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Wikipedia

Chelation therapy

March 20, 2024

Chelation therapy is a medical procedure that involves the administration of chelating agents to remove heavy metals from the body.[1] Chelation therapy has a long history of use in clinical toxicology[2] and remains in use for some very specific medical treatments, although it is administered under very careful medical supervision due to various inherent risks, including the mobilization of mercury and other metals through the brain and other parts of the body by the use of weak chelating agents that unbind with metals before elimination, exacerbating existing damage.[3] To avoid mobilization, some practitioners of chelation use strong chelators, such as selenium, taken at low doses over a long period of time.

Chelation therapy
Two molecules of deferasirox, an orally administered chelator, binding iron. Deferasirox is used in the treatment of transfusional iron overload in people with thalassemia.
[edit on Wikidata]

Chelation therapy must be administered with care as it has a number of possible side effects, including death.[4][5] In response to increasing use of chelation therapy as alternative medicine and in circumstances in which the therapy should not be used in conventional medicine, various health organizations have confirmed that medical evidence does not support the effectiveness of chelation therapy for any purpose other than the treatment of heavy metal poisoning.[4] Over-the-counter chelation products are not approved for sale in the United States.[6]

Medical uses edit

Chelation therapy is the preferred medical treatment for metal poisoning,[1][7] including acute mercury, iron (including in cases of sickle-cell disease and thalassemia),[8][9] arsenic, lead, uranium, plutonium and other forms of toxic metal poisoning. The chelating agent may be administered intravenously, intramuscularly, or orally, depending on the agent and the type of poisoning.[10]

Chelating agents edit

There are a variety of common chelating agents with differing affinities for different metals, physical characteristics, and biological mechanism of action. For the most common forms of heavy metal intoxication – lead, arsenic, or mercury – a number of chelating agents are available. Dimercaptosuccinic acid (DMSA) has been recommended by poison control centers around the world for the treatment of lead poisoning in children.[11] Other chelating agents, such as 2,3-dimercaptopropanesulfonic acid (DMPS) and alpha lipoic acid (ALA), are used in conventional and alternative medicine. Some common chelating agents are ethylenediaminetetraacetic acid (EDTA), 2,3-dimercaptopropanesulfonic acid (DMPS), and thiamine tetrahydrofurfuryl disulfide (TTFD). Calcium-disodium EDTA and DMSA are only approved for the removal of lead by the Food and Drug Administration while DMPS and TTFD are not approved by the FDA. These drugs bind to heavy metals in the body and prevent them from binding to other agents. They are then excreted from the body. The chelating process also removes vital nutrients such as vitamins C and E, therefore these must be supplemented.[12][unreliable medical source?]

The German Environmental Agency (Umweltbundesamt) listed DMSA and DMPS as the two most useful and safe chelating agents available.[13]

Side effects edit

When used properly in response to a diagnosis of harm from metal toxicity, side effects of chelation therapy include dehydration, low blood calcium, harm to kidneys, increased enzymes as would be detected in liver function tests, allergic reactions, and lowered levels of dietary elements.[16] When administered inappropriately, there are the additional risks of hypocalcaemia (low calcium levels), neurodevelopmental disorders, and death.[16]

History edit

Chelation therapy can be traced back to the early 1930s, when Ferdinand Münz, a German chemist working for I.G. Farben, first synthesized ethylenediaminetetraacetic acid (EDTA).[17] Munz was looking for a replacement for citric acid as a water softener.[17] Chelation therapy itself began during World War II when chemists at the University of Oxford searched for an antidote for lewisite, an arsenic-based chemical weapon.[17] The chemists learned that EDTA was particularly effective in treating lead poisoning.[17]

Following World War II, chelation therapy was used to treat workers who had painted United States naval vessels with lead-based paints.[17] In the 1950s, Norman Clarke, Sr. was treating workers at a battery factory for lead poisoning when he noticed that some of his patients had improved angina pectoris following chelation therapy.[18] Clarke subsequently administered chelation therapy to patients with angina pectoris and other occlusive vascular disease and published his findings in The American Journal of the Medical Sciences in December 1956.[19] He hypothesized that "EDTA could dissolve disease-causing plaques in the coronary systems of human beings."[20] In a series of 283 patients treated by Clarke et al. From 1956 to 1960, 87% showed improvement in their symptomatology.[19] Other early medical investigators made similar observations of EDTA's role in the treatment of cardiovascular disease (Bechtel, 1956; Bessman, 1957; Perry, 1961; Szekely, 1963; Wenig, 1958: and Wilder, 1962).

