic like lasix will kill you when taken with DNP.

      4. If oral temperature rises to 103 then discontinue use until temp is completely down to normal.

      5. Do not attempt to work out very intensely. When it�s hard to find the energy to go to work, don�t push yourself thinking you can get a good workout in. Long cardio sessions can be especially harmful for your health. It would also raise cortisol levels through the roof and will be very catabolic to muscle. Don�t sweat the cardio when on DNP because DNP will make you burn fat. Stay away from the treadmill!

      6. If allergies arise take some allergy medication and if that isn�t strong enough then stop the doses for at least 10 days before restarting.

      7. Watch your electrolytes. Carry a bottle of v8 juice with you. One 8-ounce serving of v8 has 900mg of potassium compared to 35mg of potassium in 8 ounces of Gatorade. Aim for 3000-5000mg of potassium (not all from vCool per day. Fresh meats and vegetables also have a lot of potassium in them. Sodium is very important too, but is usually not hard to get in the diet. Magnesium can be obtained from supplementation.

      8. Hydration. I can�t emphasize this enough. Not only will proper hydration levels make you feel better and prevent overheating, but it will also make the cycle more effective at burning fat.

      SUPPLEMENTATION:

      Antioxidants�one of the most effective will be the fat soluble vitamin E. I recommend 800 to 1000 iu of vitamin E per day of the cycle to combat the host of free radical damage caused by increased fat oxidation.

      Glycerol�this can be important to help maintain muscle hydration and prevent catabolism. It comes in liquid and can be bought over the counter. Take 3-4 tablespoons per day.

      Potassium citrate�if blood acidity becomes a problem then potassium citrate can help buffer the acid. About 2-3 grams will be very effective, but 1 gram will do the trick as well.

      Ephedrine--this can cause increased mobilization of fatty acid from the adipose cells to get them into the blood where they will be used for energy and burned. In short, ephedrine puts the fat in a place where DNP can burn it.

      CONCLUSION

      DNP is the most effective fat burner and perhaps the most complicated drug in the bodybuilding community and should not be taken to lightly by average dieters striving to lose a couple of pounds. The side effects are serious and numerous, but if used correctly, none of the side effects are permanent. Despite these numerous side effects people still use it because it works when nothing else will. I hope this article sufficiently educated you on DNP. If you choose to use it please do so with caution and use this and other literature as a guide to help you on your way to a new physique.
      COC RULES: https://brotherhoodofpain.com/anabolic-ster...e-conduct.html

      e-mail: [email protected]

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      DNP for Dummies
      HOW TO NOT FUCK UP DNP:
      Since some guys have been playing around and disrespecting DNP and then griping to the forums
      about the painful results, we need to make this VERY specific and VERY correct so that people
      won't keep jumping for DNP out of curiosity, or without the willpower they need to operate this
      responsibly. So here are my experienced guidelines to using it the RIGHT way.

      FIRST GUIDLINE: Dosing. Use ONLY 200mg a day for the first four days. I don't care that you
      don't "feel" anything yet and you wanna bump it up. DNP accumulates in the body, and not
      "feeling" something means NOTHING. It's there, and it's working (the effect on metabolism
      begins within two hours of the first dose!). Four days will let you test your tolerance: do you have
      an allergy? Does it give you a rash? etc.

      Only after those four days do you bump it up, by 200mg a day. The average dose is 400-600/
      day, and more than that gets a little severe. A full gram is the highest dose I've heard
      anyone use. I've used that much, and it's hell. I like to stay around 600 a day, which is HOT but
      safe and effective. Take caps even hours apart through the day, ending about 4-5 PM.
      SECOND GUIDLINE...How to eat on DNP. This is purely personal experience, because some guys like to carb-deplete *before* using DNP (then eat carbs as usual while on), and other guys like a low-carb approach throughout. Both are fine. Using DNP is the only time that fructose is a
      desireable cutting carb, because it keeps the liver replentished. That reduces lethargy and spares
      muscle.

      Be aware that eating high-carb foods WILL increase the heat sensation within an hour, and last
      about 2 hours. That means don't eat carbs before bed unless you want those night sweats to be
      even WORSE. Personally, I ate whatever the hell I wanted! IHOP, chinese, fajitas...Yes, I burned hot, but I still lost 1.5 pounds every 2 days. Keep protein HIGH for muscles' sake, and try it yourself.

      Foods I suggest including:
      Blueberry yogurt. Blueberries are excellent antioxidants, and yogurt cultures help with digestive
      function, gas, and stool consistency (disgustingly soft stools are common during DNP).
      Oregano-based foods. Oregano is perhaps one of the most potent antioxidants around, and one
      spoonful counts as a vegetable serving. Pineapple - I've found that pineapple helps alleviate those "DNP Blues". The fructose helps, and pineapple enzymes aid in protein digestion.
      V8 - one 12-ounce can supplies six servings of veggies, concentrated as an excellent source of
      antioxidants, lycopene, and recovery of electrolytes.
      Oatmeal - high-fiber foods are necessary. You'll find out why around, oh, day 5 or so. Trust me.

      THIRD GUIDELINE...Supplements and DNP. I suggest:
      ECA - DNP is not a stimulant. To keep energy high and aid in fat loss, use an ECA. Some advisors suggest that regular ephedrine is preferable to norephedrine because of the more direct "hit" of energy.
      Prohormones - perfectly fine on DNP. I used 1-AD just to help keep strength and muscle up, and
      it worked fine. No problems here. You won't GROW muscle on DNP, but it'll help with strength
      and protection.
      Obvious stuff - multivitamin, ZMA, etc.
      Biotest PowerDrive - No, I'm not pimping Biotest. But PowerDrive is an excellent pre-workout
      mixture that actually works. Plus it's low-carb (only 15 calories total), so it won't cause carb-heat
      in the middle of your workout.

      Antioxidants - I'm giving my own personal list, and why I use them:
      Alpha Lipoic Acid - aids in fat management and blood sugar, and an excellent antioxidant.
      Grape seed extract
      Syntrax Radox
      Green Tea
      Inositol - mood enhancement, antioxidant, and muscle support. 1 gram/3x day
      Ellagic acid - protects cell DNA/RNA from damage by free radicals, and may even attack cancerous cells. 400mg/twice a day
      Fruit antioxidants - ****************'s powder of high-potency natural fruit anti's. 1 gram, 2-3x
      day.
      Trimethylglyceine - antioxidant, helps move fat and blood lipids into the liver and out of the body. 500mg, 2-4x day.
      Vitamins E and C

      Supplements NOT to use:
      Any medications that suppress energy. No allergy meds, antidepressants, muscle relaxers, or
      beta blockers. DNP will have you low as it is; don't worsen your body's energy by taking
      something that suppresses you further.
      DRUGS - Sheesh, you'd think I wouldn't have to mention this, but two idiots in particular (on Elite Fitness) recently affirmed that some people still just don't get it. NO alcohol (not even
      "moderate"), NO ecstasy, NO GHB, etc. If you don't have the willpower to forego these habits,
      DNP is not for you.
      Syntrax Swole - a personal discovery. I tried Swole while on DNP...once. Two hours of hell,
      feeling inside-out.

      FOURTH GUIDELINE...working out on DNP. Keep lifting short, 30-40 minutes. DNP works very well, causing your body to use 150% of the calories per action you'd normally use. That means DON'T try to repeat your usual workouts. Drop to moderate weights, 8-12 reps, not to failure, and with plenty of walking rest between sets. You are NOT going to grow muscle on DNP, so don't use your usual heavy routine. Since DNP can cause light-headedness and heat dizzyness, you have my permission to skip squats in favor of leg presses this time.

      Cardio is a controversial one. My advice - do NOT do cardio on high doses of DNP (600mg or
      more). It's dangerous and counterproductive. Below that amount, some cardio is fine, but keep it
      to 20 minutes and not at full-gallop. Remember, DNP will drain water from your quickly, causing you to leech out minerals, vitamins, and salts. Don't overdo it.

      During exercise, consume at least 1 liter of water per 30 minutes of work, whether you're thirsty
      or not. DNP is evil in the way it blunts thirst, while at the same time doing the cruel trick of
      bloating your body with water WHILE dehydrating you from water in your organs. MAKE yourself drink. Always folllow DNP exercise with antioxidants, carbs, and this is a good time to use your multivitamin.

      Don't feel embarrassed about poor workouts. Just this morning I did a workout with a whopping
      nine sets (wimp!) before calling it quits. Listen to your body, and let it tell you when enough's
      enough; don't gauge workouts by what you *usually* can do otherwise.

      Purely for information's sake. Posting any of this information is not an admission that I have ever used DNP; I refer to myself in the first person as a hypothetical narrator in an academic discourse...

      DNP is Ames negative, and does not promote tumors. See for yourself at http://toxnet.nlm.nih.gov/

      http://www.epa.gov/ttn/atw/hlthef/dinitrop.html reports on health risks. While there have not been human studies, animal studies found no cancers caused by DNP administration. It is considered a toxin because it causes nausea, sweating, and weight loss.

      http://www.cyberiron.com/drugs/dinitrophenol.html reports on health risks from external exposure. In other words, don�t get it in your eyes, or on your skin if you�re allergic. Pretty elementary stuff.

      http://www.ebec2000.com/abstracts/056.htm This animal study documents a 64% increase in metabolism. "These findings confirm that DNP effectively increases metabolic rate..." Duh.

      http://www.zymed.com/pdf/04-xxxx/04-8300.pdf A PDF file about an antidote to DNP.

      http://www.boehringer-ingelheim.es/w...lesa/cap13.htm finds that DNP did not activate liver enzymes (MAT) associated with liver damage

      "Comparative study of toxicity of 4-nitrophenol and 2,4-dinitrophenol in newborn and young rats." Koizumi M, Yamamoto Y, Ito Y, Takano M, Enami T, Kamata E, Hasegawa R. Division of Risk Assessment, National Institute of Health Sciences, 1-18-1 Kamiyoga, Setagaya-ku, Tokyo 158-8501, Japan. This study found that DNP can induce death in overdosed amounts, but that up to that point no toxicity was evident, nor were there any abnormalities in physical development.

      "Phenol toxicity and conjugation in human colonic epithelial cells." Pedersen G, Brynskov J, Saermark T. Dept of Medical Gastroenterology, Herlev University Hospital, Copenhagen, Denmark.. This study found that DNP has a toxic effect on cells of the colon, with "toxic" defined in two ways: first, it interfered with metabolism (this we know�it�s the intended effect of DNP users!) and second, it interfered with bowel inflammation (not a health risk. This is caused by osmotic effect, with the worst result being softened stools and gas).

      "Mechanisms of bacterial resistance to macrolide antibiotics." Nakajima Y. Division of Microbiology, Hokkaido College of Pharmacy, 7-1 Katsuraoka-cho, Otaru, Hokkaido 047-0264, Japan. This study found that antibiotic-resistant bacteria could be thwarted with DNP. "the extent of the accumulated drug in a resistant cell increases as much as that in a susceptible cell in the presence of an uncoupling agent such as�2,4-dinitrophenol (DNP)."

      "Absence of Crabtree effect in human melanoma cells adapted to growth at low pH: reversal by respiratory inhibitors." Burd R, Wachsberger PR, Biaglow JE, Wahl ML, Lee I, Leeper DB. Departments of Radiation Oncology, Kimmel Cancer Center, Thomas Jefferson University, Philadelphia, Pennsylvania 19107, USA. Check this out�DNP actually helps make melanoma tumors easier to attack by increasing ratio of oxygen consumption to lactic acid production, while glycolysis remains the same. "Therefore, tumor acute acidification and oxygenation can be achieved by exposure�"


      "New insights in the cellular processing of platinum antitumor compounds, using fluorophore-labeled platinum complexes and digital fluorescence microscopy."
      Molenaar C, Teuben JM, Heetebrij RJ, Tanke HJ, Reedijk J. Department of Molecular Cell Biology, Leiden University Medical Centre, The Netherlands. DNP is used as a control in tests of antitumor cells because it does NOT bind to cell DNA, nor promote tumors, yet its staining abilities enable tracking of the uptake of antitumor drugs.

      Specific inhibition of breast cancer cells by antisense poly-DNP-oligoribonucleotides and targeted apoptosis." Ru K, Taub ML, Wang JH. Department of Biochemistry, State University of New York, Buffalo 14260-3000, USA Are you ready for this? DNP actually INHIBITS (!!!) breast cancers! Yes, not only does it NOT promote cancers, it�s being recognized as a cancer-fighter/blocker. "Two membrane-permeable and RNase-resistant antisense poly-2'-O-(2,4-dinitrophenyl)-oligoribonucleotides (poly-DNP-RNAs) have been synthesized as inhibitors of human breast cancer�fluorescence assay indicates that the targeted antisense inhibition by poly-DNP-RNAs leads to apoptosis of SK-Br-3 cells but does not affect nontumorigenic MCF-10A cells. The control poly-DNP-RNAs with random or sense nucleotide sequence are completely inactive." Plain English? DNP is being synthesized as an anti-cancer compound, because tests show that it blocks mutagens but does NOT affect non-mutagenic (healthy) cells, and has no RNA effects on them.

      "Heat shock protein induction by certain chemical stressors is correlated with their cytotoxicity, lipophilicity and protein-denaturing capacity." Neuhaus-Steinmetz U, Rensing L. Institute of Cell Biology, Biochemistry and Biotechnology, NW II University of Bremen, Germany. The thermic effect of DNP induces protein synthesis (heat shock protein, or HSP, synthesis). In fact, it�s quite GOOD at it: "ASA, DNP and CCCP induced HSP at lower concentrations than substances with a similar lipophilicity�"

      "Comparative effects of the metabolic inhibitors 2,4-dinitrophenol and iodoacetate on mouse neuroblastoma cells in vitro." Andres MI, Repetto G, Sanz P, Repetto M.
      National Institute of Toxicology, Seville, Spain. In this study, DNP�s observed effect was an increase in metabolism (duh!), while the other toxins compared to it had harmful in vitro effects but no increase in metabolism.

      "Inhibition of uncoupled respiration in tumor cells. A possible role of mitochondrial Ca2+ efflux." Gabai VL.Medical Radiology Research Center, Russian Academy of Medical Sciences, Obninsk. DNP not only does not cause tumors, but it inhibited their respiration by 20-25% compared to controls.

      "Amsacrine-induced lesions in DNA and their modulation by novobiocin and 2,4-dinitrophenol." Shibuya ML, Buddenbaum WE, Don AL, Utsumi H, Suciu D, Kosaka T, Elkind MM. Department of Radiology and Radiation Biology, Colorado State University, Fort Collins 80523. In this study, researchers found that DNP abrogates�or disrupts�cytotoxicity in hamsters (using cancerous cells). They expected to find that DNP would interfere with anticancer treatments, but instead found that DNP increased their effects. They state, though, that they cannot claim a proven effect of DNP on anticancer treatments yet, although they do agree that treatment with DNP actually enhanced the effects of the DNA regenerative therapy of anticancer chemotherapy.

      "Induction of endonucleolytic DNA cleavage in human acute myelogenous leukemia cells by etoposide, camptothecin, and other cytotoxic anticancer drugs: a cautionary note." Kaufmann SH. Oncology Center, Johns Hopkins Hospital, Baltimore, Maryland 21205. The authors warn that certain anti-leukemia drugs resulted in "extensive DNA degradation." BUT(good ol� DNP to the rescue!), "Preincubation with dinitrophenol abolished the effect�"

      "[Dependence of the nature of the action of metabolic inhibitors on ribosomal RNA synthesis in Ehrlich ascites carcinoma cells on cell integrity]" [Article in Russian] Akhlynina TV, Buzhurina IM, Panov MA, Rozovskaia IA, Chernaia NG. DNP actually inhibits the synthesis of RNA in carcinoma cells. In other words, it helps cancerous cells commit suicide. "Ribosomal RNA (rRNA) synthesis in the intact Ehrlich ascite carcinoma cells is selectively inhibited by papaverin (ED50 = 0.01 mM), 2,4-dinitrophenol (DPN; ED50 = 5 microM), and actinomycin D (ED50 = 0.1 microgram/ml)."

      "Autocatabolism of surface macromolecules shed by human melanoma cells."
      Bystryn JC, Perlstein J. Cancer Res 1982 Jun;42(6):2232-7. This study finds that DNP helps
      melanoma cells die (autocatabolize) while other cells are unaffected.

      http://www.geocities.com/byggdegstor/dnpforside - tons of research, including medical studies. Excerpts:

      DNP does not cause liver damage: "Their analyses demonstrate, beyond a doubt, that the liver does not suffer any damage in the course of dinitro treatment." (Biological Study of Dinitro Drugs in Humans By Dr. Jacques Bell. Bell, Jacques. 1939. Etude biologique des produits dinitres chez l'homme. Medecine. 19:749-54. Translation � 1996 Robert Ames)

      Also: "Experimental studies on animals do not show toxic effects of dinitrophenol on the kidney. Anatomical-pathological examinations of animals, even those which died from a massive dose of dinitrophenol, do not reveal any important anatomical changes, except a small degree of cytolysis. Clinical documents are not abundant, but, on the whole, do not seem to demonstrate that dinitrophenol is toxic for the kidneys."

      "Dinitrophenol has almost no action on the blood cholesterol. (Grant and Schube)."

      "it doesn't seem that dinitrophenol at usual clinical doses is likely to harm the kidneys."

      "Dinitrophenol is remarkable for its absence of effect on the cardio-vascular system...dinitrophenol is absolutely devoid of toxicity for the heart."

      "Dinitrophenol does not attack cell tissue albumin and does not determine the fat loss to the expense of the muscles, contrary to thyroxine."

      "dinitrophenol offers this precious advantage that the cessation of its use at the slightest appearance of signs indicating an imminence of intoxication results immediately in the arrest of those symptoms." (Professor Pouchet)."


