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djledda-web/raypeat-articles/processed/progesterone-deceptions.html

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Исходник Вина История 

  1. <html>

  2.     <head>

  3.         <title>

  4.             The Progesterone Deceptions

  5.         </title>

  6.     </head>

  7.     <body>

  8.         <h1>

  9.             The Progesterone Deceptions

  10.         </h1>

  11. 

  12.         <p>

  13.             In the 1930s, it was demonstrated that estrogen, even in small doses, produced abortions, and that when it

  14.             is given early enough, even a very small dose will prevent implantation of the fertilized embryo.

  15.             Progesterone was known, by the early 1940s, to protect against the many toxic effects of estrogen, including

  16.             abortion, but it was also known as nature's contraceptive, since it can prevent pregnancy without harmful

  17.             side-effects, by different mechanisms, including prevention of sperm entry into the uterus. That is,

  18.             progesterone prevents the miscarriages which result from excess estrogen (1,2), but if used before

  19.             intercourse, it prevents conception, and thus is a true contraceptive, while estrogen is an abortifacient,

  20.             not a contraceptive.

  21.         </p>

  22.         <p>

  23.             In the 1950s, there was a search for chemicals which would prevent ovulation. According to Carl Djerassi (),

  24.             drug companies were extremely reluctant to risk a religious backlash against their other products, and so

  25.             hesitated to market contraceptives. Obviously, the induction of monthly abortions would have been even

  26.             harder to sell.

  27.         </p>

  28. 

  29.         <p>

  30.             According to Djerassi (3), "Until the middle 1940s ti was assumed that progesterone's biological activity

  31.             was extremely specific and that almost any alteration of the molecule would diminish or abolish its

  32.             activity." This would obviously discourage interest from the drug companies, who could patent a substance

  33.             which they had chemically modified, but could not patent a simple natural substance. However, many

  34.             substances--even non-steroidal chemicals--were known to have estrogenic action. (4)

  35.         </p>

  36.         <p>

  37.             By 1942, Hans Selye had demonstrated that natural steroids retain their activity when administered orally.

  38.             But every drug company with a steroid patent had an obvious interest in having the public believe that there

  39.             is a reason that the natural steroids cannot be conveniently used. The doctrine that natural steroids are

  40.             destroyed by stomach acid appeared, was promoted, and was accepted--without any supporting evidence. In the

  41.             manufacture of progesterone, the precursor steroid is boiled in hydrochloric acid to free it from its

  42.             glucose residue. No one seriously believed that stomach acid hurts progesterone, except the public--and the

  43.             doctors, who had seen the claim in their medical journals, and had heard it from drug salesmen.

  44.         </p>

  45.         <p>

  46.             The myth stopped the use of the cheap tablets of progesterone, as tablets of the synthetic "progestins" came

  47.             on the market, at a much higher price. Doctors who insisted on using real progesterone were forced to buy it

  48.             in an injectable form. As a result, solubility became an issue. Progesterone is extremely insoluble in

  49.             water, and, though it is vastly more soluble in vegetable oil than in water, it does not stay in solution at

  50.             room temperature even at the low concentration of 1 part in 1000 parts of a typical vegetable oil.

  51.         </p>

  52.         <p>

  53.             When people speak of an allergy to progesterone (or even to penicillin) they generally are not aware of the

  54.             presence of a very toxic solvent.(5) For a time, progesterone was often sold dissolved in benzyl benzoate.

  55.             The Physician's Desk Reference warned of possible allergic reactions to progesterone. Now, it is supposedly

  56.             sold dissolved in vegetable oil, with about 10% benzyl alcohol as--supposedly--a "bacteriostatic agent."