In 1973, a group of practicing physicians created the Academy of Medical Preventics (now the American College for Advancement in Medicine).[19] The academy trains and certifies physicians in the safe administration of chelation therapy.[21] Members of the academy continued to use EDTA therapy for the treatment of vascular disease and developed safer administration protocols.[19]

In the 1960s, BAL was modified into DMSA, a related dithiol with far fewer side effects.[22] DMSA quickly replaced both BAL and EDTA as the primary treatment for lead, arsenic and mercury poisoning in the United States. Esters of DMSA have been developed which are reportedly more effective; for example, the monoisoamyl ester (MiADMSA) is reportedly more effective than DMSA at clearing mercury and cadmium.[22] Research in the former Soviet Union led to the introduction of DMPS, another dithiol, as a mercury-chelating agent. The Soviets also introduced ALA, which is transformed by the body into the dithiol dihydrolipoic acid, a mercury- and arsenic-chelating agent. DMPS has experimental status in the United States, while ALA is a common nutritional supplement.

Since the 1970s, iron chelation therapy has been used as an alternative to regular phlebotomy to treat excess iron stores in people with haemochromatosis.[23] Other chelating agents have been discovered. They all function by making several chemical bonds with metal ions, thus rendering them much less chemically reactive. The resulting complex is water-soluble, allowing it to enter the bloodstream and be excreted harmlessly.

Calcium-disodium EDTA chelation has been studied by the U.S. National Center for Complementary and Alternative Medicine for treating coronary disease.[24] In 1998, the U.S. Federal Trade Commission (FTC) pursued the American College for Advancement in Medicine (ACAM), an organization that promotes "complementary, alternative and integrative medicine" over the claims made regarding the treatment of atherosclerosis in advertisements for EDTA chelation therapy. The FTC concluded that there was a lack of scientific studies to support these claims and that the statements by the ACAM were false.[25] In 1999, the ACAM agreed to stop presenting chelation therapy as effective in treating heart disease, avoiding legal proceedings.[26] In 2010 the U.S. Food and Drug Administration (FDA) warned companies who sold over-the-counter (OTC) chelation products and stated that such "products are unapproved drugs and devices and that it is a violation of federal law to make unproven claims about these products. There are no FDA-approved OTC chelation products."[6]

Society and culture edit

In 1998, the U.S. Federal Trade Commission (FTC) charged that the web site of the American College for Advancement in Medicine (ACAM) and a brochure they published had made false or unsubstantiated claims. In December 1998, the FTC announced that it had secured a consent agreement barring ACAM from making unsubstantiated advertising claims that chelation therapy is effective against atherosclerosis or any other disease of the circulatory system.[25][27]

In August 2005, doctor error led to the death of a five-year-old boy with autism who was undergoing chelation therapy.[3] Others, including a three-year-old nonautistic girl and a nonautistic adult, have died while undergoing chelation therapy.[3] These deaths were due to cardiac arrest caused by hypocalcemia during chelation therapy. In two of the cases hypocalcemia appears to have been caused by the administration of Na2EDTA (disodium EDTA) and in the third case the type of EDTA was unknown.[28][29] Only the three-year-old girl had been found to have an elevated blood lead level and resulting low iron levels and anemia, which is the conventional medical cause for administration of chelation therapy.[30] According to protocol,[31] EDTA should not be used in the treatment of children.[32] More than 30 deaths have been recorded in association with IV-administered disodium EDTA since the 1970s.[3]

Use in alternative medicine edit

In alternative medicine, some practitioners claim chelation therapy can treat a variety of ailments, including heart disease and autism.[33][34] The use of chelation therapy by alternative medicine practitioners for behavioral and other disorders is considered pseudoscientific; there is no proof that it is effective.[35] Chelation therapy prior to heavy metal testing can artificially raise urinary heavy metal concentrations ("provoked" urine testing) and lead to inappropriate and unnecessary treatment.[36] The American College of Medical Toxicology and the American Academy of Clinical Toxicology warn the public that chelating drugs used in chelation therapy may have serious side effects, including liver and kidney damage, blood pressure changes, allergies and in some cases even death of the patient.[36]

Cancer edit

The American Cancer Society says of chelation therapy: "Available scientific evidence does not support claims that it is effective for treating other conditions such as cancer. Chelation therapy can be toxic and has the potential to cause kidney damage, irregular heartbeat, and even death."[4]

Cardiovascular disease edit

According to the findings of a 1997 systematic review, EDTA chelation therapy is not effective as a treatment for coronary artery disease and this use is not approved in the United States by the US Food and Drug Administration (FDA).[37]

The American Heart Association stated in 1997 that there is "no scientific evidence to demonstrate any benefit from this form of therapy." The United States Food and Drug Administration (FDA), the National Institutes of Health (NIH) and the American College of Cardiology "all agree with the American Heart Association" that "there have been no adequate, controlled, published scientific studies using currently approved scientific methodology to support this therapy for cardiovascular disease."[37] They speculate that any improvement among heart patients undergoing chelation therapy can be attributed to the placebo effect and generally recommended lifestyle changes such as "quitting smoking, losing weight, eating more fruits and vegetables, avoiding foods high in saturated fats and exercising regularly." They also are concerned that patients could put off proven treatments for heart disease like drugs or surgery.