      Interestingly, one medical theory on a health ADVANTAGE of DNP is that the slight increase in thermogenic temperature simulates the fever a body induces during a viral attack. The body increases itsheat to protect organs but kill viruses, and some theorize that DNP can do the same thing, thus killing viruses in the body. In this mechanism, DNP may have an immune-enhancing effect.
      COC RULES: https://brotherhoodofpain.com/anabolic-ster...e-conduct.html

      e-mail: [email protected]

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    5. #3
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      Many boards have DNP-guides, but in essence they are the same 3 guides over and over again; These guides are not only outdated, they tend to over do the supplements thus making it more complicated than needed and they are life-threatening to newbies because they don't elaborate enough on important aspects as the 36-hour half-life (thus the accumalative effect) and the elektrolyte-loss (they just tell you to drink V8 ).
      Not only that but instead of REALLY BASING THEIRSELVES ON SCIENTIFIC RESEARCH, they just post some PUBMED researches and long quotes out of them (not summarized or put in lay-mans terms), just to impress the reader!
      And often you have the feeling that they really don't know what they are talking about, also they tend to tell more about its history than its practical use and action (BY KNOW WE ALL KNOW IT WAS USED AS AN EXPLOSIVE, INSECTICIDE, YELLOW PAINT etc.)!
      They don't elaborate enough on Practical inconveniences as well; The foultasting and dry mouth one gets and the fact that if you are making the caps yourself without precautions it is very likely to cover the room with unremovable (except with TEK) Yellow stains everywhere.
      The final and most important thing is that this new approach is not only at least as effective at fat loss or even more so, but also countless times more convenient and with countless less horrible sides!

      A REVOLUTION IS UPON US!!

      -------------------------------------------------------------------------

      The new approach to cycling DNP:

      DNP has a 36-hour half-life meaning it will build up in your blood and due to it being an exponential 2nd degree math function, after a certain amount of time the accumalative effect will be too small (insignificant) and thus bloodlevels will peak and remain stable...

      The international Physics formula for Half-life:

      In physics
      with:
      N(0) = dosage at time zero
      N(t) = dosage left at recent time
      t(1/2) = half life in seconds/hours/days/years (depending on compound)

      N(t) = N (0) x (1/2)^(t/t(1/2))

      at 200 mg every day the peaklevel will be 540 mg...
      @ day 6 you will already be over 500 mg...!

      (but given the margin of error in capping and dosingtimes we take 600 mg as standard!)

      more info: http://forums.anabolicreview.com/sh...728&postcount=2

      So a 20 day cycle @ 200 mg ED, will result in a 540 mg peaklevel which is a very comfortable dose for any healthy grown man!

      A 20 day cycle will also yield great results, most likely greater than a "horrifying sideful" traditional 8 day cycle @ 400 mg.

      Most of you who are trying DNP for the first time are not willing to jump in a
      20 day cycle right away, so a 10 or 12 day cycle @ 200 mg will be more suitable, just make sure that you carbdeplete 2 days in advance for optimum results in such a short low dose cycle...

      DNP IS NOT SUITABLE FOR WOMEN AND MORBIDLY OBESE PEOPLE!!

      --------------------------------------------------------------------------

      Beneficial Properties:

      1. DNP is both Liver and kidneyfriendly.
      2. DNP has anti-catabolic properties.
      3. DNP boosts the immunesystem
      4. DNP is Anti-Carcinogenic
      5. DNP is non-hormonal and thus fatloss is easier to maintain

      --------------------------------------------------------------------------

      Sides:

      At such a low dose the most likely sides will be:
      Sweating (+ feeling hot)
      Heavy breathing
      Irregular Sleep Pattern
      Rashes for some (take an anti-histamine for this, if it lasts discontinue DNP!)
      Lethargy
      Decreased Strength
      Musclecramps (Not likely at all especially at such a dose with enough mineralsupplementation).
      Increased Hunger
      (especially Sugar-cravings, Sibutramine totally annihilates this side!)

      Note:
      I got "the rash" the first and last part of the second cycle...
      I never took citadrizine HCL...
      But by cycle 3 (actually end of cycle 2; so 2,5) I never developed an allergy any more...
      Still Anti-histamines can aid in fat loss if supplemented with Ephedrine and Yohimbine!

      All these can be combatted to a certain extent...

      Practical Sides:

      DNP will provide a hideous sent of it under your Armpits due to the sweating
      (especially in the last few days) so always wash under your armpits a couple of times a day and put plenty deodorant under it even before bed
      (I swear the scent will annoy you in bed).

      DNP leaves a foul and dry taste in your mouth all day long; I found out that
      drinking Diet Softdrinks helps against it so sweets always get the taste away, but seeing we want to LOSE weight Diet soda is the best option!
      (normal softdrinks contain sugar and we WANT TO LOSE WEIGHT
      best bets: Fanta, Fanta Pomelo, Fanta Cassis, Fanta Lemon, Coca Cola Lemon, Sprite etc. ALL LIGHT!).
      I finish about 2 bottles a day
      (Ice cold preferabely also seeing drinking water all day gets tiresome!!).

      --------------------------------------------------------------------------

      Effectivity:

      All over messgeboards I read that an ECA boosts metabolism by 3%,
      Clen + T3 20% and DNP 50-75%!

      I don't know where people get these numbers but it is not true!

      Fat loss not only has to do with metabolism, but also with many other processes like affecting alpha and betareceptors
      (why Yohimbine has got such fatloss potential for "love handles").
      Increased metabolism also means better proteinsynthesis, which is not always the case with these fatburners!

      Not to mention a 75%-boost on DNP would not make sense since for instance let's take a 2000 calorie boost (And that would mean a maintenance
      Caloric Requirement of about 2800 Kcal a day!!, which is very high!)
      --> giving a maximum of 250 gram pure fat loss a day!
      That would mean an 8 day cycle would yield a maximum of 2 Kg fatloss
      (I know the offdays count as well but that would be compensated by glycogen-reserves, increased appetite etc.).

      The real deal:
      A degree Fahrenheit increase in BMR on DNP is equal to a
      120% boosted Caloric-expense!

      Practical Effectivity:
      Now here's the big question......
      will it yield the same results fat loss-wise as the shorter higher dose cycles?

      Yes, not only shall the DNP be more effective, but things like T2 and Yohimbine need longer cycles to work their magic and thus you will have even better results!
      (also the fat loss will be more gradually from the ancillaries and thus prove easier to maintain that weight).

      Note: The Scale will lie and so will the mirror!
      Due to the waterbloat and thus waterweight
      (The waterbloat is less obvious then with Deca for instance since it "hides" around the middlesection + lovehandles!), also the carbdepletion will make your muscles appear less "pumped".

      So remember that while "on" you will feel fat and bloated and your muscles will be anything but pumped!
      Fun thing is 5-7 days after discontinuance you will see the drastic change in the mirror and on the scale!

      The feeling one gets when coming off is great
      (no more sweating, dry mouth, clearance of bloat etc.)!

      --------------------------------------------------------------------------

      Weightloss is semi-permanent!:

      I and many other people have noticed that after a DNP-cycle even after months less than 50% of the weightloss is gained back.
      (And that is even with crappy training and diet)
      While common rule in dieting is that the more weight one loses in a
      short time span, the more likely he/she is to gain all that weight back plus even a bit more fat most of the times (the dreaded YOYO-effect!!).

      Also this research confirms that 3 obese people (2 men and a women) after
      long term T3 and DNP supplementation lost a lot of weight and managed
      TO KEEP IT OFF!

      http://forums.anabolicreview.com/sh...730&postcount=4

      As to so many cases of people not experiencing a drastic rebound with DNP
      (anything that guarantees under 50% of the weightloss gained back is an effective diet-aid in my opinion) it got me thinking as to WHY...

      So a simple theory which I came up with:

      DNP is so dangerous, because it doesn't involve in a feedback system
      (meaning if there is to much present in the blood there is no way the body can combat that).
      Also it is non-hormonal
      (hormonal systems always have a feedback-mechanism).

      This means that it doesn't affect your body's "setpoint"
      (which is what your body thinks is your "healthy" weight and thus always wants to return to that point).

      Some mechanisms in the "setpoint" are still unknown but it mostly has to do with dopamine/adrenaline and the various Neuropeptides
      (especially B, K and Y that all regulate appetite).

      The "setpoint" is best adjusted if weightloss is as gradually as possible
      (phentermine users always get the yo-yo effect meaning all the lost weight
      + some new fat comes back after discontinuance; not only because fat is lost so rapidly but mainly because it affects all those "setpoint" features and after discontinuance they will try to regain homeostasis!).

      DNP has no (significant) role in manipulating the "setpoint"
      (meaning your body will not feel the urge to gain some weight after discontinuance).
      Also it competes with T3, meaning after you stop DNP, T3 will peak
      (instead of like with most diets; will be on low)
      couple that with the fact that it is not catabolic
      (actually a bit anti-catabolic for that matter) so your BMR stays
      rougly the same after the DNP-cycle.

      And the conclusion confirms the reality -->
      Fat loss induced by DNP is not likely to come back for a significant part!

      Note:
      Most people supplement certain compounds with DNP -->
      I for instance take Sibutramine, T2, T3 and an ECY which are
      most likely to be the MAIN cause of the "gained weight afterwards"
      due to the KNOWN disturbance of some processes in the body's metabolism by these ancillaries.

      --------------------------------------------------------------------------

      First things, First! --> Obtaining DNP

      1) Make it yourself!

      Unless you are an experienced homebrewer I can not advise to do this,
      DNP stains are impossible to remove (with the exception of with TEKTROL), and the DNP powder is at its cheapest $1 (for small amounts) per gram, considering the fact that you pay $1 for a 200 mg cap on average and you only need a small amount of caps per cycle; it is not worth it...

      The pro with making it yourself is that you can add all sorts of things in thus minimizing the amount of tabs/caps/powder one has to swallow.

      I used to make them containing per cap:
      200 mg DNP
      100 mg Quercetin (anti-histamine and anti-oxidant)
      10 mg Sibutramine HCL (Appetite suppresant)
      150 mg Magnesium Malate
      180 mg Synthetic Vitamin E (Comes down to 400 IE/IU)
      5 mg Vitamin B12
      5 mg Yohimbine HCL

      2) Buying them:

      As to such a potentially dangerous substance, if over dosed,
      I wouldn't buy it unless it was from someone who is really well known.
      There is such a guy and he makes the 200 mg DNP caps with 200 mg Quercetin (Anti-histamine and Anti-oxidant) in them for just $1.
      If you are a regular on this board and are well respected here, you can ask a mod/vet for his e-mail; Normally i wouldn't post this but it is due to the fact that in case of DNP you have to have a real trusted dealer!

      --------------------------------------------------------------------------

      Usage --> Diet:

      Lots of Water! and other fluids like DietSodas!

      A diet while on DNP is nonsense since due to its non-hormonal actions there is no benefit in shifting nutrients.

      You will get bad sugar-cravings though!
      (Yohimbine, Ephedrine and especially Sibutramine are effective in combatting this!).

      Just remember that carbs will get you heated
      (so after carb intake you will start to feel warm for about 10 minutes, but without carbs you will find everything to taste disgusting!).

      The 2 gram per lbs of bodyweight protein rule is also nonsense!
      (DNP is not catabolic at all).

      Keep your intake of vegetables high
      (especially any kind of Lettuce, cubecomber etc.)
      Also Fruits (with the exception of Bananas/strawberries/grapes)
      do combat a lot of sides
      (refrigerate some Apples, Oranges, Mangos, Peaches and a Pineapple and you will have a tasty meal that also makes you feel more at ease while "on").

      --------------------------------------------------------------------------

      Supplementing T2 and T3 or not?:

      This has been a controversial subject...

      Let's clear some things up (MALLET will thank me for it!):
      T3 is NOT catabolic!
      In certain amounts it is very ANABOLIC....

      T2 + T3 help DNP operate at peak efficiency; Maximizing Fat Loss!

      Especially since the thyroid can shut down, the amounts we supplement are quite anabolic/anti-catabolic (Why I GAINED 4 lbs LBM)!

      For the people afraid of suppressing their thyroid:
      Fact is T3 and DNP compete a little, so supplementing T3 on a DNP-cycle would be far less suppresive on TSH than on a T3/Clen or T3-only cycle.
      Not to mention the fact that getting off DNP would give your Thryroid a boost too so recovering would be easier than from the proposed T3-only cycle...

      T2 info (there is little info available on such a wonderful substance!):

      (((((I read most Pubmed researces on Thyroid-metabolites and found this to be the found most important things to know)))))

      - Potencywise: 400 mcg T2 = 50 mcg T3
      - T2 is far less catabolic than T3 even when abused:
      - T2 is far less supressive on FSH than T3
      - 3,5-T2 is more suitable for fat loss than 3,3-T2.
      - T2 is only active for about an hour.
      - T2 is most effective when supplemented with T3
      (or when natural production of T3 is high).
      - Although T3 has a long half-life, periodic intervals per day of taking it yields far better results!

      T2 is best taken as much divided during the day as possible; 3 is a minimum
      (it is only active for one hour and preferabely with meals since it will burn all the fats/carbos you get in immediately!).

      T2 unlike T3 is not likely to be catabolic even when abused
      (as previously mentioned T3 engaged in proper usage is quite anabolic!).

      T2 is available @ Team LR

      P.S. Team LR probably uses ethanol (Nail polish remover) as a dissolver so the stuff tastes like crap, right before taking it, put it in an Empty cap
      (the cap will dissolve within 2 minutes of coming in contact with a liquid so take it just before!).

      --------------------------------------------------------------------------

      Proper supplementation:

      People tend to use TOO MUCH supplements on DNP.
      Therefore making it way too complicated and frightening

      In low dose cycles the described supplements (below) are more than enough!

      In dosages like 600/800/1000 mg ED
      Magnesium/Phytochemicals/GSE become essential!

      2-10 gram Potassium Gluconoate ED
      ECY (E/C/Y/G/A @ 25/200/5/40/75 mg)
      2x Vitamin C @ 500 mg
      2x Vitamin E @ 400 IU
      3x 400 mcg T2
      3x 15 mcg T3

      Optional:
      Ketotifen or Benadryl (preferabely on hand!)
      Melatonin (preferabely on hand!)
      R-ALA
      Magnesium (very useful in higher dosages like 400 mg DNP or more!)
      Taurine @ 500 mg ED

      ECY (E/C/Y/G/A @ 25/200/5/40/75 mg):
      Ephedrine/Cafeine/Yohimbine/Guggelsterones/Acetyl-L-carnitine
      @ 25/200/5/40/75 mg!
      (should contain SYNTHETIC guggelsterones and SYNTHETIC yohimbine both available at 1fast400).

      Usage: To combat Lethargy, Curb Appetite and Cravings, to free fatty acid for better fatburning and for better fatburning in "stubborn fat".

      T2 + T3:
      Fatloss, preventing lethargy and maybe even anabolism/anti-catabolism

      Vitamin C & Vitamin E:
      Basically all the Anti-oxidants you need: A Watersoluble and a Fatsoluble one!
      due to their activity-span take twice a day!

      Potassium Gluconoate:
      You loose alot of minerals through sweating!
      The elektrolytes you have to replace are Sodium and Potassium
      (in Latin Natrium and Kalium),
      sodium is relatively easy to get through ones diet
      (tablesalt is sodiumchloride/natriumchloride).
      Potassium is a little harder to get
      (Still Potassium is present in a lot of vegetables).

      10 grams a day of Potassium Gluconoate is best
      (actually 10 grams is way overkill especially since that would mean
      1,6 gram of Potassiumsupplementation a day for a 200 mg cycle).
      2 grams is more than enough...

      Potassium Gluconoate will keep strength up and battle muscle cramps!

      Potassium gluconoate (16% Potassium) is $20 per 3 lbs at 1fast400!

      Ketotifen or Benadryl (Ketotifen is much more potent):
      As Anti-histamine (for Allergies)
      As sleeping Aid (take before bed!)
      Upgrading the Fatcell receptors
      Keeping the ECY effective (during longer runs like 30 days)

      Melatonin:
      Anti-oxdidant + Sleeping Aid.

      Taurine
      Compensate Taurine Levels in Liver...

      Magnesium or R-ala
      As Anti-Oxidant!

      Obtaining supplements:
      1fast400 for all the bulkpowders for the ECY (and all the other supplements)
      animalkits for Vitamin E powder

      --------------------------------------------------------------------------

      DNP for PCT: Will elaborate on that later!

      --------------------------------------------------------------------------

      Funny Note:
      Hitler gave it to his troops invading russia to keep them warm during Russia's infamous winters!

      --------------------------------------------------------------------------

      Phytochemicals Story!

      Morin, Luteolin, Quercetin, Kaempferol and Reservatol are especially good at supressing Sugars from being metabolized
      (not to mention their life-extentioning abilities and positive effects on Lipid Levels and Cardiac Function).
      Fisetin, Myrecetin, Baicalein, Galangin are far less effective
      (In That order --> with the most effective one mentioned first and the least effective one mentioned last).

      Epigallocachin, Epicatechin, Hesperetin, Taxifolin, Rutin, Flavonol, Flavone didn't do anything at all....

      About Phytochemicals:
      Li BH, Tian WX. Inhibitory effects of flavonoids on animal fatty acid synthase. J Biochem. 2004 Jan;135(1):85-91

      Grapeseedextract inhibits fatcells from growing instead of inhibiting sugars being metabolized like the other phytochemicals!

      About GrapeSeedExtract:
      Moreno DA, Ilic N, Poulev A, Brasaemle DL, Fried SK, Raskin I. Inhibitory effects of grape seed extract on lipases. Nutrition. 2003 Oct;19(10):876-9.

      Reservatol:
      Which frees a lot of fatty acids from stubborn fat, makes fatcells more sensitive for Adrenaline, imitates caloric restriction and actually kills fatcells to a degree!
      Not to mention its sex-boosting properties, its lifespan enhancing ability and the fact that it pumps your muscles full of Anti-oxidants especially in a
      PWO-shake to make recovery easy and thus produce an anabolic enviroment!

      About Reservatol!:
      Picard F, Kurtev M, Chung N, Topark-Ngarm A, Senawong T, Machado De Oliveira R, Leid M, McBurney MW, Guarente L. Sirt1 promotes fat mobilization in white adipocytes by repressing PPAR-gamma. Nature. 2004 Jun 17;429(6993):771-6

      Konrad Howitz, Kevin Bitterman, Haim Cohen, Dudley Lamming, Siva Lavu, Jason Wood, Robert Zipkin, Phuong Chung, Anne Kisielewski, Li-Li Zhang, Brandy Scherer, David Sinclair. Small molecule activators of sirtuins extend Saccharomyces cerevisiae lifespan. Nature 24 August 2003.