  57.         </p>

  58.         <p>

  59.             Bacteriostatic water contains 0.9% to 1.9% benzyl alcohol, and can irreversibly harm nerves. (6,7) Its use

  60.             in hospitals killed thousands of babies. Awareness of benzyl alcohol's toxicity goes back to 1918 at least;

  61.             it was proposed as an effective insecticide, and was found to be toxic to many animal systems. The safe

  62.             systemic dose (7) is exceeded with an injection of 150 mg. of progesterone, yet the local concentration is

  63.             far higher. It can cause a severe reaction even when used at a lower concentration, in bacteriostatic water.

  64.             (5)

  65.         </p>

  66. 

  67.         <p>

  68.             Other alcohols, including ethanol, have been used as solvents, but since they (ethanol even more than benzyl

  69.             alcohol) have an affinity for water, the solution decomposes in contact with tissue water.

  70.         </p>

  71.         <p>

  72.             In spite of the toxicity of the vehicle, several beneficial effects can be obtained with injected

  73.             progesterone, in serious conditions such as epilepsy or caner of the breast or uterus. Many researchers have

  74.             commented on the very obvious difficulty of giving very large amounts of progesterone. (8) My comparisons of

  75.             oral progesterone in tocopherol with other forms and methods of administration show a roughly similar

  76.             efficiency for oral and inject progesterone, and about 1/20 the effect for suppositories. Crystals of

  77.             progesterone are visible in the suppositories I have examined, and this material is obviously wasted.

  78.         </p>

  79.         <p>

  80.             An old theory of vitamin E's mechanism of action in improving fertility was that it spares progesterone.(9)

  81.             It is established that some of the effects of vitamin E and progesterone are similar, for example, both

  82.             prevent oxygen waste and appear to improve mitochondrial coupling of phosphorylation with respiration. I

  83.             suspected that if they actually both work at the same mitochondrial site, then they must have a high mutual

  84.             solubility.

  85.         </p>

  86.         <p>

  87.             Knowing the long-standing problem of administering large doses of progesterone without a toxic solvent, I

  88.             applied for and was granted a patent for the composition of progesterone in tocopherol. One of my reasons

  89.             for publishing in the form of patents is that I have had many years of experience in having my discoveries

  90.             taken up by others without acknowledgment, if they are compatible with conventional prejudices. Typically,

  91.             an editor rejects a paper, and then a few months later publishes a very similar paper by someone else. My

  92.             dissertation research, which established that an estrogen excess kills the embryo by suffocation, and that

  93.             progesterone protects the embryo by promoting the delivery of both oxygen and glucose, didn't strike a

  94.             responsive chord in the journals which are heavily influenced by funds from the drug industry.

  95.         </p>

  96.         <p>

  97.             According to a consultant for a major medical journal, the idea ""of dissolving progesterone, a fat soluble

  98.             steroid hormone, in vitamin E which is then incorporated into chylomicrons absorbed via the lymphatics, and

  99.             thus avoids the liver on the so called first pass" "is so simple it is amazing that the pharmaceutical

  100.             companies have not jumped on it." (A more sophisticated writer might have said ""stomped on it.")

  101.         </p>

  102.         <p>

  103.             In the powder form, direct and intimate contact with a mucous membrane allows lipid phase to lipid phase

  104.             transfer of progesterone molecules. Instead of by-passing the liver, much of the progesterone is picked up

  105.             in the portal circulation, where a major part of it is glucuronidated, and made water soluble for prompt

  106.             excretion.

  107.         </p>

  108. 

  109.         <p>

  110.             Since this glucuronide form cross-reacts to some extent with the ordinary progesterone in the assay process,

  111.             and since 50% of the ordinary free progesterone is carried inside the red blood cells (10,11), and 50% is

  112.             associated with proteins in the plasma, while the glucuronide hardly enters the red blood cells at all, it

  113.             is better to judge by clinical efficacy when comparing different oral forms. My comparisons show several

  114.             times higher potency in the tocopherol composition than in powder form.

  115.         </p>

  116.         <p>

  117.             Since progesterone's use as a drug antedates the 1938 law requiring special federal approval, its legal

  118.             status is similar to that of thyroid hormone. Unfortunately, for both thyroid and progesterone, there is a

  119.             tendency to cut corners for the sake of a bigger profit margin.