A systematic review published in 2005 found that controlled scientific studies did not support chelation therapy for heart disease.[38] It found that very small trials and uncontrolled descriptive studies have reported benefits while larger controlled studies have found results no better than placebo.

In 2009, the Montana Board of Medical Examiners issued a position paper concluding that "chelation therapy has no proven efficacy in the treatment of cardiovascular disease, and in some patients could be injurious."[39]

The U.S. National Center for Complementary and Alternative Medicine (NCCAM) conducted a trial on the chelation therapy's safety and efficacy for patients with coronary artery disease.[40] NCCAM Director Stephen E. Straus cited the "widespread use of chelation therapy in lieu of established therapies, the lack of adequate prior research to verify its safety and effectiveness, and the overall impact of coronary artery disease" as factors motivating the trial.[41] The study has been criticized by some who said it was unethical, unnecessary and dangerous, and that multiple studies conducted prior to it demonstrated that the treatment provides no benefit.[3]

The US National Center for Complementary and Alternative Medicine began the Trial to Assess Chelation Therapy (TACT) in 2003.[40] Patient enrollment was to be completed around July 2009[24] with final completion around July 2010,[40] but enrollment in the trial was voluntarily suspended by organizers in September 2008 after the Office for Human Research Protections began investigating complaints such as inadequate informed consent.[42] Additionally, the trial was criticized for lacking prior Phase I and II studies, and critics summarized previous controlled trials as having "found no evidence that chelation is superior to placebo for treatment of CAD or PVD."[3] The same critics argued that methodological flaws and lack of prior probability made the trial "unethical, dangerous, pointless, and wasteful."[3] The American College of Cardiology supported the trial and research to explore whether chelation therapy was effective in treating heart disease.[42] Evidence of insurance fraud and other felony convictions among (chelation proponent) investigators further undermined the credibility of the trial.[43]

The final results of TACT were published in November 2012. The authors concluded that disodium EDTA chelation "modestly" reduced the risk of adverse cardiovascular outcomes among stable patients with a history of myocardial infarction.[44] The study also showed a "marked" reduction in cardiovascular events in diabetic patients treated with EDTA chelation.[45] An editorial published in the Journal of the American Medical Association said that "the study findings may provide novel hypotheses that merit further evaluation to help understand the pathophysiology of secondary prevention of vascular disease."[46] Critics of the study characterized the study as showing no support for the use of chelation therapy in coronary heart disease, particularly the claims to reduce the need for coronary artery bypass grafting (CABG, pronounced "cabbage").[47][48][49]

Autism edit

Main article: Thiomersal controversy

Quackwatch says that autism is one of the conditions for which chelation therapy has been falsely promoted as effective, and practitioners falsify diagnoses of metal poisoning to trick parents into having their children undergo the risky process.[50] As of 2008, up to 7% of children with autism worldwide[51] had been subjected to chelation therapy.[52] The death of two children in 2005 was caused by the administration of chelation treatments, according to the American Center for Disease Control. One of them had autism.[53] Parents either have a doctor use a treatment for lead poisoning, or buy unregulated supplements, in particular DMSA and lipoic acid.[52] Aspies For Freedom, an autism rights organization, considers this use of chelation therapy unethical and potentially dangerous.[54] There is little to no credible scientific research that supports the use of chelation therapy for the effective treatment of autism.[34][51][55][56][57][58][59]