      Molecules Discovered That Extend Life In Yeast, Human Cells; Group Of Compounds Found In Red Wine, Vegetables Simulate Benefit Of Low-calorie Diet. Science Daily, 25-8-2003

      That's why I wondered a cap containing
      a Fatinhibitor like Orlistat (or maybe an even more effective one in the future)
      and a Glucose-inhibitor like the mentioned Flavonides and GrapeSeedExtract should make the eating of Fast Food/Junk Food perfectly acceptable!
      COC RULES: https://brotherhoodofpain.com/anabolic-ster...e-conduct.html

      e-mail: [email protected]

      >>>WE WILL NEVER EMAIL ABOUT SPONSORSHIP INFORMATION!<<<

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    8. #4
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      United States Patent 4,673,691
      Bachynsky June 16, 1987
      Human weight loss inducing method


      Abstract

      A human weight reduction method in which 2,4-dinitrophenol and a thyroid hormone preparation are administered to the patient. The dinitrophenol is administered in dosages sufficient to elevate the patient's body temperature, typically 250 mg every other day. The thyroid hormone preparation preferably contains 3,5,3'-triiodothyronine and is administered in dosages sufficient to substantially maintain the patient's serum T3 concentration originally present at treatment onset.
      Inventors: Bachynsky; Nicholas (1110 Pine Cir., Sea Brook, TX 77586)
      Assignee: Bachynsky; Nicholas (Sea Brook, TX)
      Appl. No.: 668501
      Filed: November 5, 1984

      Current U.S. Class: 514/567; 514/909
      Intern'l Class: A61K 031/195
      Field of Search: 514/728,909,567
      References Cited [Referenced By]
      U.S. Patent Documents
      4087554 May., 1978 Haydock et al. 514/728.


      Other References

      Chem. Abst. 66:82758c (1967)--Rossini et al.
      Chem. Abst. 71:27671x (1969)--Tomita et al.
      Chem. Abst. 77:109780v (1972)--Tiller et al.
      Chem. Abst. 82:25791q (1975)--Wahl et al.
      Chem. Abst. 88:167300b (1978)--Kaplan et al.
      Chem. Abst. 89:191455x (1978)--Organesyan et al.
      Chem. Abst. 100:168805y (1984)--Sydykov.
      Chem. Abst. 102:56608w (1985)--Langer.
      Simkins, S., "Dinitrophenol and Desiccated Thyroid in the Treatment of Obesity," JAMA 108, pp. 2110-2117 and 2193-2199 (1937).
      Tainter, M. L. et al., "Dinitrophenol in the Treatment of Obesity," JAMA 105, pp. 332-336 (1935).
      Tiller, F. W. et al., "The Effects of Noradrenaline and 2,4-Dinitrophenol on the Oxygen Consumption of Different-Aged Rats After Treatment with Triiodothyronine or Methylthiouracil," Arch. Int. Pharmacodyn. 198, pp. 377-384 (1972) (With Translation).
      Wahl, R. et al., "Influence of Various Drugs on the Adsorption of Thyroid Hormones to Liver Mitochondria," Z. Naturforsch, 29, pp. 608-617 (1974) (With Translation).
      Schimmel, M. et al., "Thyroidal and Peripheral Production of Thyroid Hormones," Annals of Internal Medicine 87, pp. 760-768 (1977).
      Arena, Jay M., Poisoning, pp. 86 and 92 (Charles C. Thomas, Springfield, Ill. (1978).
      Cazeneuve, P. et al., "Sur les effets produits par l'ingestion et l'infusion intra-veineuse de trois colorants jaunes, derives de la houille," C.R. Acad. Sci. 101, pp. 1167-1169 (1885).
      Brobeck, J. R., "Food Intake as a Mechanism of Temperature Regulation," Yale Journal of Biology and Medicine 20, pp. 545-552 (1948).
      Cutting, W. C. et al., "Actions and Uses of Dinitrophenol," JAMA 101, pp. 193-195 (1933).
      Diechmann, W. B. et al., Symptomatology and Therapy of Toxicological Emergencies, pp. 452-453 (Academic Press, New York 1964).
      Counsel on Pharmacy and Chemistry, "Dinitrophenol Not Acceptable for N.N.R.," JAMA 105, pp. 31-33 (1935).
      Horner, W. D., "Cataract Following Dinitrophenol Treatment for Obesity," Archives of Opthalmology 16, pp. 447-461 (1936).
      Negherbon, W. O., Handbook of Toxicology, vol. 3, pp. 303-308, (W. B. Saunders Co., Philadelphia 1959).
      Perkins, R. G. "A Study of the Munitions Intoxications in France," Public Health Reports 34, pp. 2335-2374 (1919).
      Sims, E. A. H. et al., "Endocrine and Metabolic Effects of Experimental Obesity in Man," Recent Progress in Hormone Research 29, pp. 457-496 (1973).
      Spector, W. S., Handbook of Toxicology, vol. 1, p. 118, (W. B. Saunders Co., Philadelphia, 1956).
      Tainter, M. L. et al., "A Case of Fatal Dinitrophenol Poisoning," JAMA 102, pp. 1147-1149 (1934).
      Physician's Desk Reference, 37th ed., pp. 1896-1897 (1983).

      Primary Examiner: Robinson; Douglas W.
      Attorney, Agent or Firm: Pravel, Gambrell, Hewitt & Kimball

      Claims


      I claim:

      1. A method of inducing weight loss in a patient, comprising the steps of:

      (a) administering 2,4-dinitrophenol or salt thereof at a rate ranging from about 60 to about 250 mg/day; and

      (cool.gif concurrently administering 3,5,3'-triiodothyronine to the patient at a rate ranging from about 25 to about 100 mcg/day.

      2. The method of claim 1, wherein said 3,5,3'-triiodothyronine is substantially free of thyroxine.

      3. The method of claim 1, wherein said 3,5,3'-triiodothyronine administration is at a rate ranging from about 50 to about 100 mcg/day.

      4. The method of claim 1, wherein said dinitrophenol is administered at said rate with dosages given only on alternate days.

      5. The method of claim 1, wherein said dinitrophenol is administered at said rate with primary dosages given on alternate days and smaller, supplemental dosages given on the days immediately subequent to said alternate days.

      6. The method of claim 1, wherein 2,4-dinitrophenol is administered.

      7. A method of inducing weight loss in a patient, comprising the steps of:

      (a) administering 2,4-dinitrophenol to the patient at a rate ranging from about 125 to about 250 mg/day; and

      (cool.gif concurrently administering 3,5,3'-triiodothyronine substantially free of thyroxine to the patient at a rate ranging from about 50 to about 100 mcg/day.

      8. The method of claim 7, wherein said dinitrophenol and said 3,5,3'-triiodothyronine are administered at initial rates of about 250 mg of said dinitrophenol every other day and about 50 mcg 3,5,3'-triiodothyronine per day, and following 2-12 weeks of said administration at said initial rates, are administered at subsequent rates of about 250 mg of said dinitrophenol every other day alternated with about 125 mg of said dinitrophenol on subsequent days and about 100 mcg 3,5,3'-triiodothyronine per day.
      Description


      This invention relates to a method of inducing weight loss in patients by the concurrent administration of 2,4-dinitrophenol and 3,5,3'-triiodothyronine.

      BACKGROUND OF THE INVENTION

      Obesity is a common problem. Simply stated, obesity is an excess accumulation of adipose tissue which contains fat stored in the form of triglycerides. The number of cells in the body is determined at least by late adolescence and while the number of adipocyte cells may increase, it does not decrease. Thus, weight gain can result from an enlargement of adipocyte cells or an increase in their number. Typically, obese individuals have hypertrophic cells and the severely obese have an increase in adipose cell number as well as hypertrophy. An obese patient only reduces the fat in his cells when he loses weight. Further, he may not ever lose the tendency to gain weight.

      Body weight is regulated by an endogenous body mechanism. Physiological and neurological properties establish and maintain a given weight. Briefly stated, glycerol which is released during hydrolysis of triglycerides and adipose tissue is widely believed to regulate caloric intake and metabolism. Others have postulated that caloric intake is affected by both body temperature and environmental temperature. In addition, cell size and number affect energy regulation. Weight gain cannot be predicted solely on the amount of calories ingested.

      In normal persons, thermogenesis is an adaptive mechanism which increases the metabolic rate after overeating. While a normal person will experience an increase in thermogenesis following increased caloric intake, the obese either has a substantially decreased thermogenic mechanism or lacks this particular mechanism entirely.

      The use of dinitrophenol to treat obesity is known. Dinitrophenol is known to elevate the body temperature and produces a marked increase in caloric metabolism. However, ingestion of massive amounts of dinitrophenol causes toxicity by the uncoupling of oxidative phosphorylation in the mitochondria of cells. Because of this toxicity, excessive amounts can result in profuse diaphoresis, fever, thirst, tachycardia and respiratory distress which can lead to hyperpyrexia, profound weight loss, respiratory failure and death. The minimum fatal human oral dose is estimated at one to three grams (approximately 20-30 mg/kg).

      In methods heretofore known to using dinitrophenol to induce weight loss, while initial daily dosages have usually been much less than the toxic amount, about 100-250 mg, as the treatment progressed the patient normally developed a tolerance for dinitrophenol and the dosage was increased to obtain the same results. This increased dosage led to an increased frequency of toxic symptoms and general disuse of dinitrophenol in inducing weight loss.

      It has also been known to use drugs with thyroid hormone activity for the treatment of obesity. However, as described in Physicians' Desk Reference, Medical Economics Co. Inc., (Oradell, N.J.), 37th Ed. (1983), in euthyroid patients, it is well established that doses within the daily hormonal requirements are ineffective for weight reduction. However, larger doses may produce serious or even life-threatening manifestations of toxicity.

      SUMMARY OF THE INVENTION

      The present invention avoids the necessity of increased dosages of dinitrophenol and the concomitant toxicity problems associated therewith as treatment progresses while obtaining improved results. It has been discovered that the use of dinitrophenol induces hypothyroidism which can be prevented by concurrently administering thyroid hormone preparation with the dinitrophenol.

      Briefly, the present invention is a method of inducing weight loss in patients, including the steps of administering dinitrophenol to the patient in an amount sufficient to clinically increase thermogenesis of the patient, and concurrently administering a thyroid hormone preparation to the patient in an amount sufficient to substantially maintain the serum concentration of 3,5,3'-triiodothyronine of the patient originally present at treatment onset.

      DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENT

      It has been discovered that the ingestion of dinitrophenol induces hypothyroidism. Athough it is not fully understood, it is believed that the normal thyroid gland produces both thyroxine (referred to herein as T4) and 3,5,3'-triiodothyronine (referred to herein as T3). However, approximately eighty percent of the serum T3 present in the body is produced by the extrathyroidal monodeiodination of T4 to T3. When dosages of dinitrophenol are taken, hypothyroidism is induced, not by a reduction in activity of the thyroid, but by a reduction of the rate of extrathyroidal conversion of T4 to T3. While both T4 and T3 are biologically active, T3 is much more active than T4. Thus, the reduction in serum T3 concentration induced by taking dinitrophenol substantially offsets the metabolic effect of the dinitrophenol. By analogy, the reduction in serum T3 concentration is similar to that observed in fasting patients. Typically, normal serum T3 concentration ranges from about 70 to about 200 ng/dl.

      It has further been discovered that deficient serum T3 concentrations resulting from administration of dinitrophenol can be restored to normal concentrations by concurrently administering a thyroid hormone preparation therewith.

      In practicing the method of this invention, dinitrophenol is administered to the patient. The metabolically active dinitrophenols suitable for use in the invention include 2,4-dinitrophenol and the salts thereof. By the term administration is meant any suitable manner of introducing the medication into the patient's body, including orally (p.o.) and topically. The preferred manner of administering dinitrophenol is orally, as in the form of a tablet or capsule.

      The amount of dinitrophenol given should be sufficient so that the patient experiences increased body temperature. Preferably, the body temperature is elevated approximately 1.degree. F. The dose of dinitrophenol required to obtain this result varies from patient to patient, depending on factors such as, for example, weight, age, health, environmental conditions, physical activity, nutrition, and psychological state, but will normally be in the range of from about 60 to about 500 mg per day, or about 0.60 to about 5.0 mg/kg of body weight per day. Preferably, the dinitrophenol is administered in daily or alternating daily dosages, insuring that no cumulative effective results, such as excessive thermogenesis.

      It is essential that the amount of dinitrophenol administered not exceed toxic doses. In a few patients, adverse reactions may occur at dosages of dinitrophenol which are not effective to elevate the body temperature, contraindications including any clinical state in which there is hypermetabolism, such as hyperthyroidism, ongoing infections, and pregnancy, and any other clinical conditions such as heart disease, chronic obstructive pulmonary disease, Addison's disease, liver disorders, or renal failure. Most are safely treated with suitable results from the aforementioned dosages.

      Concurrently with the administering of the dinitrophenol, or shortly thereafter, a thyroid hormone preparation is administered to the patient. As used herein, the term thyroid hormone preparation includes any suitable preparation which restores the serum T3 concentration, including preparations containing 3,5,3'-triiodothyronine, thyroxine, derivatives thereof or combinations thereof. Preferably, the thyroid hormone preparation contains T3. Because of the varying potency of such preparations, dosages of thyroid harmone preparation are reported herein on a T3 equivalent basis.

      The thyroid hormone preparation is administered in an amount sufficient to maintain the pretreatment serum T3 concentration in the patient, typically about 70-200 ng/dl in normal patients. Generally, from about 25 to about 200 mcg T3 equivalent per day, or from about 0.3 to about 2.7 mcg T3 equivalent per kilogram of body weight per day, is sufficient. Preferably, the thyroid hormone preparation is administered daily. In an especially preferred embodiment, the thyroid hormone preparation is administered orally with the dinitrophenol.

      As described above, the rate of extrathyroidal conversion of T4 to T3 may vary as treatment with the dinitrophenol progresses. Thus, it may be necessary to increse or decrease the dosage of the thyroid hormone preparation accordingly.

      It is preferred that in the practice of the method of this invention, the patient be closely monitored, especially in the initial stages of treatment. Recommended pretreatment and initial treatment protocol includes physical examination, electrocardiogram, and stress electrocardiogram if indicated, complete blood count, urinalysis, thyroid function studies (T3, T4 and reverse T3), serum electrolytes, HDL cholesterol, serum creatinine, blood urea nitrogen, uric acid, calcium, pulmonary function tests and liver function tests including liver enzymes, biliribin, and alkaline phosphatase.

      In an especially preferred embodiment, the patient is started on initially lower dosage rates of dinitrophenol, about 250 mg every other day, and thyroid hormone preparation, about 25-50 mcg/day on a T3 equivalent basis. After 2-12 weeks of this treatment, if no adverse reactions are noted, the dosage rates may be increased to about 250 mg dinitrophenol alternated daily with about 125 mg, i.e. 250 mg on even-numbered days and 125 mg on odd-numbered days, and to about 100 mcg/day thyroid hormone preparation on a T3 equivalent basis. When the weight goal of the patient is achieved, the administration of the dinitrophenol may be discontinued, and the thyroid hormone preparation continued to maintain the patient's weight. While dietary control need not be strict, weight loss and weight maintenance are facilitated by moderate caloric intake of less than about 1800 calories per day, during and following treatment.

      This method is illustrated by way of the case histories which follow.

      Case 1

      A white female 31 years of age with a weight in excess of 200 pounds had attempted to loss weight with various diet plans. She had only been able to achieve about a 20-pound loss, and had immediately regained the weight. The patient was nulliparous and had no ongoing medical problems. Upon physical examination, she had a weight of 208.5 pounds, a height of 5 feet, 3 inches, and a blood pressure of 132/80, without any goiter. Laboratory analyses, including complete blood count, liver profile, serum electrolytes, kidney function tests and thyroid function tests, were all within normal limits. Because of her familial history of heart disease, she underwent a stress electrocardiogram which was normal other than early fatigue and calf cramping.

      The patient was started on CYTOMEL brand of liothyronine sodium (manufactured by Smith, Kline and French), 50 mcg/day p.o., and on 2,4-dinitrophenol, 250 mg every other day p.o. On the 19th day of medication, the patient had normal vital signs and the dosages were increased to 100 mcg/day liothyronine, and 250 mg/day dinitrophenol alternated every other day with 125 mg/day. The patient was subsequently maintained on these dosages and returned for follow-up examinations approximately every 3 weeks. The weight loss history is seen in Table 1. After 241 days of medication, the patient has achieved her weight goal of 135 pounds. Administration of the dinitrophenol was discontinued and the patient was maintained on liothyronine, 100 mcg/day p.o. No weight gain was subsequently observed.



      TABLE 1
      ______________________________________
      ----------Day----------Weight (lbs)
      ______________________________________
      ----------1 -----------208 1/2
      ----------19 ----------202 1/2
      ----------35 ----------196 1/2
      ----------49 ----------189 1/2
      ----------69 ----------184
      ----------92 ----------175
      ----------113 ---------167
      ----------134 ---------160
      ----------155 ---------152 1/2
      ----------180 ---------148
      ----------206 ---------146
      ----------241 ---------135
      ______________________________________


      Case 2

      A male 40 years of age with a weight of approximately 250 pounds had attempted to lose weight with a variety of diet plans and diet medications. Success had been limited to 5-10 pound weight losses, with immediate regain. On physical examination, the patient has a height of 5 feet, 10 inches, a weight of 255 pounds and a blood pressure of 160/100. Complete blood count, SMAC, serum electrolytes, thyroid function tests, glucose tolerance tests and stress electrocardiogram were normal.

      The patient was started on liothyronine, 50 mcg/day p.o., and on dinitrophenol, 250 mg every other day p.o. After two weeks, the blood pressure returned to normal (130/80), and the dosages were increased to 100 mcg/day liothyronine and 250 mg dinitrophenol alternated daily with 125 mg. The weight loss history is presented in Table 2. Once the weight goal of 167 pounds had been achieved, the patient was taken off the dinitrophenol administration and the 100 mcg/day liothyronine medication was maintained. The patient was instructed to restrict caloric intake to approximately 1800 calories per day. No subsequent weight gain was observed.