  120.         </p>

  121.         <p>

  122.             For example, steroid acetates are generally a little cheaper than the simple natural steroid. Some people

  123.             assume that an acetate or butyrate can be substituted for the steroid itself. This can cause dangerous

  124.             reactions.

  125.         </p>

  126.         <p>

  127.             Medroxyprogesterone acetate is considered a progestin (though it is not supportive of gestation), because it

  128.             modifies the uterus in approximately the wasy progesterone does, but it is luteolytic, and lowers the

  129.             ovaries' production of progesterone while progesterone itself has a positive effect on the corpus luteum,

  130.             stimulating progesterone synthesis. Defining "progestin" in a narrow way allows many synthetics to be sold

  131.             as progestogens, though some of them are strongly estrogenic, allowing them to function as

  132.             contraceptives--it is odd that contraceptives and agents which suppress progesterone synthesis should be

  133.             officially called "supported of pregnancy." It is probably partly the acetate group in the

  134.             medroxyprogesterone acetate molecule which makes it bind firmly to receptors, yet causes it to block the

  135.             enzymes which would normally be involved in progesterone metabolism. (I think testosterone, even, might be a

  136.             safer progestin than medroxyprogesterone acetate.) Pregnenolone acetate similarly blocks the enzymes which

  137.             normally metabolize pregnenolone. (12) In aspirin, it has been found that it is the acetyl group which (by a

  138.             free radical action) blocks an enzyme involved in prostaglandin synthesis.

  139.         </p>

  140.         <p>

  141.             If the category called "progestogens" or "progestins" is to be defined on the basis of a single tissue

  142.             reaction, then it is possible to classify progesterone with the toxic synthetic substances, but then it

  143.             becomes highly deceptive to imply that progesterone is <strong><em>just</em></strong> a progestin, or that

  144.             it has any of the <strong><em>other properties </em></strong>

  145. 

  146.             of the toxic synthetics, but this continues to be done. The warnings about "progestins causing birth

  147.             defects," for example, cause epileptic women t use conventional anti-seizure drugs (all of which cause birth

  148.             defects) during pregnancy, and to avoid natural progesterone, which generally could control their seizures.

  149.             Thus, a false message attached to progesterone creates precisely the harm it claims to want to prevent. In

  150.             my communications with the regulatory agencies, I have concluded that their attempts to deceive are too

  151.             blatant to ascribe to incompetence. Whether it's the Forest Service the FDA, the principle is the same: The

  152.             regulatory agencies have been captured by the regulated industries.

  153.         </p>

  154.         <p>

  155.             Another place to cut costs is in the tocopherol. Tocopherol acetate does have vitamin E activity, but sine

  156.             it is only about half as efficiently absorbed as the simple tocopherol (13), it is a mistake to save a few

  157.             dollars an ounce, at the expense of losing half of the therapeutic effect. People who have compared natural

  158.             progesterone in natural tocopherols with other compositions have insisted that the other compositions must

  159.             not contain progesterone.

  160.         </p>

  161.         <p>

  162.             The taste of natural vitamin E is stronger than that of the synthetic forms, but since the mixture is

  163.             absorbed by any tissue it contacts, including various parts of the bowel, it can be taken in a capsule. If a

  164.             small amount of olive oil is used with it, absorption through the skin is very rapid. Many women use it

  165.             vaginally, spread onto a diaphragm, to hold it in contact with the membranes. The efficiency of absorption

  166.             by all routes is so high that patients should be warned against its anesthetic effect, until their dosage

  167.             requirement is known approximately. Some physicians prefer concentrations higher than 10%, but the risk of

  168.             accidental drunkenness or anesthesia is higher with the stronger solutions.