See also edit

References edit

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  2. ^ "Chelation: Therapy or "Therapy"?". poison.org. National Capital Poison Center. 6 May 2013 [2010]. Retrieved 9 October 2013.
  3. ^ a b c d e f g Atwood, K.C. IV; Woeckner, E.; Baratz, R.S.; Sampson, W.I. (2008). "Why the NIH Trial to Assess Chelation Therapy (TACT) should be abandoned". Medscape Journal of Medicine. 10 (5): 115. PMC 2438277. PMID 18596934.
  4. ^ a b c . American Cancer Society. 1 November 2008. Archived from the original on 5 July 2010. Retrieved 14 September 2013.
  5. ^ "Deaths Associated with Hypocalcemia from Chelation Therapy - Texas, Pennsylvania, and Oregon, 2003-2005". www.cdc.gov. Retrieved 2016-10-13.
  6. ^ a b Food and Drug Administration (FDA) (14 October 2010). "FDA issues warnings to marketers of unapproved 'chelation' products" (Press release). Archived from the original on January 11, 2017.
  7. ^ Flora, Swaran J. S.; Pachauri, Vidhu (2010-06-28). "Chelation in Metal Intoxication". International Journal of Environmental Research and Public Health. 7 (12): 2745–2788. doi:10.3390/ijerph7072745. PMC 2922724. PMID 20717537.
  8. ^ Fortin, Patricia M.; Fisher, Sheila A.; Madgwick, Karen V.; Trivella, Marialena; Hopewell, Sally; Doree, Carolyn; Estcourt, Lise J. (May 8, 2018). "Interventions for improving adherence to iron chelation therapy in people with sickle cell disease or thalassaemia". The Cochrane Database of Systematic Reviews. 2018 (5): CD012349. doi:10.1002/14651858.CD012349.pub2. ISSN 1469-493X. PMC 5985157. PMID 29737522.
  9. ^ Hider, Robert C.; Kong, Xiaole (2013). "Chapter 8. Iron: Effect of Overload and Deficiency". In Astrid Sigel, Helmut Sigel and Roland K. O. Sigel (ed.). Interrelations between Essential Metal Ions and Human Diseases. Metal Ions in Life Sciences. Vol. 13. Springer. pp. 229–294. doi:10.1007/978-94-007-7500-8_8. ISBN 978-94-007-7499-5. PMID 24470094.
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    • Kosnett, M J (2010). "Chelation for Heavy Metals (Arsenic, Lead, and Mercury): Protective or Perilous?". Clinical Pharmacology & Therapeutics. 88 (3): 412–415. doi:10.1038/clpt.2010.132. ISSN 0009-9236. PMID 20664538. S2CID 28321495.
    • Medical Letter consultants (September 20, 2010). "Nonstandard uses of chelation therapy". The Medical Letter on Drugs and Therapeutics. 52 (1347): 75–6. PMID 20847718.
    • Food and Drug Administration (14 October 2010). "Consumer Updates - FDA Warns Marketers of Unapproved 'Chelation' Drugs". fda.gov. Retrieved 3 July 2014.
  17. ^ a b c d e "Chemistry in its element: compounds". Royal Society of Chemistry. Retrieved 30 June 2014.
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  19. ^ a b c d Efrain Olszewer; James P. Carter (1988). "EDTA Chelation Therapy in Chronic Degenerative Disease". Medical Hypotheses. 27 (1): 41–49. doi:10.1016/0306-9877(88)90082-5. PMID 3144646.
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  22. ^ a b Kalia, Kiran; Flora, Swaran J.S. (2005). "Strategies for safe and effective therapeutic measures for chronic arsenic and lead poisoning". Journal of Occupational Health. Japan Society for Occupational Health. 47 (1): 1–21. doi:10.1539/joh.47.1. PMID 15703449.
  23. ^ , Hemochromatosis for healthcare professionals, Division of Nutrition and Physical Activity, National Center for Chronic Disease Prevention and Health Promotion, Centers for Disease Control and Prevention, U.S. Dept. of Health and Human Services, 1 November 2007, archived from the original on 2008-02-24, retrieved 29 March 2008
  24. ^ a b . National Center for Complementary and Alternative Medicine (NCCAM), National Institutes of Health, U.S. Dept. of Health and Human Services. March 2007. Archived from the original on 2007-10-15. Retrieved 11 November 2007.
  25. ^ a b "American College for Advancement in Medicine: Case Timeline" (FTC Case Timeline with links to documents). Federal Trade Commission (FTC). 13 July 1999. Retrieved 1 July 2010.
  26. ^ "United States of America Federal Trade Commission In the Matter of American College for Advancement in Medicine, a corporation. File no. 962 3147. Agreement Containing Consent Order". Federal Trade Commission. 12 January 1998. Retrieved 1 July 2010. "Attachment A" (Notification letter).
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  28. ^ Brown, M.J.; Willis, T.; Omalu, B.; Leiker, R. (2006). . Pediatrics. 118 (2): e534–6. doi:10.1542/peds.2006-0858. PMID 16882789. S2CID 28656831. Archived from the original on 2009-07-27. Retrieved 2007-11-13.
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  30. ^ Centers for Disease Control Prevention (CDC) (2006). "Deaths associated with hypocalcemia from chelation therapy - Texas, Pennsylvania, and Oregon, 2003-2005". Morbidity and Mortality Weekly Report. Centers for Disease Control and Prevention. 55 (8): 204–7. PMID 16511441.
  31. ^ Drugs, Committee on (1995-07-01). "Treatment Guidelines for Lead Exposure in Children". Pediatrics. 96 (1): 155–159. doi:10.1542/peds.96.1.155. ISSN 0031-4005. PMID 7596706. S2CID 2477907.
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External links edit