      TABLE 2
      ______________________________________
      ----------Day----------Weight (lbs)
      ______________________________________
      ----------1 -----------255
      ----------14 ----------241
      ----------30 ----------232
      ----------44 ----------227
      ----------65 ----------220
      ----------76 ----------214
      ----------97 ----------208
      ----------125 ---------203
      ----------153 ---------197 3/4
      ----------181 ---------193
      ----------209 ---------189
      ----------279 ---------178
      ----------321 ---------167
      ______________________________________


      Case 3

      A white male 38 years of age with a weight of approximately 342 pounds had made numerous attempts to lose weight "with all methods" without any success. Upon physical examination, the patient had a weight of 352 pounds, a height of 5 feet, 11 inches and a blood pressure of 150/110. Other than a slight enlargement of the heart on X-ray and +3 pitting edema, the physical examination was unremarkable. Laboratory analysis initially revealed a blood sugar of 372 with a glycohemoglobin of 14.3 (normal 4.4-8.2). The remaining tests, including stress electrocardiogram, were within normal limits. The patient was started on liothyronine, 50 mcg/day p.o., and dinitrophenol, 250 mg every other day, and was instructed to restrict his caloric intake to approximately 1800 calories per day. On the 59th day of treatment, the dosages were increased to 100 mcg/day liothyronine, and 250 mg/day dinitrophenol alternated every day with 125 mg. The patient's weight loss history is presented in Table 3. Following treatment, the dinitrophenol administration was discontinued and the patient was maintained on liothyronine, 100 mcg/day p.o. and instructed to maintain his caloric intake to approximately 1800 calories per day. No subsequent weight gain was observed.



      TABLE 3
      ______________________________________
      ----------Day----------Weight (lbs)
      ______________________________________
      ----------1 -----------354
      ----------24 ----------333
      ----------38 ----------314
      ----------59 ----------317
      ----------80 ----------297 1/4
      ----------101 ---------288
      ----------122 ---------275
      ----------143 ---------260 1/2
      ----------164 ---------254
      ----------185 ---------243 1/2
      ----------206 ---------246
      ----------227 ---------235 1/2
      ----------248 ---------234
      ----------269 ---------229
      ----------290 ---------222
      ______________________________________


      The above cases illustrate the effectiveness of the method with obese patients unable to reduced their weight by conventional methods.

      Having described any weight loss method above, many variations in the details thereof will occur to those skilled in the art. It is intended that all such variations which fall within the scope and spirit of the appended claims be embraced thereby.
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      Why you might want to use DNP.

      Add some DNP to an animals diet. DNP can get metabolism up at least 50% which is conservative as some say 75% This would mean if the animal eats 3000 calories maintenance they are now at 1500 calories a day with no change in diet! A 2500 calorie a day would leave them with 1250 calories a day. There are 4086 calories in 1lb of fat and at 3000 calories a day your DNP adjusted calories for the day is 1500. Multiply that x 7 days to give you 10500 calorie deficit which is 2.5 lbs of fat loss for the week. At the 2500 calorie you have a 2.14 lb fat loss. These are both below what the BO diets claim and you don't have to stop eating!

      If your animals weigh around 200lbs their effective dose is 400mg and the max can be as high as 800mg a day.
      High fat diets market on the basis that you are going to be able to lose 1.5?2lbs of fat by just changing your diet!

      1 gram of fat is 9 calories. There are 454 grams in a 1 pound. This gives you 4086 calories for 1lb of fat. If you want to lose that 1lb of fat you have to have a 4086 calorie deficit to do it. In other words, you need ?4086 calories in your diet if you want to lose 1 lb of fat. Now, Let's say you are at 3000 cal a day for maintenance. That is 21000 calories a week. You believe the marketing of the post above and think you can lose 1.5lbs of fat. That, my friends, is 6129 calories which you have to subtract from 21000 which leaves you with 14871 calories for the week or 2124 calories a day. You are going from 3000 to 2124 a day. If you want to lose that great sounding 2 pounds you are now at 12828 for the week or 1832 calories a day.

      Let's be realistic and put you at 2500 maintenance calories. To lose 1.5lb you now need 11371 calories a week or 1624 calories a day or a nearly 900 calorie a day change. To lose the magical 2lb a week you need 9328 calories for the week or 1333 calories a day or a 1167 calorie change per day! That is rather difficult, but let?s add some DNP which can get you metabolism up at least 50% which would mean you are now at only 1500 calories a day for a 3000 calorie diet with no change in diet! A 2500 calorie a day would leave you with 1250 calories a day.
      These are both below what the BO diets claim and you don't have to stop eating!


      What you want to keep in mind

      Everyone is different.

      Don?t take it on an empty stomach or it will feel like you have indigestion for most of the day.

      I wanted to stress not to just go balls out (5mg/kg) and you should move up gradually on DNP for your first experience.

      If you have an allergic reaction with red spots and itching then stop the DNP and get some Benadryl and then you should be able to start again.

      The type of diet will also affect how you feel, as well as the type of workouts you are doing. These are variables you also will have to figure out for yourself. The logic of my dieting regimen follows that while you are DNP all the glycogen/glucose is being scavenged to provide ATP for the mitochondria so you will want to eat a regular diet. High fat BO is not going to help you build muscle even though DNP is anti?proteolytic (protein sparing).. Furthermore, when you eat fat it is more likely to go to fat! That is scientifically proven. So if I'm trying to burn fat, why would I want to eat it right back?

      DNP is anti-proteolytic which means it uses carbohydrates or fats exclusively to supply energy for the mitochondria and does not facilitate muscle breakdown, however, this does not therefore mean DNP is positive for muscle building. The cells are running on overdrive and they are not going to be looking to make themselves bigger which requires even more energy.

      Everyone is different and other supplements you take will affect your results, but as a whole, most people are not going to do well or feel well on high fat and DNP. I also have found that taking particular supplements helps with how will you feel while on the DNP.

      I feel better when I don't do huge carbs, however, when I don't do any as in high fat type diets, my workouts suffer just the same. Each individual has to decide for themselves and put those factors into perspective with what their goals are and how fast they want to accomplish them and how bad they are willing to feel for the desired weight loss.

      WARNING: DNP will turn everything and anything yellow including skin, clothes, carpet, and hair. I dropped a capsule in my DNP container and bent over to look for it and my hair touched the edge of the container and my hair got dyed yellow! My hair did not even touch the DNP, but just the side of the container for about 2 seconds! DNP for the most part is not removable or bleachable with normal chemicals. It will also track. By that I mean, you think you have washed it off your hands and you touch something and later you see yellow spots on what you touched. If you are making caps you need 2 pairs of gloves, at least, as the DNP goes through the first pair due to an atrraction it has for moisture. DNP sublimes and floats. Due to this sublimation it will land on EVERYTHING if you leave it out even if there is no air circulation. DNP goes through EVERYTHING including plastic, hdpe plastic, pet plastic, plastic bags, nitrile and latex gloves. It can be washed out of clothing with hot water and detergents that have phenolic compounds in them such as Tide. DNP is not solvated by laquer thinner, acetone, paint thinner, or turpentine or any of the common organic solvents. If you wash your hands immediately after touching DNP with gamma-butyrolactone, otherwise know as GBL and use to make GHB, and then a detergent such as Dawn dishwashing soap, the stain will come out for the most part.

      I have to say that a certain guru which some people keep quoting is what I feel to be a very unreliable source. I will give him credit for bringing DNP to the forefront, but I will bet you a million bucks that he has never done it or mixed it. Here is a quote that bears this out; 'I don't see what the worry is about everything turning yellow? I have no problems, I just dry it out and cut it with a credit card and cap it.?

      That is total BULL****!. Anyone who has used or mixed DNP powder knows that it will get on EVERYTHING and turn it yellow. It goes through plastic bags. Just today I was sending someone 3g for research and I put it into a ziploc and 2 hours later I came back and the envelope under the bag was YELLOW! It goes through 1 laver of rubber gloves. It turns white HDPE bottles yellow. It floats everywhere. I had to put my stuff in a hood because it got on everything I had sitting out and I had to wash all my glassware and scales before I could use them again. DNP floats by sublimation which would be known just be reading the safety sheet or the Merck Index.. On the basis of that statement alone I have some real problems believing anything he says on the subject, but another famouns quote is, ?DNP will raise your body temp high enough to kill you!? This also proves that he has never done it because as you will find, your body temp only goes up about one degree. Ok, enough about the fake guru.

      Someone just asked me if the **** I sent them was real. Well, if you want a test then rub it on your hands and throw some on your carpet. When your carpet has to be replaced because NOTHING can remove the yellow and you look like a total ass because your hands are bright yellow, then you can ask me if it is real!

      Mostly people are taking DNP for 1 week at a time because it exhausts you and you sweat a lot, usually that is what I do, but due to my ?work? with DNP I got a dose while on an ECA week and that combination of DNP-ECA was like methamphetamine. In fact it was better because it had less side affects. I would venture that DNP-PPACA would also have the same methamphetamine effects. At this time I do not know, however, whether PPA works on the same receptor so I would not do them back to back in cycles. ECAY where Y is yohimbine is also a combination that has me*h type benefits. Clen-DNP did not exert any magical me*h benefits that I noticed.
      Have not taken PPACA or PPACA-DNP or PPACAY.

      Tyramine and yohimbine are awesome and someone that I hold using it was getting goosebumps and asked a pharmacologist what the goosebumps were about. The pharmacologist told him that it meant he was burning a lot of calories. I love this combination and it is just like me*h due to large releases of NA although it only lasts 4 hours or so.
      DNP also ?upgrades? the effects of clen. If you have used clen before and it had/has stopped working, then DNP will bring back it?s glory.

      I like to keep the clen and DNP a week apart due to the affects they have on T3 although they work on different mechanism it is just a precaution to keep from shutting down the T3. You could add Y to it for an added benefit which will not cause downgrade of anything. Reports on DNP-Y indicate a higher rise in body temperature on this combination.

      Due to the systemic affects of DNP, it affects EVERY cell in the body that has mitochondria, including smooth (digestive) and muscle and fat as well, you will not see a significant rise in body temp like you see with clen or ECA. Clen and ECA work primarily on muscle cells and that causes a rise in body temp just as if you were working out. I don?t know why this is such a difficult concept for some to understand, but I was sweating like hell recently, and I took my temp and it was 95.8. ON DNP!


      DNP MECHANISMS

      The basics first. DNP is a classified as a chemical poison. It?s mode of action is to disrupt the ETC (electron transport chain) and cause uninhibited exchange of protons. This exchange of protons is what is responsible for making ADP into ATP. NOTHING can stop the disruption of this process once it starts. DNP works no matter what! High or low T3 has nothing to do with whether or not DNP affects the mitochondria and burns off extra energy. DNP gets into the cell and into the mitochondria and causes proton release. No other hormones are needed or noted.

      Even so, it works in much the same way as clen or ECA or PPACA or thyroid. They ALL cause the metabolism to speed up. These all work via the mitochondria as well, although the non-DNP diet drugs work on the receptors first and DNP goes directly to the mitochondria, the results are the same which is speeding up the metabolism to burn fat.

      Some other important facts you should know are how ephedrine and beta-3 activation drugs work.
      These both cause uncoupling of the ETC chain just like DNP! Ephedrin works part of its magic via beta-3's and much research has been done looking for a magic beta-3 drug. Why, we have it and it is called DNP! If you are sitting around and something is making you hotter, you are most likely experiencing an uncoupling of the ETC chain. No big deal, but DNP just causes a greater effect.
      I knew there was a reason that you CANNOT die from DNP usage, at least the doses many are doing. I talked to a couple people about this but just couldn't find the info to prove it. Ok, so what does DNP do? It uncouples the ETC or oxidative phosphorylation as was elaborate upon above, allowing electron flow to go unchecked at maximal rate and resulting in heat production and ATP depletion.

      ATP depletion is the key. What condition exists when you have totally exhausted all ATP and no more is being created? A very good instance we all know about is when you are dead and it is called ?rigor mortis?. Rigor mortis results because no more ATP is binding to the myosin head of the sarcomere in the muscle fibers.

      So what does this have to do with us? No one has ever had rigor mortis on DNP or even severe cramping that has ever been documented. Furthermore, and to be more specific as to the uncoupler DNP, the electron gradient is collapsed and it runs unchecked at maximal as I have explained above, but as the gradient continues to increase electron transport becomes more difficult and the process SLOWS! Additionally, under very large artificially created electrochemical proton gradients, normal electron flow stops and may even result in
      REVERSE electron transport flow!

      All that was complicated and here is what it means. The respiration chain has a safety mechanism which allows for feedback controls to keep you from killing yourself. This is also another reason you will not want to do DNP for long periods. If you have taken enough as to create a large gradient the flow of electrons your burning of calories might even STOP! This will happen if you don?t eat enough calories and appears to be more detrimental on a high fat type diet because as you will see below, glucose can ameliorate charge differentials in the mitochondria and at the cell surface while on DNP.


      DNP works NO MATTER WHAT! It uncouples the electron transport train (ETC) and there is nothing you can do to stop it. Some have said it doesn't work after a small dose or only after taking DNP for 2 days or so. I think they are the same kind of person who would take a drink of beer and say, 'Oh, I'm not drunk so alcohol doesn't work'! Alcohol still affects your brain cells and hormone levels and slows down the metabolism. Just because you didn't drink enough to be drunk doesn't mean nothing happens!

      DNP is anti?proteolytic. This means DNP does not break down protein via the mechanism through which DNP works. DNP is actually better for you than cardio because exercise is PROTEOLYTIC which in itself is another reason to not be doing a high fat diet. High fat diets and exercise both lower insulin and raise glucagon levels which cause breakdown of protein. It is a proven fact that 10?20% of energy from exercise comes from AA breakdown as well as release of glutamine from the cells. DNP burns calories and does not affect hormone levels. Someone said something about it causing ketosis which is likely if you don't eat any carbs, but DNP is not, by itself going to affect insulin levels like glucose disposal agents metformin or phenformin.

      DNP is not going to be advantageous to muscle building. THIS DOES NOT DISAGREE WITH WHAT I WROTE ABOVE! It is anti?proteolytic via its mode of action, BUT if there is not enough energy in the cells to build muscle it ain't gonna happen. Again, diet is key.

      DNP is one of the SAFEST drugs you can take!!!!! Why? Am I nuts?! I am basing this on DNP's mode of action. DNP has one purpose and mechanism and affects nothing else, but the mitochondria. DNP does not affect hormone levels as do clen, ECA, T3, etc. It has no side affects that you don't expect such as shakes or cramping. Compare DNP to some of the Drugs the FDA has approved and look at their side effects and then tell me what is safer! HAHA!

      After you read this study you need to ask yourself, need I say more? In the earlier paragraph on the mechanisms of DNP on the mitochondria I explained the safety mechanism which could keep DNP from being totally depleted of ATP. Some were saying ATP depletion would result in cell death. The study below illustrates another mechanism which I didn?t know about. The crux of it can be summarized by this sentence: ?The failure to find a reduction in ATP concentration in either fibre type during prolonged exercise in the face of a progressive increase in the number of fibers showing little or no glycogen concentration suggests that protective mechanisms exist that prevent an energy crisis. The nature of these protective mechanisms remains to be elucidated. ? In other words,

      When glycogen is gone there is a mechanism which keeps ATP from being depleted which is unknown at present!


      Energy metabolism in human slow and fast twitch fibers during prolonged cycle exercise.

      Author Ball?Burnett M; Green HJ; Houston ME
      Address Department of Kinesiology, University of Waterloo, Ontario, Canada.
      Source J Physiol (Lond), 437():257?67 1991 Jun
      Abstract

      1. The effects of prolonged exercise on energy metabolism in type I and type II muscle fibers in the vastus lateralis muscle were investigated in six male subjects (20.0 +/? 0.5 years, mean +/? S.E.M.) who performed one?legged cycling at 61% of maximum O2 consumption (VO2,max; determined with one leg) until fatigue or for a maximum of 2 h. 2. Analysis of pools of freeze?dried fibers obtained by needle biopsy and separated into specific types by the myofibrillar ATPase histochemical procedure indicated higher (P less than 0.05) lactate concentrations in type II fibers compared to type I fibers at 15 min (43.9 +/? 9.7 and 51.2 +/? 9.8 mmol (kg dry wt)?1) and at 60 min (18.2 +/? 4.7 and 25.9 +/? 6.5 mmol (kg dry wt)?1). No differences existed in lactate concentration between fibre types for pre?exercise (10.0 +/? 1.6 and 13.3 +/? 2.8 mmol (kg dry wt)?1) or post?exercise. 3. Glycogen degradation was most pronounced in type I fibers. By the end of exercise, glycogen concentration was 82.4 +/? 45 mmol glucosyl units (kg dry wt)?1 in type I fibers and 175 +/? 62 mmol glucosyl units (kg dry wt)?1 in type II fibers. 4. No significant changes in ATP and creatine phosphate (CrP) were found in either fibre type with exercise. 5. It is concluded that, at least for lactate and glycogen, fibre?specific differences are evident in prolonged submaximal exercise. The cause of the difference probably relates both to the unique energy metabolic characteristics of each fibre type and to the manner in which they are utilized during the exercise. 6. The failure to find a reduction in ATP concentration in either fibre type during prolonged exercise in the face of a progressive increase in the number of fibers showing little or no glycogen concentration suggests that protective mechanisms exist that prevent an energy crisis. The nature of these protective mechanisms remains to be elucidated.

      DNP will make you breathe harder via a mechanism called cellular hypermetabolism. You aren?t going to die if you are breathing hard! DNP works by increasing ventilation and oxygen consumption via hypermetabolism of the cell. DNP makes you breath hard.


      Role of tissue hypermetabolism in stimulation of ventilation by dinitrophenol.
      Author Levine S
      Source J Appl Physiol, 43(1):72?4 1977 Jul
      Abstract

      Several authors have hypothesized that tissue hypermetabolism accounts for increases in ventilation (VE) elicited by 2,4?dinitrophenol. However, some data in the literature indicate that stimulation of VE by isomers of dinitrophenol is unrelated to tissue metabolic rate. To test this latter concept, we compared three different isomers of dinitrophenol (i.e., 2,4?dinitrophenol (2,4?DNP), 2,5?dinitrophenol (2,5,?DNP), 2,6?dinitrophenol (2,6?DNP) with respect to stimulation of VE and with respect to stimulation of oxygen consumption (VO2). In all experiments, 3?4 mg/kg of one dinitrophenol isomer was administered to chloralose anesthetized dogs by intra?arterial infusion. 2,4?DNP elicited large increments in both VE and VO2, 2,6?DNP elicited moderate increments in both VE and VO2, whereas 2,5?DNP elicited small increments in both VE and VO2. These observations demonstrate a correlation between ventilatory and metabolic changes affected by isomers of dinitrophenol. Accordingly, these results are consistent with the hypothesis that ventilatory stimulation by congeners of dinitrophenol is related to tissue hypermetabolism.




      How to feel good on 600mg of DNP!

      This is not an advertisement because I sell more encapsulated DNP for research than I care to spend time making. Note: I sell it for ?Research?

      The longer I took DNP the more I realized those who had originally recommended DNP use were not looking at the big picture, and they had most likely never used it or mixed it themselves, and/or were just complete morons!