  169.         </p>

  170.         <p>

  171.             It is an indication of the tocopherol solution's high availability that medical researchers such as Roy

  172.             Hertz (8), who thought they were administering maximal doses by combining injections with suppositories,

  173.             never mentioned the problem of an anesthetic effect from an overdose. Similarly, it si evidence of the

  174.             extremely poor availability of the micropulverized progesterone that the researchers have administered

  175.             hundreds of milligrams per day, without mentioning the symptoms of an overdose. Because of the difficulties

  176.             involved in scientifically studying the clinical effectiveness of various formulations, I think the most

  177.             practical way of evaluating the effectiveness of different progesterone formulations is to measure the

  178.             amount extractable from the red blood cells, a few hours after the peak serum level has been reached. This

  179.             will reasonably reflect the amounts reaching brain cells, adrenal glands, and the various other cells on

  180.             which progesterone has its therapeutic action.

  181.         </p>

  182. 

  183.         <h3>REFERENCES</h3>

  184. 

  185.         <p>

  186.             1. A A. Gidley-Baird, et aI., Failure of implantation in human in vitro fertilization and embryo transfer

  187.             patients: the effects of altered progesterone/estrogen ratios in humans and mice, Fertility and Sterility

  188.             45(1): 69-74, 1986.

  189.         </p>

  190.         <p>

  191.             2. J. L. Yovich, et aI., Early luteal serum progesterone concentrations are higher in pregnancy cycles,

  192.             Fertility and Sterility 44 (1): 185-189, 1985.

  193.         </p>

  194.         <p>

  195.             3. C. Djerassi, The making of the pill, Science 84: 127-129, 1984.

  196.         </p>

  197.         <p>

  198.             4. R. Kehl, Les Glandes Endocrines, Presses Universitaires de France, Paris, 1952.

  199.         </p>

  200.         <p>

  201.             5. J. A. Grant, et aI., New England Journal of Medicine 306(2): 108, 1982, Unsuspected benzyl alcohol

  202.             hypersensitivity.

  203.         </p>

  204.         <p>

  205.             6. T. E. Feasby, et aI., Neurotoxicity of bacteriostatic water, New England Journal of Medicine 308(6):

  206.             966-7, 1983.

  207.         </p>

  208. 

  209.         <p>

  210.             7. E. T. Kimura, et aI., Parenteral toxicity studies with benzyl a1cohol,Toxicol Appl Pharmacol18: 60-68,

  211.             1971.

  212.         </p>

  213.         <p>

  214.             8. A. White, editor, Symposium on Steroids in Experimental and Clinical Practice, The Blakiston Co., N.Y.,

  215.             1951, p. 401.

  216.         </p>

  217.         <p>

  218.             9. A. Fraschini, II Metodo Biologico di Rinvigorimento, Edizioni Minerva Medica, Milan, 1954.

  219.         </p>

  220.         <p>

  221.             10. E. Mulder, et aI., Metabolism of free and conjugated steroids by intact and haemolysed mammalian

  222.             erythrocytes, Biochim. Biophys. Acta 263: <em>290-297, </em>

  223.             1972.

  224.         </p>

  225.         <p>

  226.             11. M. Holzbauer, The association of steroids with blood cells in vivo, J. of Steroid Biochemistry 3:

  227.             579-592, 1972.

  228.         </p>

  229.         <p>

  230.             12. S. Lieberman, et aI., A heuristic proposal for understanding steroidogenic processes, Endocrine Reviews

  231.             5(1): 128-148, 1984.

  232.         </p>

  233.         <p>

  234.             13. L. J. Machlin and E. Gabriel, Kinetics of tissue alpha-tocopherol uptake and depletion, following

  235.             administration of high levels of

  236.         </p>

  237. 

  238.         <p>

  239.             vitamin E, p. 48 in annals of the N.Y. Academy of Science 393,B. Lubin and I. J. Machlin, editors, New York,

  240.             1982.

  241.         </p>

  242. 

  243.         © Ray Peat Ph.D. 2007. All Rights Reserved. www.RayPeat.com

  244.     </body>

  245. </html>