  • Chelation Therapy: Unproven Claims and Unsound Theories - Quackwatch

March 20, 2024
chelation, therapy, medical, procedure, that, involves, administration, chelating, agents, remove, heavy, metals, from, body, long, history, clinical, toxicology, remains, some, very, specific, medical, treatments, although, administered, under, very, careful,. Chelation therapy is a medical procedure that involves the administration of chelating agents to remove heavy metals from the body 1 Chelation therapy has a long history of use in clinical toxicology 2 and remains in use for some very specific medical treatments although it is administered under very careful medical supervision due to various inherent risks including the mobilization of mercury and other metals through the brain and other parts of the body by the use of weak chelating agents that unbind with metals before elimination exacerbating existing damage 3 To avoid mobilization some practitioners of chelation use strong chelators such as selenium taken at low doses over a long period of time Chelation therapyTwo molecules of deferasirox an orally administered chelator binding iron Deferasirox is used in the treatment of transfusional iron overload in people with thalassemia edit on Wikidata Chelation therapy must be administered with care as it has a number of possible side effects including death 4 5 In response to increasing use of chelation therapy as alternative medicine and in circumstances in which the therapy should not be used in conventional medicine various health organizations have confirmed that medical evidence does not support the effectiveness of chelation therapy for any purpose other than the treatment of heavy metal poisoning 4 Over the counter chelation products are not approved for sale in the United States 6 Contents 1 Medical uses 1 1 Chelating agents 2 Side effects 3 History 4 Society and culture 4 1 Use in alternative medicine 4 1 1 Cancer 4 1 2 Cardiovascular disease 4 1 3 Autism 5 See also 6 References 7 External linksMedical uses editChelation therapy is the preferred medical treatment for metal poisoning 1 7 including acute mercury iron including in cases of sickle cell disease and thalassemia 8 9 arsenic lead uranium plutonium and other forms of toxic metal poisoning The chelating agent may be administered intravenously intramuscularly or orally depending on the agent and the type of poisoning 10 Chelating agents edit There are a variety of common chelating agents with differing affinities for different metals physical characteristics and biological mechanism of action For the most common forms of heavy metal intoxication lead arsenic or mercury a number of chelating agents are available Dimercaptosuccinic acid DMSA has been recommended by poison control centers around the world for the treatment of lead poisoning in children 11 Other chelating agents such as 2 3 dimercaptopropanesulfonic acid DMPS and alpha lipoic acid ALA are used in conventional and alternative medicine Some common chelating agents are ethylenediaminetetraacetic acid EDTA 2 3 dimercaptopropanesulfonic acid DMPS and thiamine tetrahydrofurfuryl disulfide TTFD Calcium disodium EDTA and DMSA are only approved for the removal of lead by the Food and Drug Administration while DMPS and TTFD are not approved by the FDA These drugs bind to heavy metals in the body and prevent them from binding to other agents They are then excreted from the body The chelating process also removes vital nutrients such as vitamins C and E therefore these must be supplemented 12 unreliable medical source The German Environmental Agency Umweltbundesamt listed DMSA and DMPS as the two most useful and safe chelating agents available 13 Chelator Used inDimercaprol British anti Lewisite BAL acute arsenic poisoning 14 acute mercury poisoning 14 lead poisoning in addition to EDTA 14 Lewisite poisoning for which it was developed as an antidote Dimercaptosuccinic acid DMSA lead poisoning 14 arsenic poisoning 14 mercury poisoning 14 Dimercapto propane sulfonate DMPS severe acute arsenic poisoning 14 severe acute mercury poisoning 14 Penicillamine Mainly in copper toxicity 14 Occasionally adjunctive therapy in gold toxicity 14 arsenic poisoning 14 lead poisoning 14 rheumatoid arthritis 14 Ethylenediamine tetraacetic acid calcium disodium versenate CaNa2 EDTA lead poisoning 14 Deferoxamine Deferasirox and Deferiprone acute iron poisoning 14 iron overload 15 Side effects editWhen used properly in response to a diagnosis of harm from metal toxicity side effects of chelation therapy include dehydration low blood calcium harm to kidneys increased enzymes as would be detected in liver function tests allergic reactions and lowered levels of dietary elements 16 When administered inappropriately there are the additional risks of hypocalcaemia low calcium levels neurodevelopmental disorders and death 16 History editChelation therapy can be traced back to the early 1930s when Ferdinand Munz a German chemist working for I G Farben first synthesized ethylenediaminetetraacetic acid EDTA 17 Munz was looking for a replacement for citric acid as a water softener 17 Chelation therapy itself began during World War II when chemists at the University of Oxford searched for an antidote for lewisite an arsenic based chemical weapon 17 The chemists learned that EDTA was particularly effective in treating lead poisoning 17 Following World War II chelation therapy was used to treat workers who had painted United States naval vessels with lead based paints 