      Myth #1.
      You die on DNP from heat related to overdose.
      Wrong!
      You die from dehydration resulting in heat exhaustion and then heat stroke.

      Myth #2.
      You can do it on high fat-low carbohydrate type diets.
      NO YOU CAN?T!
      High fat-low carbohydrate diets are based on keeping your blood sugar and insulin low. DNP will also drive down your blood sugar, so if you want to have blurry vision due to low blood sugar and feel like hell, you go right ahead.
      Glucose also has some beneficial cellular effects when used with DNP..
      Myth #3. You will go blind.
      Right! If you do high fat-low carbohydrate diets and don?t keep your blood sugar up and/or don?t take pyruvate.

      All about DNP : Animal's manuel (continued)


      Myth #4.
      You can?t work out on DNP.
      Yes you can, if you know what you are doing and which I am about to tell you.

      As you may already know you, should be taking the following per day.

      1200-1500mg magnesium in 2-3 divided doses.
      2-3000mg vitamin C.
      1200IU of vitamin E
      200mcg of selenium.
      1000-2000mg of calcium (can?t take it with the magnesium, though. Take it before bed)
      Melatonin if you can?t sleep and it is also one of the best and cheapest anti-oxidants.
      50mg of zinc a day
      one iron tab as hemoglobin is a protein as well.
      A potassium gluconate tab or two a day
      Taurine at 3g a day.
      Glutamine at 15g a day sublingual or with carb/protein drink.


      I think taurine will be most beneficial for cramping and holding onto water. I have worked with some mountain bikers that were having trouble with cramps and had tried using the proverbial potassium supplementation cure and it didn?t work. I had them take the taurine and magnesium and the cramping went away. Taurine is also give to people who have leg cramps at night at a dosage of 3-6g a day resulting in total alleviation of the cramps. Clenbuterol depletes the liver of its taurine supply which changes the osmotic pressure and therefore stops T4-T3 conversion. Taking supplemental taurine can alleviate this.

      Glutamine also regulates water, but is a ***** to take and unless you want your small intestine to absorb most of it you have to take it sublingual. You can fool the body a bit by putting it into your carb/protein drink after you work out or by taking 2g doses throughout the day. Glutamine ALSO causes a rise in insulin.

      IF you are on clenbuterol, pyruvate and glycerol will help you a little, and I don't know why, but I still got some cramping on clen after an event even on P and G. The latest research I have indicates that the reason clen may cause cramping is due to TAURINE depletion so by taking the 3g a day taurine you should be able to ameliorate those effects as well and keep your thyroid levels normal as well.

      In addition to the vitamins and minerals you should be taking:

      3-6g Pyruvate (P)
      3 tablespoons Glycerol (G)

      If you can't get the G and P go right to the taurine which may be cheaper as well.
      Glycerin (glycerol) is avail in the skin care section of your pharmacy and 4oz is about1?2 dollars or there are larger versions in white bottles and the brand name is H something. Just buy it from a vet and a gallon is around $20!

      I felt like **** when I went above 400mg and sweat profusely on single large doses of 600mg and 800mg which lasted for 2 days. I weigh around 95kg (210).

      The object of the DNP dosing with the glycerol and pyruvate was to test their benefits on what is considered an overdose of DNP while maintaining my exercise level in the middle of summer.

      Here is what I was taking:
      600mg of DNP which would be 6mg/kg which is well above the recommended 3-5mg.

      DNP is said to have a half life of 36 hours and this is what I have based the following dosing scheme. I also have anecdotal evidence that DNP can last 48 hours or more. When I took an 800mg dose after 3 days on 300mg a day I sweat for 48 hours straight and that 800mg was the last dose I took.

      You have to divide the 600mg into two doses of 300mg 12 hours apart.
      After you hit your 600mg limit you don?t take the next 300mg for 36 HOURS from the first dose!
      So, if I took the first dose at 6AM on Sunday morning and the second 300 mg dose at 6PM Sunday night, the 3rd dose would not be until 6PM on Monday evening. The fourth dose would again follow 12 hours from the 3rd which would be at 6AM on Tuesday morning.

      I am also taking EC with this just for fun although at only 2 x a day for the EC to keep energy levels up and lessen the carb craving that goes with DNP.

      How am I not sweating all over the place and not feeling like **** and/or dehydrating in the middle of summer while going on hour or longer rides in 85 plus heat?. Let me tell you again that I hated the way DNP made me feel.


      YOU HAVE TO TAKE GLYCEROL AND PYRUVATE!
      I don?t know if you can take one without the other because I was using the glycerol (G) and pyruvate (P) to enhance endurance and stem dehydration which I am very prone to. I think, however, that you will have to do them both as there may be a synergistic benefit. I have taken G alone and while you have more water to hold on to, you just seem to sweat more which is also backed up by the research. The G-P cocktail let me drink ? my normal volume of water on rides and that is what made me try the DNP-ECA experiment.

      Glycerol dose. YOU ONLY NEED 1 TABLESPOON 3 TIMES A DAY! One in the morning, one in the afternoon and one right before bed. Don?t listen to the researchers who tell you to take 1 gram for every kg body weight 1-2 hours before and event. They are idiots and obviously have never taken it or asked the athletes how they feel. Let me tell you, you feel awful taking that much glycerol! You feel bloated and sometimes get a headache and you **** A LOT! 1 tablespoon 3 times a day comes out to ? what they recommend to take 2 hours before an event. The glycerol keeps your muscles hydrated and limits the sweating. It will fight the dehydrating effects of the ECA. As we know, DNP is carbohydrate/fat specific and glycerol also is a 3 carbon carbohydrate source that can?t go to fat!. Glycerol also increases power output which may be an added benefit of the type of carb source it is. Glycerol is converted to glucose in the liver and in the liver is where it stays for the most part and does not, therefore, raise insulin levels.

      Before I explain the pyruvate, let me tell you that glycerol and glycerin are the same thing! A good recipe for taking your glycerol is 1 packet of Kool-aid, 1/8 cup sugar, 1 tablespoon glycerol and 32-oz of water. The glycerol makes the kool-aid taste like OJ because there are alcohols and fermentation products in the OJ which the glycerol mimics.

      Pyruvate dose. 2-5grams a day. Start out at 900mg or so 3 times a day and go up from there. I am at 1.5g 2-3 times a day and if you don?t work your way up it will give you gas and the runs. As I mentioned above, I think the P is working synergistically to hold on to the water in your muscles. Additionally, it is another 3 carbon energy source and/or it is manipulating the Krebs Cycle intermediates and allows for a different energy production pathway. Pyruvate changes/manipulates an ATP/energy pathway and decreases lactic acid output and if it ain?t the Krebs cycle I don?t really care. It works.

      Some abstracts on the benefits of pyruvate.

      Pyruvate and the heart and glucose and insulin.

      Cardiac metabolism and electromechanics of human heart.
      Author Prasad K
      Source Recent Adv Stud Cardiac Struct Metab, 10():119?37 1975
      Abstract



      Part 2
      The effects of substrates on the metabolic inhibitor?induced changes in the action potential and contraction of papillary muscles obtained from patients undergoing corrective open?heart surgery were studied. Anoxia produced a marked shortening of the action potential duration and a decrease in the resting potential, rate of rise of action potential, effective refractory period, and contractility. In anoxic muscle, although glucose completely restored the action potential duration, effective refractory period, and resting potential to control levels, it was unable to completely restore the contractility to the control level. Substrate depletion and metabolic inhibitors (iodoacetate, dinitrophenol) produced effects similar to that of anoxia, but at a faster rate. Glucose restored the action potential and, to a lesser extent, contractility to the control level in dinitrophenol?treated muscle but was ineffective in so doing the iodoacetate?treated muscle. Pyruvate, however, was effective in restoring the action potential and contracility in iodoacetate?treated muscle. Pretreatment of the muscle with glucose and, particularly, with glucose plus insulin prevented the combined effects of anoxia and lack of glucose on the action potential and contractility for a prolonged period. These results suggest that intravenous infusion of glucose and insulin before and during surgery might prevent or reduced the effect of anoxia on the electrical and mechanical activity of the heart during open?heart surgery.

      Pyruvate was able to restore the action potential (charge) of cells treated with DNP! Unfortunately, most of you won?t understand what an AP is even if I explained it, but I will tell you that restoring it is signiificant!

      Now you have a recipe on how to feel good on an overdose of DNP! To recap you need:
      3 Tablespoons glycerol 3x a day.
      1g Pyruvate 3x a day.
      Taurine at 3g a day.
      DNP at 36 hour intervals.

      If you start to feel bad, just drink some sugared pop or take some glucose or maltodextrin with your psuedo-OJ mix. The only drawback is that you will still smell rather bad and will emit a vinegar type odor although you won?t be sweating all over everything. If you notice you are starting to sweat more it is time for another glycerol dose.

      Use of AS during DNP

      You can use DNP during an AS cycle although the muscle loss from DNP is minimal, if any, so I don?t think this is the best use of your AS. If, however, you have hit a plateau the DNP for a week will help you break through that plateau in the subsequent week off. Now, I have experienced this, as have others, but as to whether or not it is from an upregulation or having a rush of T3 available or a type of overcompensation rebound is unknown, but it is cool and it happens..

      Use of AS after DNP or dieting.

      DNP and dieting BOTH stop conversion of T3-T4. T3 is responsible for protein synthesis. If you have been on a diet for 2 weeks or more your thyroid will be depressed and so will protein synthesis due to low T3. By adding AS you will be increasing protein synthesis while waiting for your thyroid to come back online so you won?t get fat right after a diet.

      Use non-aromatizing AS like equipoise, ganabol, maxigan, trenbolone (finaplix or Anibolan), winny-V. Or you can use testosterone and an anti-aromatase like cytadren or arimidex. If you want to keep the fat off you HAVE TO use those anti-aromatazes with the testosterones and d-bols as they are the only ones that stop conversion of testosterone to estradiol. Estradiol conversion will make you fat, especially around the waist! If you have to use a testosterone and want to lose fat, I would use cytadren because it increase hormones which cause fat loss as well as increasing IGF-1 levels! (Bet you didn?t know that!) I would, however, not stay on cytadren longer than one month and dosage is one tab divided into 4 doses per day.
      A line from a study showing that estrogen makes you fatter for the non-believers!
      Obes Res 1995 Nov;3 Suppl 4:561S?568S
      Topical fat reduction.
      Greenway FL, Bray GA, Heber D
      Department of Medicine, UCLA School of Medicine, Torrance, CA, USA.

      The fat on women's thighs is more difficult to mobilize due to increased alpha?2 adrenergic receptor activity induced by estrogen. Lipolysis can be initiated through adipocyte receptor stimulation (beta adrenergic) or inhibition (adenosine or alpha?2 adrenergic) or by inhibition of
      phosphodiesterase.

      While yes, they talk about women and estrogen and fat, the mechanism is still absolute and spans the sexes. Estrogen makes fat cells resistant to lipolysis. Still want to take that test without and anti-estrogen?


      Get to fat burning faster!

      This is something you can try after you have used DNP once and know your tolerance and is a DNP manual exclusive! Your working dose will be around 400mg a day, correct? The first day, however, you are going to take 600mgs in divided doses! It takes DNP a couple days to build up so this won't bother you in the least. On the second day you will start taking 200mg caps every 8 hours until you are sweating or getting the heat you want. Now you are at your tolerance dose and you can space it out to the 36 hour dosing.


      NEW!
      Use a blood buffer to combat free radicals and lactic acid!

      Add up to one tablespoon of baking soda, sodium citrate, or potassium citrate to your drink of choice throughout the day. A mix of the sodium and potassium would be best. Why?
      What does DNP and exercise have in common? During high intensity exercise (supramaximal) ATP production is supplied by anaerobic glycolysis. This increases levels of H+ (protons) both inside and outside the cell via lactate and results in the feeling of fatique (Hermansen and Osnes; Sahlin) In the past, the use of sodium bicarbonate (baking soda) has been used and has been shown to decrease acidosis via buffering of the blood. The problem with baking soda is gastric distress and high salt intake with the recommended dosage of 300mg/kg which is around a tablespoon of baking soda for most people. Dosage for sodium citrate is 100mg-500mg per kg and did not give stomach problems to the users. Time to exhaustion was increased 15% which is the same as with baking soda. Alkalosis (making the blood basic) has been found to increase the rate of lactate and proton release from muscle into the blood. An increase in muscle pH causes phosphofructokinase inhibition (PFK) which is the controlling enzyme in glycogen utilization and therefore causes an increase in lactate formation. Those two mechanisms also will hold true for DNP as DNP releases protons which causes the heat. Get it out of the cell with the citrates.


      Testomonial:
      Hey animal just thought I?d let you know the great results I had with the DNP. I got tested hydrostatically and I'm at 4.8%. DNP is really the ****. Anyway, a buddy of mine is competing in a month and he's currently at 7% bf(he's about 190lbs) and he'd like to do it for two weeks. I understand that the lower one's bodyfat % the greater amount needed (I responded very well to 4mg/kilo but I was also dieting)


      Questions I have answered for DNP users

      Are all of the losses on DNP fat losses?
      You can?t ever say ALL in the scientific world, but it is the best we can get!


      Animal, you have been a big help already. I've got some questions for ya. I am 195#, and plan on taking 200 mg in evening and 200mg before bed. I also plan on taking pyruvate and glycerol (via your recommendation). I'll going to use a 8on/8off cycle.
      1) Should I attempt to lift while on dnp?
      Sure.

      2) What dosage glycerol and pyruvate do you reccommend?
      3 tablspoons a day on the G and 3g of the P

      3) You said that you experienced an anabolic "burst" directly after coming off of dnp. Could this be contributed to your muscles reglycogenating themselves?
      No, because I didn?t really get pumped, but strength went up.

      or do you feel that this is genuine protein synthesis?
      Yes, or nerve excitation/generation or a return of T3. Let me explain the nerve generation in more detail for a moment. When you do strength exercises of 5 reps or less you are training the nerves to fire more muscle cells and to fire those muscle cells in the sequence you want. Now, if we add DNP we are exhausting our muscle cells and they can?t fire as strongly. Result? Your nervous system trains more nerves to fire other muscle cells which had previously gone un or underused when energy stores were high. You are getting a nerve training session due to exhaustion! The more I think about it the more it is like those overtraining programs where you overtrain for a week and you get a rebound. That is what is happening except you are overtraining at the same weights due to the DNP.
      Hehe. It is called overcompensation training and I?ll take it!


      A user:
      Found some info 'bout DNP "With even a low dosage, in the area of 3?5 mg/kg of body weight a day, it will rate your metabolic rate 30%. If this dosage is continued daily, it will raise your metabolism by 50%. At this rate you can burn about 1 lb. of fat a day."

      Animal:
      Now, let's think about this for a second. If metabolism can go from 30?50% that means there is a residual amount left over from the previous dose and therefore the 36hour clearance dosing schedule which I recommend. Furthermore, when I overdosed on 800mg I sweat for OVER 48 hours so this tells me that the half-life can be even longer in some circumstances. It is, nonetheless, up to you as to how you want to take it. If every 24 hours is tolerable for you, then do it.

      A user:
      That's not what I've noticed. At present I'v even gained some weight. I'm 98 kg now. I don't look a bit harder but maybe I shouldn't expect that after only 4 days.
      You WILL hold onto to water! You WILL be depleting carbs from the muscle that will make you look flat! Most WILL NOT notice the benefits until a week or two later upon cessation of DNP. Some see benefits right away, but they appear to already have a bodyfat below 10%.

      A speculator wrote:
      For a person that is highly active and on a calorie restricted diet, DNP will deplete ATP within a matter of days. When this happens your body temperature will go back to normal. The only thing you can do at this point is supplement with in the dosage area of about 150 mcg/day."

      Animal:
      Believe me, you will feel wasted (tired) and LOSE muscle on the regimen and the liver does not control oxidative phosphorylation in every cell. You will still be hot regardless of your T3 levels.


      Question:
      Won't the conversion of T4-T3 come back and function again after discontinuing DNP administration?

      Animal
      Yes, and as long as you do some carbs at 600g a day for three days after.

      Or do I have to look to get T3 as well?
      Animal
      Not really, if ATP was being ever totally depleted you would be cramping. Lack of ATP generation happens when you are what? DEAD!!!!!! It is called rigomortis and if people who write right about DNP had an education or an inkling about body chemistry and process they would know this! Total ATP depletion resulting in death of the cell is not possible. There is some safety mechanism and I imagine it is via the fat cells, but you will not deplete your ATP unless you are an anorexic or dead.

      User:
      And isn't a total lack of ATP what we want, so we can start burning fat instead of ATP?
      Animal:
      Wrong and this is not your fault, but again those who claim to be experts who are dispensing such disinformation. Once the ATP to ADP and to AMP is changed below a certain amount the cell gets it energy from another source which would be the fat. You are looking to burn the glycogen and then the fat is used. This does not mean ATP is gone!

      Why is thermogenesis stopped if there isn't any ATP?
      Animal:
      Read above and it is never stopped. DNP NEVER stops working unless the proton gradient is severely altered. Even in such a case, parts of the mitochondria can have one direction of proton gradient while another section can have a DIFFERENT proton flow!

      User:
      Is this why you want a break after one week? To load up with ATP so thermogenesis can start again?
      Animal:
      No, so you don't feel like **** all the time and so you can get the liver converting T4-T3 again

      Is a one?week?break enough? Or maybe too short if I'm in a hurry.
      You could do DNP for 2 weeks or more if you want.

      Wouldn't it be enough just to discontinue the DNP?cycle to let the liver start converting T4 to T3?
      That is why you stop after a week!

      Where are ATP?molecules stored?
      In and/around the mitochondria and in the cytosol of the cell and ATP is attached to certain enzymes waiting for activation.

      How much ATP do we have in storage?
      That is a major calculation and I haven't looked for an answer, but I don?t think it is important as you can never get rid of all of it.

      A speculator:
      "The administration of DNP, at a dose of 3.5 mg per kilo, increases the total production of heat by about 40%, from the 3rd or 4th day. This increase of the metabolism is due MOSTLY to an increase in the combustion of the fat and a LITTLE to combustion of carbohydrates."
      Any comments on this?
      Animal:
      Again, you are seeing a residual affect. The molecules that the mitochondria use for production of ATP can come from carbs or fat, but the important part is that it is not from muscle.