17 In the 1950s Norman Clarke Sr was treating workers at a battery factory for lead poisoning when he noticed that some of his patients had improved angina pectoris following chelation therapy 18 Clarke subsequently administered chelation therapy to patients with angina pectoris and other occlusive vascular disease and published his findings in The American Journal of the Medical Sciences in December 1956 19 He hypothesized that EDTA could dissolve disease causing plaques in the coronary systems of human beings 20 In a series of 283 patients treated by Clarke et al From 1956 to 1960 87 showed improvement in their symptomatology 19 Other early medical investigators made similar observations of EDTA s role in the treatment of cardiovascular disease Bechtel 1956 Bessman 1957 Perry 1961 Szekely 1963 Wenig 1958 and Wilder 1962 In 1973 a group of practicing physicians created the Academy of Medical Preventics now the American College for Advancement in Medicine 19 The academy trains and certifies physicians in the safe administration of chelation therapy 21 Members of the academy continued to use EDTA therapy for the treatment of vascular disease and developed safer administration protocols 19 In the 1960s BAL was modified into DMSA a related dithiol with far fewer side effects 22 DMSA quickly replaced both BAL and EDTA as the primary treatment for lead arsenic and mercury poisoning in the United States Esters of DMSA have been developed which are reportedly more effective for example the monoisoamyl ester MiADMSA is reportedly more effective than DMSA at clearing mercury and cadmium 22 Research in the former Soviet Union led to the introduction of DMPS another dithiol as a mercury chelating agent The Soviets also introduced ALA which is transformed by the body into the dithiol dihydrolipoic acid a mercury and arsenic chelating agent DMPS has experimental status in the United States while ALA is a common nutritional supplement Since the 1970s iron chelation therapy has been used as an alternative to regular phlebotomy to treat excess iron stores in people with haemochromatosis 23 Other chelating agents have been discovered They all function by making several chemical bonds with metal ions thus rendering them much less chemically reactive The resulting complex is water soluble allowing it to enter the bloodstream and be excreted harmlessly Calcium disodium EDTA chelation has been studied by the U S National Center for Complementary and Alternative Medicine for treating coronary disease 24 In 1998 the U S Federal Trade Commission FTC pursued the American College for Advancement in Medicine ACAM an organization that promotes complementary alternative and integrative medicine over the claims made regarding the treatment of atherosclerosis in advertisements for EDTA chelation therapy The FTC concluded that there was a lack of scientific studies to support these claims and that the statements by the ACAM were false 25 In 1999 the ACAM agreed to stop presenting chelation therapy as effective in treating heart disease avoiding legal proceedings 26 In 2010 the U S Food and Drug Administration FDA warned companies who sold over the counter OTC chelation products and stated that such products are unapproved drugs and devices and that it is a violation of federal law to make unproven claims about these products There are no FDA approved OTC chelation products 6 Society and culture editIn 1998 the U S Federal Trade Commission FTC charged that the web site of the American College for Advancement in Medicine ACAM and a brochure they published had made false or unsubstantiated claims In December 1998 the FTC announced that it had secured a consent agreement barring ACAM from making unsubstantiated advertising claims that chelation therapy is effective against atherosclerosis or any other disease of the circulatory system 25 27 In August 2005 doctor error led to the death of a five year old boy with autism who was undergoing chelation therapy 3 Others including a three year old nonautistic girl and a nonautistic adult have died while undergoing chelation therapy 3 These deaths were due to cardiac arrest caused by hypocalcemia during chelation therapy In two of the cases hypocalcemia appears to have been caused by the administration of Na2EDTA disodium EDTA and in the third case the type of EDTA was unknown 28 29 Only the three year old girl had been found to have an elevated blood lead level and resulting low iron levels and anemia which is the conventional medical cause for administration of chelation therapy 30 According to protocol 31 EDTA should not be used in the treatment of children 32 More than 30 deaths have been recorded in association with IV administered disodium EDTA since the 1970s 3 Use in alternative medicine edit In alternative medicine some practitioners claim chelation therapy can treat a variety of ailments including heart disease and autism 33 34 The use of chelation therapy by alternative medicine practitioners for behavioral and other disorders is considered pseudoscientific there is no proof that it is effective 35 Chelation therapy prior to heavy metal testing can artificially raise urinary heavy metal concentrations provoked urine testing and lead to inappropriate and unnecessary treatment 36 The American College of Medical Toxicology and the American Academy of Clinical Toxicology warn the public that chelating drugs used in chelation therapy may have serious side effects including liver and kidney damage blood pressure changes allergies