      Another fact found in the same report as above:
      "In prolonging the administration of the medication, one observes an increase of the tolerance of carbohydrates."
      Does this mean we get increased insulin?sensitivity?
      That is a weird sentence and I don't know what it means, but I think it means you will be more receptive to carbs. You now have increased your insulin sensitivity and this could explain the DNP users? craving for carbs while using DNP.
      .
      So when I eat carbs (I've noticed that I start to sweat then) the body starts burning fat?
      No, the body burns excess ATP and food intake itself is thermogenic.

      Why simple sugars? That means I should walk around eating candy all day?
      Candy is not really a simple sugar as it usually has fat or fructose with it.
      You want a simple sugar every so often to get some insulin rise and some fructose will help recarb the liver as fructose is about 4 times better at recarbing the liver than glucose. Glucose is, BTW, 2 times at good at recarbing muscle when compared to fructose.

      What happens with the carbs?
      They are burned and insulin release and helps change charge on the cells.

      Insulin is secreted. I've noticed that. (If it wouldn't I'd go glucose?high?'n?crazy.) Do I store carbs as glycogen?
      AHAHA! So much for the speculators that say you have to do insulin!
      You won't have time to make glycogen and the glucose will go right to ATP production.

      What about cataracts and skin lesions?
      That is a long term chronic dose situation and why you take pyruvate.

      Have you noticed anything?
      Yes, your sweat smells bad, but no lesions. Another reason you want simple sugars or insulin is that DNP starts to make your vision blurry if you are on a low carb diet.
      COC RULES: https://brotherhoodofpain.com/anabolic-ster...e-conduct.html

      e-mail: [email protected]

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      Analysis of someone else?s recommendations:

      Comment
      After 7 days, DNP dislodges T4 off the carrier proteins, allowing the T4 to be excreted rapidly.


      THIS IS A FUNCTION OF THE PRESENCE OF ATP. END OF DISCUSSION! This has been proven with many people who have used pyruvate which provides an easily usable energy source. Most users only stay on it 7 days so the point would be moot. Since you have depleted the carbs from the liver you are changing the ability of the liver to change T4 to T3. This happens with ANY diet within 7 days. With DNP you have inhibition of conversion via heat (small factor I believe) and via glycogen depletion. This loss of water due to glycogen depletion changes the osmolarity of the liver cells and inhibits the conversion of T4-T3. Now, with the concomitant loss of water you have a loss of charge which is what we are trying to control with the taurine dosing..

      Comment
      I have used T3, and recorded the average elevated body temperature at day 4 on DNP. After 7 days, the temp will decline, so I use T3 2X a day to restore the elevation.

      Animal.
      Really? Most people, including myself, hardly notice any temperature change. I used T3 at 50mcg up to 100mcg on day 5 and never felt worse or more run down than any other DNP experiments I have done.

      Comment:
      It really doesn't matter how much or how long for the T3, because though excessive?looking, T3 blood level will be normal.

      Animal:
      This is NOT true because people have had their thyroid tested while on DNP and their thyroid levels were sky high. Excess thyroid can be responsible for what when calorie deprived? Muscle breakdown. Carbs are gone due to DNP. Your cells are going to be looking to scavenge energy so they are not going to have any protein synthesis because this requires energy. You are going to be in ketosis which is producing glucagon which is responsible for protein breakdown. You will, therefore, have no insulin which is responsible for anabolism of glycogen. You will have no blood sugar or liver glycogen left. Now what is going to happen?! Muscle breakdown. DNP is carb/fat specific and since there is no glycogen/glucose circulating due to high fat-low carbohydrate diet, where is the energy coming from? Ketones can't be made into carbs and about the only source of carbs you are going to have is the glycerol molecule which results from fat breakdown which is minimal. Now throw your excess T3 on there. Hmmm? Sounds like a recipe for muscle breakdown to me.

      Comment:
      Besdies, you'll get sick before you have to worry of being on T3 so long. Trust me, children: DNP for 7 days, and 7 off. You'll be much healthier.

      Reply.
      I totally disagree! Many of us have permanently lowered body temps due to clen?T3 usage which many of the same moron gurus recommended even when using clen for 2-3 weeks. The thyroid is going to see excess T3 in the blood and do you think it is going to want to produce more T4 and T3 on its own? This is what I really don't like about doing the T3, here. Yea, it is only for a week, but 2 weeks on clen which is not even T3 has ****ed up many of us,. If your theory panned out then why couldn?t we do 1 week AS cycles or why have all the 2x2x2 cycles fallen into the pit of futility? I know we are talking different receptors, but they all still function via the negative feedback system.

      Auxillary



      (Consultation question)
      After this Clen, DNP, and high fat diet experience I'm hoping to be down to around 7%BF. Which would leave me at about 165?170lbs. That is too small for me. I want to go on a cycle after that and try to put on a good 20lbs. I have a great diet for my cycle, so I know if I dont make the 20lbs gain I want its not because of nutrition. ( A problem i seem to always have). I wanted to know your thoughts on a cycle that I could really put on a good 20lbs. I know how much of your gains you keep depends on what you do prevent losses ( example: Clomid, and something to regulate cortisone levels, along with others, I have a gains keeper formula I plan to use). but If I do this I want to keep the majority of my gains. That?s why I wanted to include primo since you usually keep what you gain from primo.

      Answer
      Yea, but you don?t gain much and Eq or ganabol would be better as would fina.

      Can you think of a good combo to add to primo for permanent MASS gains?????
      Answer
      Test (Tp, Tc, Te) or a trenbolone (fina, anibolan, parabolan). D-bol then fina always works nicely, too.

      Maybe deca and sustanon or deca and omandren????
      Answer:
      Wouldn?t go with deca and sus and omna are more or less the same.

      Any other s??? ? I have heard if you want to keep gains tests are not good to use
      (enthanate, cyp etc.)
      Answer:
      BS. You have to know how to come off and not overtrain as you are coming off. Think about it. You have gotten stronger which is a result of nerve training. Now if you lift and let your muscles recover longer when off the AS you won?t lose your size!

      . Do I have to take insulin while on DNP if I am taking equipoise and finaplix?
      Answer:
      No, not really and not if you are going to stay on only for a week at about 400mg or less DNP dose.

      Do I have to take cytomel, clen or ECA stack while on DNP?
      Answer:
      I would take EC, but do the others after being careful to note that Clen and T3 will suppress your natural T3. Would be better to throw in tyramine and yohimbine or mazindol.

      I have quite a bit of clen, and cytomel, but no ephedrine.
      Answer:
      You can sub in PPA or adipokinetix or pyruvate or nicotine or mazindol.
      ( I have never had a problem doing nicotine as a chew or as cigars and then quitting, but this is obviously not for all)

      I didn't understand if you said whether or not to start with a low dosage of DNP or not.
      Answer:
      I would if you have never done it before just to see what your tolerance is.

      Question:
      Also, you told me that I should not take cytomel while I am using> the DNP but to use it after the DNP. I was under the impression that DNP suppresses the thyroid and that I should use the cytomel while using the DNP so I will keep burning fat. Would you please explain this to me?

      Answer:
      DNP alters the blood and liver glucose levels and THIS is what keeps the liver from converting T4?T3. If you eat normally this won't happen so drastically and T3 will return to normal soon after stopping DNP. Now, if you have low Blood sugar levels and you add T3 you are going to lose muscle as well as is seen in people that are on low calorie diets who supplement T3. T3 without the right energy and hormones stores is disastrous to muscle.

      Other dieting stuff

      ketotifen and upgrade of clen receptors, but you need 10 1mg tabs of ketotifen a day which will make you hungry and sleepy.

      I was thinking of the efficacy or more like the ?sense of adding t3 toDNP.
      Well, if you are adding-T3 you are going to have a lot of T4 AND T3 floating around and the thyroid is going to read that as an exess and shut down T3 and T4 production.

      Other cycles for DNP use

      Why not do DNP in even smaller doses like that of ephedrine up to 100mg or so?. It will speed up the metabolism and cause a loss of weight without all the discomfort and t4-t3 conversion shutdown. Furthermore, by speeding up the metabolism it may help upgrade steriod receptors and clen receptors with much less discomfort for the user.
      DNP seems to upgrade clen receptor sites as well as steroid receptor sites.
      The rebound for the AS upgrade is only known from anecdotal feedback from myself and others, but if you increase the metabolism of the cell it only stands to reason that you are going to decrease the time it takes to regenerate the receptor sites. The ATP depletion and opening of ATP channels is also likely to be playing a part in these benefits as well, but that is research that probably won?t be done. So the channel part in the upgrade is just speculation.

      Some may need to build?up the dose to start. I had to do it for 3 days and then do 800mg before I started to sweat like a pig for 2 days! Now moderate doses of 200mg make me sweat although not to the same extent, but at least I know I?ve taken it. Kinda like bee stings. You don't have any allergic reaction until one sting and then you get the benefits (problems) from one sting. I do know of a case with a women that had similiar results and said it wasn't working and even talked to w8 about it, but then she ordered more so this has to be what the problem was/is.


      Response to someone that was throwing up and nauseated from DNP use.

      You have low blood sugar!
      This is a classic symptom which can occur with diabetics who use too much insulin. When I use too much insulin and then ride too soon after I would see spots. DNP caused me to see spots as well. DNP depletes all your blood sugar and glycogen first and this will give you low blood sugar, nausea, etc. That is why you want to get your insulin up with glucose once or twice a day on DNP and DO NOT do high fat diets on DNP. W8 will disagree with me on this, but when you look at the actions happening at the liver you will realize that high fat diets just extenuates the slowdown of T4 to T3 conversion.


      Q: But when I?m off I?m gonna keep carbs almost non-existant to burn more fat, and take Adipokinetix to avoid a rebound off of the DNP.
      A: DNP stops conversion of T4-T3 due to carb depletion so you may not want to do that although the Adipo is good. DNP, Adipo, clen, ECA, DNP would be a good way to go or do the clen right before a week of DNP, but only for a week.


      Q: IM OFF MY CYCLE IN AWEEK. THEN IM GONNA TAKE CLOMID, PS,NOLVADEX, TO AVOID A LOSS INGAINS. THEN ITS CUTTING TIME.
      A: Nolvadex and clomid are redundant, do one or the other. PS sucks, but if you already have it, then use it.


      Good things about DNP:

      Biological Study of Dinitro Drugs in Humans
      By Dr. Jacques Bell
      Translation Copyright 1996 Robert Ames

      There is a fundamental difference between biological experimentation with dinitrophenol in humans and what was done in the laboratories of physiologists. These last are essentially interested in hyperthermia (Andre Mayer,Leon Binet, etc.). Yet, in medicine, the doses of dinitrophenol employed do not determine any elevation of temperature. The physiological effects, observed in these conditions, differ considerably from those made by the experimenter. It is thus for example that the animal in hyperthermia presents a polypnoea [rapid, shallow breathing], a hyperglycemia, a hypoglobulinemia that one does not observe with therapeutic doses; it is because experimental hyperthermia is essentially a combustion of carbohydrates, while therapeutic hypermetabolism is
      mainly a combustion of lipids, as is shown by the lowering of respiratory quotient.




      Part 3
      One shouldn't be surprised at these differences. The clinician uses strychnine as a tonic; the experimenter employs it to cause convulsions. The clinician uses adrenaline, at titrated doses, to produce a manageable hypertension; the physiologist, with massive doses causes acute edema of the lung.
      Yet, to base the clinical use of adrenaline or of strychnine on acute edema of the lung or experimental convulsions, constitutes an obvious error. It is the same for dinitrophenol.

      In France, besides, one uses almost exclusively dinitrophenyl?lysidine, which, according to the same terms of the study made by Professor Pouchet, "is easy to purify by crystallization, to easily modify the first of its components from the point of view of toxicity, dissolves easily in water, and, by addition of the methylglyoxalidine (lysidine)group, favors energetically the elimination of waste."

      After Professor Pouchet, we have, in our thesis [1], demonstrated the superiority of this last product; in what follows, it is by comparison with him that we will study the biology of the dinitro drugs.


      We shall see, in order:

      I. Their action on the basal metabolism,
      II. Their visceral action,
      III. Their nutritional action.

      I. ACTION ON BASAL METABOLISM

      After the experimental research of Magne, Mayer and Plantefol, in animals, the experiments of Cutting and Tainter has confirmed, in humans, that dinitrophenol is a drug which strongly increases the metabolism, exaggerating the oxidation process of the organism by direct action on the cellular metabolism. These authors have observed a rise of close to 20% after one hour, being able to attain 70% in ten hours and a tendency to return to normal at 24 hours if the administration of the medicine is not continued.

      This increase is not due to a sympathetic deregulation. The dinitro treatment respects the autonomic nervous system, in an inverse way from thyroxine, which, at slimming doses, determines rapidly some tremors, insomnia, and a mental instability of the type "basedowien." [a thyroid illness where one secretes too much thyroid hormones]

      In the thyroid illnesses, or the thyroid treatments, there is an inverse connection between the level of the basal metabolism and that of blood cholesterol, this being as much lower as the metabolism is higher. One doesn't observe similar phenomena in the course of dinitro treatment.
      This fact indicates that the changes caused in the blood cholesterol in the course of thyroid treatment are directly linked with the thyroid medication and not at all to do with the elevation of the metabolism which is responsible for the reduction of obesity. Dinitrophenol has almost no action on the blood cholesterol. (Grant and Schube).

      An attentive exploration of the nutritional changes in the course of dinitro treatment, in the cases of five obese women, has shown the following facts:

      1. The administration of dinitrophenol, at a dose of 3.5 mg per kilo, increases the total production of heat by about 40%, from the 3rd or 4th day.

      2. This increase of the metabolism is due mostly to an increase in the combustion of the fat and a little to combustion of carbohydrates.

      3. Dinitrophenol does not attack cell tissue albumin and does not determine the fat loss to the expense of the muscles, contrary to thyroxine.

      II. VISCERAL ACTION

      Dinitro treatment respects the liver, the kidneys, the cardio?vascular system and the blood.

      This innocuity for the principal visceral functions is without doubt one of the main reasons for the distribution of this therapy.
      Tainter, Stockton and Cutting have reported a series of cases in which one had measured the plasma bile index and determined the test of Van de Bergh. Their analyses demonstrate, beyond a doubt, that the liver does not suffer any damage in the course of dinitro treatment.

      Experimental studies on animals do not show toxic effects of dinitrophenol on the kidney (Taitner, Cutting, Woodand Proescher). Anatomical?pathological examinations of animals, even those which died from a massive dose of dinitrophenol, do not reveal any important anatomical changes, except a small degree of cytolysis. Clinical documents are not abundant, but, on the whole, do not seem to demonstrate that dinitrophenol is toxic for the kidneys.

      As T.L. Schulte and M.L. Tainter wrote, "it doesn't seem that dinitrophenol at usual clinical doses is likely to harm the kidneys."

      Dinitrophenol is remarkable for its absence of effect on the cardio?vascular system. Even when the basal metabolism is found elevated to significant levels, there is no change in the rhythm of the pulse (Rosenblum).

      On this point, dinitrophenol differs from all the other metabolic accelerants known. It is an observation that all the clinicians, today, have had occasion to make.

      All the clinicians know that, contrary to thyroxine, dinitrophenol is absolutely devoid of toxicity for the heart.

      The research of Professor Loeper and of his students has demonstrated the physiological and clinical importance of myocardiac glycogen. Extensive studies by P.N. Taussig have shown that dinitrophenol does not reduce cardiac glycogen at all and that, on this point, it differs completely from thyroxine.

      III. ACTION ON NUTRITION

      The influence of dinitro therapy on nutrition has been the object of a very important clinical study.

      "One does not observe variations in the elimination of chlorine; eliminated phosphorus varies sometimes more, sometimes less, the elimination of sulphur increases slightly, especially in the form of sulphur conjugates, urines show a small increase of total nitrogen and of urea." (Prof. Pouchet).

      It is a well known fact that the administration of thyroid extract or hyperthyroidism is accompanied by an increased secretion of calcium and of phosphorus. This calcium and phosphorus in the urine are not due to the acceleration of metabolism, as one does not observe these facts either during fever, nor in the course of leukemias which raise the metabolism (J.C. Aub, N.B. Bauer, C.I. Heath, Alright, Bauer and Aub).

      Thyroxine reduces bone density.

      With dinitrophenol, nothing of the sort is observed. The experiments of Clarence L. Robbins show that dinitrophenol, in spite of the elevation of the metabolism that it produces, does not cause any increase of the loss of calcium or of phosphorus. An increase of 37% in the basal metabolism, caused by the ingestion of dinitrophenol, does not lead to modification in the excretion of these elements.

      In normal individuals, when one administers dinitrophenol during a short period, it produces a small elevation of reduced substances in the blood after fasting (although one would not be able to call this hyperglycemia). When one administers the medication over a longer period, this phenomenon is not produced and there is a marked elevation of the tolerance to carbohydrates.

      In diabetics, following treatments of short duration, the results are variable, the tolerance to glucose being as often increased as it is decreased, with parallel changes in the fasting blood sugar level. But, in prolonging the administration of the medication, one observes an increase of the tolerance of carbohydrates. Anyway, in basing himself on the study of 32 cases of diabetes, Simkins concludes that dinitrophenol is not toxic for diabetics. Here marks that this observation goes counter to some assertions that have been a little prematurely advanced.

      Dinitrophenyl?lysidine at therapeutic doses therefore has an action on the organism which is completely physiological. This action has been demonstrated in obesity where it has been compared to the actions of thyroid medication and physical exercise.

      The existence of obesities of glandular origin, especially by thyroid insufficiency, has resulted in the use of thyroxine in numerous subjects.

      "This wasn't without inconveniences, sometimes grave, characterized especially by cardiac and nervous troubles; the effective dose of thyroxine is, in fact, very close to the toxic dose. Further, we has frequently seen these accidents persisting after the administration even of a single dose, which leads to the impossibility of stopping them immediately by a simple suspension of the medication. Yet, from the point of view of its specific action on the basal metabolism, dinitrophenol offers this precious advantage that the cessation of its use at the slightest appearance of signs indicating an imminence of intoxication results immediately in the arrest of those symptoms."
      (Professor Pouchet).

      Finally, thyroxine causes a nitrogen malnutrition: it burns the muscle and fatigues the heart.
      Dinitrophenol?lysidine, to the contrary, causes a lipid?glycemic loss: it is the elimination of reserve materials without attacking visceral and muscle tissue.

      As for physical exercise, it seems to act exactly like dinitro therapy. Marcowitz, in his communication to the Academy of Medicine of Toronto on October 9, 1934, based on 90 cases of obesity, having followed this treatment during a period of 16 months, concludes that its action may be succinctly described in saying that the effects on the organism are similar to those of physical exercises.

      The fact is besides established by physiologists, since dinitrophenol raises thermogenesis and not the metabolic quotient.

      All the clinicians know actually that dinitro medication is irreplaceable in cases of monstrous obesities which prevent all exercise. It can be used in the obese for whom occupations, life style or cardiac troubles do not permit physical exercises. It is indispensible for the grossly obese in cases of abdominal operations and immobilization due to illness (inflammation of fallopian tubes, appendicitis, etc.) for which there is an urgency to obtain a reduction of subcutaneous fat.

      But this clinical use has not been able to be extended other than when the experimental research pursued on humans, with a dinitro drug free from impurities, has been able to demonstrate the biological effects of it in a very precise way.

      Studies to ponder which helps you see where my answers have come from

      All about DNP : Animal's manuel (continued)


      Here is why you need to eat a regular diet:

      Subject: DNP, Insulin, and ATP?sensitive Potassium channels

      [Some of the following is speculative. Caveat lector.]
      Ion channels are membrane proteins that control the flux of ions across an otherwise impermeable cell membrane. Potassium(K) channels were first decribed by Noma [1] in 1983, and later in 1991 the ATP?sensitive K channel (KATP) was described by the same researcher [2]. Potassium channels determine cell membrane potential.

      KATP channels exist in most excitable cells. They are regulated by the intracellular level of ATP as well as by various nucleotide diphosphates, pH and lactate concentrations. The activity of KATP channels is inhibited by increasing the intracellular ATP concentration. Closure of these channels in response to glucose metabolism depolarizes the cell, stimulating voltage?dependent electrical activity, and calcium ion (Ca) entry. In the pancreatic beta cells, an increase in blood sugar level leads to an elevated ATP/ADP ratio, which in turn inhibits KATP channels, so as to alter the membrane potential and cause insulin release. It is accompanied by increases in respiratory rate, pyridine and flavin nucleotide reduction state, and intracellular pH [3].
      Thus, the KATP channel couples nutrient metabolism to the membrane potential.

      o Increase in blood glucose ?> increase in glucose metabolism ?> increase in intracellular ATP ?> inhibition of KATP channel.

      o Channel CLOSED: cell depolarized, Ca++ uptake, insulin exocytosis.

      KATP channels play an important role in the control of vascular tone [4]. Polarization following potassium channel activation
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      Biological Study of Dinitro Drugs in Humans

      By Dr. Jacques Bell
      Bell, Jacques. 1939. Etude biologique des produits dinitres chez l'homme. Medecine. 19:749-54.
      Translation � 1996 Robert Ames


      After Professor Pouchet, we have, in our thesis [1], demonstrated the superiority of this last product; in what follows, it is by comparison with him that we will study the biology of the dinitro drugs.
      We shall see, in order:
      I. Their action on the basal metabolism,
      II. Their visceral action,
      III. Their nutritional action.

      I. ACTION ON BASAL METABOLISM
      After the experimental research of Magne, Mayer and Plantefol, in animals, the experiments of Cutting and Tainter has confirmed, in humans, that dinitrophenol is a drug which strongly increases the metabolism, exaggerating the oxidation process of the organism by direct action on the cellular metabolism. These authors have observed a rise of close to 20% after one hour, being able to attain 70% in ten hours and a tendency to return to normal at 24 hours if the administration of the medicine is not continued.
      This increase is not due to a sympathetic deregulation. The dinitro treatment respects the autonomic nervous system, in an inverse way from thyroxine, which, at slimming doses, determines rapidly some tremors, insomnia, and a mental instability of the type "basedowien." [a thyroid illness where one secretes too much thyroid hormones]

      In the thyroid illnesses, or the thyroid treatments, there is an inverse connection between the level of the basal metabolism and that of blood cholesterol, this being as much lower as the metabolism is higher. One doesn't observe similar phenomena in the course of dinitro treatment.

      This fact indicates that the changes caused in the blood cholesterol in the course of thyroid treatment are directly linked with the thyroid medication and not at all to do with the elevation of the metabolism which is responsible for the reduction of obesity. Dinitrophenol has almost no action on the blood cholesterol. (Grant and Schube).

      An attentive exploration of the nutritional changes in the course of dinitro treatment, in the cases of five obese women, has shown the following facts:

      1. The administration of dinitrophenol, at a dose of 3.5 mg per kilo, increases the total production of heat by about 40%, from the 3rd or 4th day.

      2. This increase of the metabolism is due mostly to an increase in the combustion of the fat and a little to combustion of carbohydrates.

      3. Dinitrophenol does not attack cell tissue albumin and does not determine the fat loss to the expense of the muscles, contrary to thyroxine.

      II. VISCERAL ACTION
      Dinitro treatment respects the liver, the kidneys, the cardio-vascular system and the blood.

      This innocuity for the principal visceral functions is without doubt one of the main reasons for the distribution of this therapy.
      Tainter, Stockton and Cutting have reported a series of cases in which one had measured the plasma bile index and determined the test of Van de Bergh. Their analyses demonstrate, beyond a doubt, that the liver does not suffer any damage in the course of dinitro treatment.

      Experimental studies on animals do not show toxic effects of dinitrophenol on the kidney (Taitner, Cutting, Wood and Proescher). Anatomical-pathological examinations of animals, even those which died from a massive dose of dinitrophenol, do not reveal any important anatomical changes, except a small degree of cytolysis. Clinical documents are not abundant, but, on the whole, do not seem to demonstrate that dinitrophenol is toxic for the kidneys.

      As T.L. Schulte and M.L. Tainter wrote, "it doesn't seem that dinitrophenol at usual clinical doses is likely to harm the kidneys."
      Dinitrophenol is remarkable for its absence of effect on the cardio-vascular system. Even when the basal metabolism is found elevated to significant levels, there is no change in the rhythm of the pulse (Rosenblum).

      On this point, dinitrophenol differs from all the other metabolic accelerants known. It is an observation that all the clinicians, today, have had occasion to make.

      All the clinicians know that, contrary to thyroxine, dinitrophenol is absolutely devoid of toxicity for the heart.

      The research of Professor Loeper and of his students has demonstrated the physiological and clinical importance of myocardiac glycogen. Extensive studies by P.N. Taussig have shown that dinitrophenol does not reduce cardiac glycogen at all and that, on this point, it differs completely from thyroxine.

      III. ACTION ON NUTRITION
      The influence of dinitro therapy on nutrition has been the object of a very important clinical study.

      "One does not observe variations in the elimination of chlorine; eliminated phosphorus varies sometimes more, sometimes less, the elimination of sulphur increases slightly, especially in the form of sulphur conjugates, urines show a small increase of total nitrogen and of urea." (Prof. Pouchet).

      It is a well known fact that the administration of thyroid extract or hyperthyroidism is accompanied by an increased secretion of calcium and of phosphorus. This calcium and phosphorus in the urine are not due to the acceleration of metabolism, as one does not observe these facts either during fever, nor in the course of leukemias which raise the metabolism (J.C. Aub, N.B. Bauer, C.I. Heath, Alright, Bauer and Aub).

      Thyroxine reduces bone density.
      With dinitrophenol, nothing of the sort is observed. The experiments of Clarence L. Robbins show that dinitrophenol, in spite of the elevation of the metabolism that it produces, does not cause any increase of the loss of calcium or of phosphorus. An increase of 37% in the basal metabolism, caused by the ingestion of dinitrophenol, does not lead to modification in the excretion of these elements.

      In normal individuals, when one administers dinitrophenol during a short period, it produces a small elevation of reduced substances in the blood after fasting (although one would not be able to call this hyperglycemia). When one administers the medication over a longer period, this phenomenon is not produced and there is a marked elevation of the tolerance to carbohydrates.

      In diabetics, following treatments of short duration, the results are variable, the tolerance to glucose being as often increased as it is decreased, with parallel changes in the fasting blood sugar level. But, in prolonging the administration of the medication, one observes an increase of the tolerance of carbohydrates. Anyway, in basing himself on the study of 32 cases of diabetes, Simkins concludes that dinitrophenol is not toxic for diabetics. He remarks that this observation goes counter to some assertions that have been a little prematurely advanced.

      Dinitrophenyl-lysidine at therapeutic doses therefore has an action on the organism which is completely physiological. This action has been demonstrated in obesity where it has been compared to the actions of thyroid medication and physical exercise.

      The existence of obesities of glandular origin, especially by thyroid insufficiency, has resulted in the use of thyroxine in numerous subjects.

      "This wasn't without inconveniences, sometimes grave, characterized especially by cardiac and nervous troubles; the effective dose of thyroxine is, in fact, very close to the toxic dose. Further, we has frequently seen these accidents persisting after the administration even of a single dose, which leads to the impossibility of stopping them immediately by a simple suspension of the medication. Yet, from the point of view of its specific action on the basal metabolism, dinitrophenol offers this precious advantage that the cessation of its use at the slightest appearance of signs indicating an imminence of intoxication results immediately in the arrest of those symptoms." (Professor Pouchet).

      Finally, thyroxine causes a nitrogen malnutrition: it burns the muscle and fatigues the heart. Dinitrophenol-lysidine, to the contrary, causes a lipid-glycemic loss: it is the elimination of reserve materials without attacking visceral and muscle tissue.
      As for physical exercise, it seems to act exactly like dinitro therapy. Marcowitz, in his communication to the Academy of Medicine of Toronto on October 9, 1934, based on 90 cases of obesity, having followed this treatment during a period of 16 months, concludes that its action may be succinctly described in saying that the effects on the organism are similar to those of physical exercises.

      The fact is besides established by physiologists, since dinitrophenol raises thermogenesis and not the metabolic quotient.

      All the clinicians know actually that dinitro medication is irreplaceable in cases of monstrous obesities which prevent all exercise. It can be used in the obese for whom occupations, life style or cardiac troubles do not permit physical exercises. It is indispensible for the grossly obese in cases of abdominal operations and immobilization due to illness (inflammation of fallopian tubes, appendicitis, etc.) for which there is an urgency to obtain a reduction of subcutaneous fat.

      But this clinical use has not been able to be extended other than when the experimental research pursued on humans, with a dinitro drug free from impurities, has been able to demonstrate the biological effects of it in a very precise way.

      1. La Therapeutique dinitree (J.-B. Bailliere et Fils, editeurs, 1937


      more studies


      ATP-Sensitive Potassium Ion Channels
      Some of the following is speculative. Caveat lector.]
      Ion channels are membrane proteins that control the flux of ions across an otherwise impermeable cell membrane. Potassium (K) channels were first decribed by Noma [1] in 1983, and later in 1991 the ATP-sensitive K channel (KATP) was described by the same researcher [2]. Potassium channels determine cell membrane potential.

      KATP channels exist in most excitable cells. They are regulated by the intracellular level of ATP as well as by various nucleotide diphosphates, pH and lactate concentrations. The activity of KATP channels is inhibited by increasing the intracellular ATP concentration. Closure of these channels in response to glucose metabolism depolarises the cell, stimulating voltage-dependent electrical activity, and calcium ion (Ca) entry. In the pancreatic beta cells, an increase in blood sugar level leads to an elevated ATP/ADP ratio, which in turn inhibits KATP channels, so as to alter the membrane potential and cause insulin release. It is accompanied by increases in respiratory rate, pyridine and flavin nucleotide reduction state, and intracellular pH [3].
      Thus, the KATP channel couples nutrient metabolism to the membrane potential.

      � Increase in blood glucose --> increase in glucose metabolism --> increase in intracell ATP --> inhibition of KATP channel.
      � Channel CLOSED: cell depolarized, Ca++ uptake, insulin exocytosis.

      KATP channels play an important role in the control of vascular tone [4]. Polarization following potassium channel activation (opening) results in lessened calcium influx and smooth muscle relaxation.

      � KATP channel BLOCKED --> vascular tone increases.
      � KATP channel ACTIVATED --> vascular tone decreases.

      Besides being regulated by intracellular signals, potassium channels may also be regulated by membrane potential. Thus, in excitable cells in the heart, muscle, and nervous system, voltage-gated potassium channels are activated during an action potential; the activities of these potassium channels determine to a large extent the shape of the action potential, hence the strength of the signaling.

      � KATP BLOCKED --> more strength
      � KATP ACTIVATED --> less strength

      Drugs which block KATP channels: tolbutamide, glyburide, glibenclamide.

      Drugs which activate KATP channels: Prostaglandin E2 and I2, adenosine, lemakalim.

      Drugs which activate K channels: pinacidil, cromakalim.

      Mitochondria also contain a K+ channel that causes rapid K+ uptake when open [5].

      DNP
      What happens when someone takes the decoupler dinitrophenol (DNP)? Blood glucose will result in increased metabolism, but the level of ATP in the cell does not increase! In fact, it is depleted. So in this case, the KATP channel is not inhibited, and it stays open. Calcium is not taken into the cell, and insulin is not released. The person taking DNP has in effect given himself temporary diabetes.
      Insulin is needed to facilitate the uptake of glucose into cardiac, skeletal, and adipose tissue, and to convert glucose to glycogen in the liver. It is anti-proteolytic and protects against the various ailments commonly seen in diabetics, such as vision problems and polyneuropathy. Not coincidentally, the same problems can result from ingesting DNP.

      This is why, when one takes DNP, one also needs to take exogenous insulin.

      Since the KATP channel remains open, vascular and muscular tone relax. Probably blood pressure will decrease. Strength will diminish.

      It would seem that an antidote for DNP might be anything that causes the KATP channel to close, for example the drug glibenclamide.

      References
      1. Noma A. 1983. Nature 305: 147.
      2. Noma A, Takano M. 1991. The ATP-sensitive K+ channel. Jpn J Physiol 41(1):77-87.
      3. Civelek VN, Deeney JT, et al. 1996. Temporal sequence of metabolic and ionic events in glucose-stimulated clonal pancreatic-cells. Biochem. J. 315: 1015-1019. Boston University Medical Center.
      4. Nichols, C.G. and Lederer, W.J. 1991. ATP-sensitive potassium channels in the cardiovascular system. American Journal of Physiology 261:H1675-H1686.
      5. Paucek, P, Mironova, G, et al. 1992 "Reconstitution and partial purification of the glibenclamide-sensitive, ATP-dependent K+ channel from rat liver and beef heart mitochondria," J. Biol. Chem. 267, 26062.
      6. Nakamura S. 1989. Glucose reverses DNP induced changes in action potentials. Cardiovascular Res. 23(4):286-294.
      ----------------------------------------------------------------------------------

      Biological Study of Dinitro Drugs in Humans
      By Dr. Jacques Bell
      Bell, Jacques. 1939. Etude biologique des produits dinitres chez l'homme. Medecine. 19:749-54.
      Translation � 1996 Robert Ames
      There is a fundamental difference between biological experimentation with dinitrophenol in humans and what was done in the laboratories of physiologists. These last are essentially interested in hyperthermia (Andre Mayer, Leon Binet, etc.). Yet, in medicine, the doses of dinitrophenol employed do not determine any elevation of temperature. The physiological effects, observed in these conditions, differ considerably from those made by the experimenter. It is thus for example that the animal in hyperthermia presents a polypnoea [rapid, shallow breathing], a hyperglycemia, a hypoglobulinemia that one does not observe with therapeutic doses; it is because experimental hyperthermia is essentially a combustion of carbohydrates, while therapeutic hypermetabolism is mainly a combustion of lipids, as is shown by the lowering of respiratory quotient.
      One shouldn't be surprised at these differences. The clinician uses strychnine as a tonic; the experimenter employs it to cause convulsions. The clinician uses adrenaline, at titrated doses, to produce a manageable hypertension; the physiologist, with massive doses causes acute edema of the lung.
      Yet, to base the clinical use of adrenaline or of strychnine on acute edema of the lung or experimental convulsions, constitutes an obvious error. It is the same for dinitrophenol.
      In France, besides, one uses almost exclusively dinitrophenyl-lysidine, which, according to the same terms of the study made by Professor Pouchet, "is easy to purify by crystallization, to easily modify the first of its components from the point of view of toxicity, dissolves easily in water, and, by addition of the methylglyoxalidine (lysidine) group, favors energetically the elimination of waste."

      After Professor Pouchet, we have, in our thesis [1], demonstrated the superiority of this last product; in what follows, it is by comparison with him that we will study the biology of the dinitro drugs.
      We shall see, in order:
      I. Their action on the basal metabolism,
      II. Their visceral action,
      III. Their nutritional action.

      I. ACTION ON BASAL METABOLISM
      After the experimental research of Magne, Mayer and Plantefol, in animals, the experiments of Cutting and Tainter has confirmed, in humans, that dinitrophenol is a drug which strongly increases the metabolism, exaggerating the oxidation process of the organism by direct action on the cellular metabolism. These authors have observed a rise of close to 20% after one hour, being able to attain 70% in ten hours and a tendency to return to normal at 24 hours if the administration of the medicine is not continued.
      This increase is not due to a sympathetic deregulation. The dinitro treatment respects the autonomic nervous system, in an inverse way from thyroxine, which, at slimming doses, determines rapidly some tremors, insomnia, and a mental instability of the type "basedowien." [a thyroid illness where one secretes too much thyroid hormones]

      In the thyroid illnesses, or the thyroid treatments, there is an inverse connection between the level of the basal metabolism and that of blood cholesterol, this being as much lower as the metabolism is higher. One doesn't observe similar phenomena in the course of dinitro treatment.

      This fact indicates that the changes caused in the blood cholesterol in the course of thyroid treatment are directly linked with the thyroid medication and not at all to do with the elevation of the metabolism which is responsible for the reduction of obesity. Dinitrophenol has almost no action on the blood cholesterol. (Grant and Schube).

      An attentive exploration of the nutritional changes in the course of dinitro treatment, in the cases of five obese women, has shown the following facts:

      1. The administration of dinitrophenol, at a dose of 3.5 mg per kilo, increases the total production of heat by about 40%, from the 3rd or 4th day.

      2. This increase of the metabolism is due mostly to an increase in the combustion of the fat and a little to combustion of carbohydrates.

      3. Dinitrophenol does not attack cell tissue albumin and does not determine the fat loss to the expense of the muscles, contrary to thyroxine.

      II. VISCERAL ACTION
      Dinitro treatment respects the liver, the kidneys, the cardio-vascular system and the blood.

      This innocuity for the principal visceral functions is without doubt one of the main reasons for the distribution of this therapy.
      Tainter, Stockton and Cutting have reported a series of cases in which one had measured the plasma bile index and determined the test of Van de Bergh. Their analyses demonstrate, beyond a doubt, that the liver does not suffer any damage in the course of dinitro treatment.