and in some cases even death of the patient 36 Cancer edit The American Cancer Society says of chelation therapy Available scientific evidence does not support claims that it is effective for treating other conditions such as cancer Chelation therapy can be toxic and has the potential to cause kidney damage irregular heartbeat and even death 4 Cardiovascular disease edit According to the findings of a 1997 systematic review EDTA chelation therapy is not effective as a treatment for coronary artery disease and this use is not approved in the United States by the US Food and Drug Administration FDA 37 The American Heart Association stated in 1997 that there is no scientific evidence to demonstrate any benefit from this form of therapy The United States Food and Drug Administration FDA the National Institutes of Health NIH and the American College of Cardiology all agree with the American Heart Association that there have been no adequate controlled published scientific studies using currently approved scientific methodology to support this therapy for cardiovascular disease 37 They speculate that any improvement among heart patients undergoing chelation therapy can be attributed to the placebo effect and generally recommended lifestyle changes such as quitting smoking losing weight eating more fruits and vegetables avoiding foods high in saturated fats and exercising regularly They also are concerned that patients could put off proven treatments for heart disease like drugs or surgery A systematic review published in 2005 found that controlled scientific studies did not support chelation therapy for heart disease 38 It found that very small trials and uncontrolled descriptive studies have reported benefits while larger controlled studies have found results no better than placebo In 2009 the Montana Board of Medical Examiners issued a position paper concluding that chelation therapy has no proven efficacy in the treatment of cardiovascular disease and in some patients could be injurious 39 The U S National Center for Complementary and Alternative Medicine NCCAM conducted a trial on the chelation therapy s safety and efficacy for patients with coronary artery disease 40 NCCAM Director Stephen E Straus cited the widespread use of chelation therapy in lieu of established therapies the lack of adequate prior research to verify its safety and effectiveness and the overall impact of coronary artery disease as factors motivating the trial 41 The study has been criticized by some who said it was unethical unnecessary and dangerous and that multiple studies conducted prior to it demonstrated that the treatment provides no benefit 3 The US National Center for Complementary and Alternative Medicine began the Trial to Assess Chelation Therapy TACT in 2003 40 Patient enrollment was to be completed around July 2009 24 with final completion around July 2010 40 but enrollment in the trial was voluntarily suspended by organizers in September 2008 after the Office for Human Research Protections began investigating complaints such as inadequate informed consent 42 Additionally the trial was criticized for lacking prior Phase I and II studies and critics summarized previous controlled trials as having found no evidence that chelation is superior to placebo for treatment of CAD or PVD 3 The same critics argued that methodological flaws and lack of prior probability made the trial unethical dangerous pointless and wasteful 3 The American College of Cardiology supported the trial and research to explore whether chelation therapy was effective in treating heart disease 42 Evidence of insurance fraud and other felony convictions among chelation proponent investigators further undermined the credibility of the trial 43 The final results of TACT were published in November 2012 The authors concluded that disodium EDTA chelation modestly reduced the risk of adverse cardiovascular outcomes among stable patients with a history of myocardial infarction 44 The study also showed a marked reduction in cardiovascular events in diabetic patients treated with EDTA chelation 45 An editorial published in the Journal of the American Medical Association said that the study findings may provide novel hypotheses that merit further evaluation to help understand the pathophysiology of secondary prevention of vascular disease 46 Critics of the study characterized the study as showing no support for the use of chelation therapy in coronary heart disease particularly the claims to reduce the need for coronary artery bypass grafting CABG pronounced cabbage 47 48 49 Autism edit Main article Thiomersal controversy Quackwatch says that autism is one of the conditions for which chelation therapy has been falsely promoted as effective and practitioners falsify diagnoses of metal poisoning to trick parents into having their children undergo the risky process 50 As of 2008 update up to 7 of children with autism worldwide 51 had been subjected to chelation therapy 52 The death of two children in 2005 was caused by the administration of chelation treatments according to the American Center for Disease Control One of them had autism 53 Parents either have a doctor use a treatment for lead poisoning or buy unregulated supplements in particular DMSA and lipoic acid 52 Aspies For Freedom an autism rights organization considers this use of chelation therapy unethical and potentially dangerous 54 There is little to no credible scientific research that supports the use of chelation therapy for the effective