      Experimental studies on animals do not show toxic effects of dinitrophenol on the kidney (Taitner, Cutting, Wood and Proescher). Anatomical-pathological examinations of animals, even those which died from a massive dose of dinitrophenol, do not reveal any important anatomical changes, except a small degree of cytolysis. Clinical documents are not abundant, but, on the whole, do not seem to demonstrate that dinitrophenol is toxic for the kidneys.

      As T.L. Schulte and M.L. Tainter wrote, "it doesn't seem that dinitrophenol at usual clinical doses is likely to harm the kidneys."
      Dinitrophenol is remarkable for its absence of effect on the cardio-vascular system. Even when the basal metabolism is found elevated to significant levels, there is no change in the rhythm of the pulse (Rosenblum).

      On this point, dinitrophenol differs from all the other metabolic accelerants known. It is an observation that all the clinicians, today, have had occasion to make.

      All the clinicians know that, contrary to thyroxine, dinitrophenol is absolutely devoid of toxicity for the heart.

      The research of Professor Loeper and of his students has demonstrated the physiological and clinical importance of myocardiac glycogen. Extensive studies by P.N. Taussig have shown that dinitrophenol does not reduce cardiac glycogen at all and that, on this point, it differs completely from thyroxine.

      III. ACTION ON NUTRITION
      The influence of dinitro therapy on nutrition has been the object of a very important clinical study.

      "One does not observe variations in the elimination of chlorine; eliminated phosphorus varies sometimes more, sometimes less, the elimination of sulphur increases slightly, especially in the form of sulphur conjugates, urines show a small increase of total nitrogen and of urea." (Prof. Pouchet).

      It is a well known fact that the administration of thyroid extract or hyperthyroidism is accompanied by an increased secretion of calcium and of phosphorus. This calcium and phosphorus in the urine are not due to the acceleration of metabolism, as one does not observe these facts either during fever, nor in the course of leukemias which raise the metabolism (J.C. Aub, N.B. Bauer, C.I. Heath, Alright, Bauer and Aub).

      Thyroxine reduces bone density.
      With dinitrophenol, nothing of the sort is observed. The experiments of Clarence L. Robbins show that dinitrophenol, in spite of the elevation of the metabolism that it produces, does not cause any increase of the loss of calcium or of phosphorus. An increase of 37% in the basal metabolism, caused by the ingestion of dinitrophenol, does not lead to modification in the excretion of these elements.

      In normal individuals, when one administers dinitrophenol during a short period, it produces a small elevation of reduced substances in the blood after fasting (although one would not be able to call this hyperglycemia). When one administers the medication over a longer period, this phenomenon is not produced and there is a marked elevation of the tolerance to carbohydrates.

      In diabetics, following treatments of short duration, the results are variable, the tolerance to glucose being as often increased as it is decreased, with parallel changes in the fasting blood sugar level. But, in prolonging the administration of the medication, one observes an increase of the tolerance of carbohydrates. Anyway, in basing himself on the study of 32 cases of diabetes, Simkins concludes that dinitrophenol is not toxic for diabetics. He remarks that this observation goes counter to some assertions that have been a little prematurely advanced.

      Dinitrophenyl-lysidine at therapeutic doses therefore has an action on the organism which is completely physiological. This action has been demonstrated in obesity where it has been compared to the actions of thyroid medication and physical exercise.

      The existence of obesities of glandular origin, especially by thyroid insufficiency, has resulted in the use of thyroxine in numerous subjects.

      "This wasn't without inconveniences, sometimes grave, characterized especially by cardiac and nervous troubles; the effective dose of thyroxine is, in fact, very close to the toxic dose. Further, we has frequently seen these accidents persisting after the administration even of a single dose, which leads to the impossibility of stopping them immediately by a simple suspension of the medication. Yet, from the point of view of its specific action on the basal metabolism, dinitrophenol offers this precious advantage that the cessation of its use at the slightest appearance of signs indicating an imminence of intoxication results immediately in the arrest of those symptoms." (Professor Pouchet).

      Finally, thyroxine causes a nitrogen malnutrition: it burns the muscle and fatigues the heart. Dinitrophenol-lysidine, to the contrary, causes a lipid-glycemic loss: it is the elimination of reserve materials without attacking visceral and muscle tissue.
      As for physical exercise, it seems to act exactly like dinitro therapy. Marcowitz, in his communication to the Academy of Medicine of Toronto on October 9, 1934, based on 90 cases of obesity, having followed this treatment during a period of 16 months, concludes that its action may be succinctly described in saying that the effects on the organism are similar to those of physical exercises.

      The fact is besides established by physiologists, since dinitrophenol raises thermogenesis and not the metabolic quotient.

      All the clinicians know actually that dinitro medication is irreplaceable in cases of monstrous obesities which prevent all exercise. It can be used in the obese for whom occupations, life style or cardiac troubles do not permit physical exercises. It is indispensible for the grossly obese in cases of abdominal operations and immobilization due to illness (inflammation of fallopian tubes, appendicitis, etc.) for which there is an urgency to obtain a reduction of subcutaneous fat.

      But this clinical use has not been able to be extended other than when the experimental research pursued on humans, with a dinitro drug free from impurities, has been able to demonstrate the biological effects of it in a very precise way.

      1. La Therapeutique dinitree (J.-B. Bailliere et Fils, editeurs, 1937).

      ---------------------------------------------------------------------------------------------------------------------------------------------------------------------

      Concerning Two Cases of Cataract Caused by Dinitrophenol
      By Jean Sedan (Marseille)
      Sedan, Jean. 1939. A propos de deux cas de cataracte par phenols dinitres. Annales d'Oculistes. 176:191.
      Translation � 1996 Robert Ames

      The implementation of the treatment for obesity by dinitrophenol dates only from 1933, the year when it was suddenly and rapidly put in the limelight by the work of the Americans Tainter, Mehrtens and Cutting.

      These authors have established that the ingestion of dinitrophenol accelerates metabolism, causing a marked elevation in temperature. It seemed that dinitrophenol was a specially effective treatment for obesity. In 1936, Horner estimated that in the first 15 months following the appearance of the medication in the market, one hundred thousand persons used it to lose weight.

      Incidents and accidents multiplied and appeared sufficiently serious that the American Medical Association warned the public against the dangers of unsupervised treatment.

      Here we discuss only the case of cataracts, which Horner had said that it occurs in one case in 1000 treatments. At the end of this report we will note the principle bibliographic references concerning the American literature devoted to the subject and which is of a great value, but we wish to emphasize how the European work and especially French are on the other hand still rare and even exceptional.

      One can say that it is by the work of Onfray and Gilbert Dreyfus presented to the Congress of the S.F.O. [Societe Francaise des Oculistes?] in 1937 that French opthamologists had their attention drawn to the subject. This remarkably precise work is enriched by two observations of which one is due to Doctor A. Gallois, of Besancon. We frequently reference this, for it contains in addition to minutely observed details, important physio-pathogenic considerations and a complete history of the subject.
      Apart from this work, we should also to point out the observations of Van de Hoeve and Polak-Daniels published in Holland in 1936, as well as the French summaries and reviews of Halbron on cataracts and of Laignel-Lavastine on dinitrophenol intoxication.

      Finally, we emphasize the interest of the work of Vogt on the cataracts caused by dinitrophenol in Switzerland and of G. Ciotola of those caused by alphadinitrophenol in Italy, both published in 1937. The same year, Stein and Crevecoeur pointed out that in their opinion this affectation was, when all is said and done, quite rare if one thinks of the enormous dissemination of dinitro treatment. This was also the opinion of Andre Mayer, based on the fact that despite the considerable number of intoxications by dintrophenol observed in munitions factories, no cases of cataracts have been noted.

      Finally, in 1938, Carlotti and Rivoire de Nice presented a case of cataract by dintrophenyl-lysidine which developed "with almost lightning-like rapidity."
      * * *
      It was possible for us to observe two very demonstrative cases. In one there was an arrest of development of opacity after the patient stopped taking dinitrophenol, which is more than a rarity, a real exception in the pathological history of dinitrophenol cataracts.

      OBSERVATION I. -- Mme. K... Lea, 32 years old presented herself to me in December 1937 with a marked lowering of the vision of both eyes, which began a few weeks earlier, developing extremely fast and was all the more disturbing since she works at a very visual profession in the editing of a newspaper and as she is especially partial to this pleasant and remunerative position. I noticed a beginning of bilateral cataract appearing striated and fleecy which is found almost constantly in the description of toxic lens opacities of this kind. The opacity is situated mainly at the level of the equator of the lens, but also involves the posterior part of the central mass. The vision is only 4/10 in the right and 5/10 in the left, these two acuities correctable to 7/10 O.D.G. -- 2.50.

      Mme K... thus learned that she was rapidly becoming myopic.
      The most minute research were done in view of identifying a possible cause of this bilateral cataract. All the blood and urine tests were negative. Very complete clinical examinations by Doctor P..., referring physician, point to the same conclusion that it is impossible to relieve Mmme. K...'s pathological process at all.
      It is then that I thought of asking her about the possibility of a dinitrophenol anti-obesity treatment, even though the corpulence of my client did not seem excessive. She told me then of having taken two pills each day of 0.30 grams of dinitrophenol in series of ten days with a rest of 15 days, for the past year and a half.
      She had, without the least dietary restriction, lost 19 kilograms out of 87 [42 pounds out of 191]. It was at that point that she began complaining about her vision.

      I wasn't aware of the topic at that time except by the short summaries of American works, but I didn't hesitate to warn her against what I considered to be the real origin of her sickness.
      Very anxious about her state, she was easily convinced and stopped that therapy suddenly and definitively.

      I had the opportunity to see her in March, July and October 1938 and I noticed with great interest the complete arrest in the development of these catacts, which accompanied in very precise fashion the progressive and total disappearance of myopia to the extent that although it was possible to note an appreciable modification in the lens opacities, the visual acuity was spontaneously returned to 7/10 (uncorrected) at the end of October 1938.

      We add that Mme. K..., doubly happy, very far from regaining weight in spite of the renunciation of dinitrophenol, had lost another 5 kilos by a very strict nutritional discipline complemented with rigorous gymnastic practices and the introduction into her life of a new intoxification, certainly less dangerous than the preceeding -- tea.

      In this case, the role played by the toxin in the opacification of the lens seems to us demonstrated in an almost experimental fashion by the disappearance of the myopia at the moment of the cessation of the intoxification and even more by the incontestable and enduring stabilization of the state of opacities that maintained itself for six months. In contrast, the development was very sudden in a month before the application of this measure. It is presumed that only the precocity of the requested medical consultation and of the medical diagnostic given, has permitted a stop in the development of this toxic cataract -- a completely unusual phenomenon.

      We emphasize that the treatment had included plainly excessive doses and that however the opacification only appeared late in the treatment. On this topic remember that in the discussion which followed the expose made to the S.F.O. in 1937 by MM. Onfray and Gilbert Dreyfus-Arruga, who had occasion to observe and operate in America [illegible] ... don't generally appear except at the end of many months and even sometimes six to twelve months after the cessation of treatment. These late-developing cataracts are almost always bilateral.

      OBSERVATION II.
      [Not included. Summary: A 32 year old woman weighing 90 kg. (198 pounds) began taking dinitrophenol on February 1st, 1937. She began with 9 to 10 pills daily, each being 30 mg. of DNP. After a week she increased the dose to 12 pills / day (360 mg.). At this dosage she lost 800 grams per week, or 10 kg. (22 pounds) in three months, without changing her diet. She stopped taking DNP for four months and then began again. So she took 32.4 grams of DNP in the first 90 days and the same amount in the second course. American reports indicated that cataracts had resulted from doses as small as 100 mg. per day for a total of 40 grams.

      On June 10th 1938, after several days in a very sunny seaside resort, the patient began to lose vision in her left eye, and on July 12th, the other eye was affected. By August 1st she was unable to see to drive. By September she was blind.
      Fortunately, surgery produced favorable results.]

      It is necessary, indeed, to publicize cases in order to attract the attention of physicians and of the French public to the danger of intoxification by dinitrophenol. The fact that we have been able to stabilize, if not make regress one cataract of this class by stopping all toxic ingestion is but another reason which compels us to make it known.

      These arguments and our observations are so needed to challenge the imagination and influence young women against harmful weight loss techniques that the work appears discouraging.

      Indeed, in ending, we repeat the unlikely remark that our second patient made to us upon taking leave following the success of her first operation: "And now, Doctor, do not oppose my taking of dinitrophenol since I no longer risk having cataracts."
      References

      � ALLEN and BENSON. -- Late development of cataracts following use of dinitrophenol about a year before. JAMA, 1935, V, 105, p. 795.
      � BARKAN, BORLEY, FINE and BETTMAN. -- Operative results in cataracts coincident with dinitrophenol therapy. Cal W. Med. 1936, XXXXIV, p. 360.
      � BENCE, JONES. -- On the rate of passage of crystalloids into and out of the vascular and non-vascular textures of the body. Pr. R. Soc., 1863, London, 14, 400.
      � BOARDMAN. -- Rapidly developing cataracts after dinitrophenol. JAMA, 1935, CV, p. 108.
      � CAMERON, cited by HORNER. -- Arch. of opth. 1936, XVI, p. 452.
      � CARLOTTI and RIVOIRE. -- Sur un cas de cataracte per le Dinitrophenyllyside. Rev. O.N.O., Nov. 1938, p. 622-624.
      � CAZENEUVE and LEPINE. -- Sur les effets produits par l'ingestion et l'injection intraveineuse de trois colorants jaunes derives de la houille. C.R. Ac. Sc. de Paris, 1885, CI, p. 1, 167.
      � CIOTOLA (G.). -- Cataracte par alpha-dinitrophenol. Boll. d'Oc., 16, 1937, p. 531.
      � COGAN D. and COGAN F. -- Dinitrophenol cataract. JAMA, 1935, CV, p. 794.
      � CUTTING, MEHRTENS, TAINTER. -- Dinitrophenol, not acceptable for N.N.R. JAMA. 1935, CV, p. 31. (Important bibliography on the subject).
      � DALLY. -- Du nouveau sur le dinitrophenol. Concours Med. 1935, L, p. 3, 491.
      � EBSTEIN and ROSENBLUM. -- Peripheral neuritis and abortion following dinitrophenol therapy. J. Lab. an Clin. Med. 1935, XX, p. 1, 118.
      � GIBBS-Reichert. -- Am. Chem. J., 1891, XIII, p. 289.
      � GUTZEIT (R.). -- Cure d'obesite et cataracte. Munch. med. Wschr., 2, 1937, p. I.724.
      � HALBRON. -- Les cataractes apres emploi therapeutique du dinitrophenol. Sem. des Hopitaux de Paris, XII, 1937, p. 329.
      � HORNER, JONES, BOARDMAN. -- Cataracts following the use of dinitro. JAMA, 1935, CV, p. 108.
      � HORNER. -- Cataracts after dinitrophenol. Ar. of Opth. 1936, XVI, p. 446-461.
      � HORNER (W.-D.). -- Cataracts following dinitrophenol treatment for obesity. Transact. of the opth. sect. of the Amer. Med. Ass., 1936.
      � KNISKERN. -- Cataract following dinitrophenol. JAMA, 1935, CV, p. 794.
      � KOCH-LEE and TAINTER. -- Dinitrophenol on liver function. Calif. and W. Med., 1935, XXXXIII, p. 337.
      � LAIGNEL-LAVASTINE. -- Soc. Med. des Hopit. de Paris, 1937.
      � LAZAR. -- Cataract following dinitrophenol. JAMA, 1935, CV, p. 794.
      � LEUTSKER. -- Instance of circulatory collapse attributed to dinitrophenol. U.S. Nav. Med. Bull., 1935, XXXIII, p. 394.
      � MAC BRYDE-TAUSIG. -- Functional changes in liver, heart and muscles loss of dextrose tolerance resulting from dinitrophenol. JAMA, 1935, CV, p. 13.
      � MAGNE, MAYER, PLANTEFOL, et al. -- Etude sur l'action du dinitrophenol. An. de Physiol., 1932, CV, p. 12.
      � NADLER. -- Peripheral neuritis caused by prolonged use of dinitrophenol. JAMA, 1935, p. 12.
      � ONFRAY and GILBERT DREYFUS. -- Bull. et Memoires S.F.O., 1937, (I, pp. 114-12.
      � ONETO-GALINO-NATALE. -- Developpement de cataracte aux deux yeux, consequence d'un traitment au dinitrophenol pour amaigrissement. Soc. Argentin. of., 24 Oct. 1937.
      � PERKINS. -- A study of munitions intoxication in France. Pub. Health Rep., 1919, XXXIV, p. 2, 335.
      � RODIN. -- Cataracts following the use of dinitrophenol. Calif. West Med. 44.4, 1936, p. 3.
      � SCHUTES. -- Dinitrophenol. Am. J. Opth., 1935, 18, p. 752.
      � SPAETH (E.-B.). -- Cataractes dues au dinitrophenol avec symptomes de tetanie. Am. J. Opth., Apr. 1936, p. 320-323.
      � STEIN and CREVECOEUR. -- Semaine des Hopitaux de Paris, 15 Dec. 1937.
      � TAINTER, CUTTING and STOCKTON. -- Use of dinitrophenol in nutritional disorders. Am. J. Pub. Health., 1934, XXIV, p. 1045.
      � VAN DER HOEVE and POLAK-DANIELS. -- Cataracte et dinitrophenol. Nederl. Tijdsch. V. Genessk., I, 1936, no. 2, p. 126.
      � VOGT (A.). -- La Cataracte par dinitrophenol en Suisse. Schweiz. Med. Wocst., 76-37, 11 Sep. 1937, p. 873.
      � WHALMAN. -- Dinitrophenol cataract. Am. J. O., Oct. 1936, XIX, p. 885.
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      Great read Pain and if anyone is even considering using that poison they should read every word and then research more and talk with peeps that ACTUALLY ran it.
      *Commitment to Excellence* Excellence is our goal here at BOP. There is a saying that goes like this....if you dont have any haters then you arent doing something right! Haters love success so lets blow the top off of the Bodybuilding internet world!"

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      Agreed. Great read. Read every word and understand DNP. If you use DNP just be smart about it.

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      Wow, i thought i knew it all but damn, that is a lot of great info thanks Pain

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