treatment of autism 34 51 55 56 57 58 59 See also editList of ineffective cancer treatments DetoxificationReferences edit a b Aaseth Jan Crisponi Guido Anderson Ole 2016 Chelation Therapy in the Treatment of Metal Intoxication Academic Press p 388 ISBN 978 0 12 803072 1 Chelation Therapy or Therapy poison org National Capital Poison Center 6 May 2013 2010 Retrieved 9 October 2013 a b c d e f g Atwood K C IV Woeckner E Baratz R S Sampson W I 2008 Why the NIH Trial to Assess Chelation Therapy TACT should be abandoned Medscape Journal of Medicine 10 5 115 PMC 2438277 PMID 18596934 a b c Chelation Therapy American Cancer Society 1 November 2008 Archived from the original on 5 July 2010 Retrieved 14 September 2013 Deaths Associated with Hypocalcemia from Chelation Therapy Texas Pennsylvania and Oregon 2003 2005 www cdc gov Retrieved 2016 10 13 a b Food and Drug Administration FDA 14 October 2010 FDA issues warnings to marketers of unapproved chelation products Press release Archived from the original on January 11 2017 Flora Swaran J S Pachauri Vidhu 2010 06 28 Chelation in Metal Intoxication International Journal of Environmental Research and Public Health 7 12 2745 2788 doi 10 3390 ijerph7072745 PMC 2922724 PMID 20717537 Fortin Patricia M Fisher Sheila A Madgwick Karen V Trivella Marialena Hopewell Sally Doree Carolyn Estcourt Lise J May 8 2018 Interventions for improving adherence to iron chelation therapy in people with sickle cell disease or thalassaemia The Cochrane Database of Systematic Reviews 2018 5 CD012349 doi 10 1002 14651858 CD012349 pub2 ISSN 1469 493X PMC 5985157 PMID 29737522 Hider Robert C Kong Xiaole 2013 Chapter 8 Iron Effect of Overload and Deficiency In Astrid Sigel Helmut Sigel and Roland K O Sigel ed Interrelations between Essential Metal Ions and Human Diseases Metal Ions in Life Sciences Vol 13 Springer pp 229 294 doi 10 1007 978 94 007 7500 8 8 ISBN 978 94 007 7499 5 PMID 24470094 Flora Govinder Mittal Megha Flora Swaran J S 2015 01 01 Flora S J S ed 26 Medical Countermeasures Chelation Therapy Handbook of Arsenic Toxicology Oxford Academic Press pp 589 626 ISBN 978 0 12 418688 0 retrieved 2020 12 07 Chisolm J J Jr 2000 Safety and efficacy of meso 2 3 dimercaptosuccinic acid DMSA in children with elevated blood lead concentrations Journal of Toxicology Clinical Toxicology 38 4 365 75 doi 10 1081 CLT 100100945 PMID 10930052 S2CID 21793727 Bridges Sarah January 2006 The promise of chelation Mothering No 134 pp 54 61 Kommission Human Biomonitoring des Umweltbundesamtes Human Biomonitoring Committee of the Federal Environmental Agency Federal Republic of Germany 1999 Bekanntmachung des Umweltbundesamtes Einsatz von Chelatbildnern in der Umweltmedizin Stellungnahme der Kommission Human Biomonitoring des Umweltbundesamtes Notice of the Federal Environmental Agency use of chelating agents in environmental medicine Opinion of the Commission Human biomonitoring of the German Federal Environment Agency Bundesgesundheitsblatt Gesundheitsforschung Gesundheitsschutz in German 42 10 823 4 doi 10 1007 s001030050288 S2CID 30922256 a b c d e f g h i j k l m n o Masters Susan B Trevor Anthony J Katzung Bertram G 2008 Katzung amp Trevor s Pharmacology Examination amp Board Review 8th ed McGraw Hill Medical pp 481 3 ISBN 978 0 07 148869 3 Crisponi Guido Nurchi Valeria M Lachowicz Joanna 2019 Chapter 3 Iron Chelation for Iron Overload in Thalassemia In Sigel Astrid Freisinger Eva Sigel Roland K O Carver Peggy L eds Essential Metals in Medicine Therapeutic Use and Toxicity of Metal Ions in the Clinic Vol 19 Berlin de Gruyter GmbH pp 49 86 doi 10 1515 9783110527872 009 ISBN 978 3 11 052691 2 PMID 30855104 S2CID 73727755 a href Template Cite book html title Template Cite book cite book a journal ignored help a b American College of Medical Toxicology American Academy of Clinical Toxicology February 2013 Five Things Physicians and Patients Should Question Choosing Wisely an initiative of the ABIM Foundation American College of Medical Toxicology and American Academy of Clinical Toxicology retrieved 5 December 2013 which cites Kosnett M J 2010 Chelation for Heavy Metals Arsenic Lead and Mercury Protective or Perilous Clinical Pharmacology amp Therapeutics 88 3 412 415 doi 10 1038 clpt 2010 132 ISSN 0009 9236 PMID 20664538 S2CID 28321495 Medical Letter consultants September 20 2010 Nonstandard uses of chelation therapy The Medical Letter on Drugs and Therapeutics 52 1347 75 6 PMID 20847718 Food and Drug Administration 14 October 2010 Consumer Updates FDA Warns Marketers of Unapproved Chelation Drugs fda gov Retrieved 3 July 2014 a b c d e Chemistry in its element compounds Royal Society of Chemistry Retrieved 30 June 2014 Heidi Braun Grebe Philip J Gregory 2002 Inhibition of Warfarin Anticoagulation Associated with Chelation Therapy 22 8 Pharmacotherapy a href Template Cite journal html title Template Cite journal cite journal a Cite journal requires journal help a b c d Efrain Olszewer James P Carter 1988 EDTA Chelation Therapy in Chronic Degenerative Disease Medical Hypotheses 27 1 41 49 doi 10 1016 0306 9877 88 90082 5 PMID 3144646 M R Lewin 1997 Chelation therapy for cardiovascular disease Review and commentary Tex Heart Inst J 24 2 81 89 PMC 325409 PMID 9205980 Ronald L Hoffman February 2014 The facts and fictions of chelation therapy The Clinical Advisor Retrieved 30 June 2014 a b Kalia Kiran Flora Swaran J S 2005 Strategies for safe and effective therapeutic measures for chronic arsenic and lead poisoning Journal of Occupational Health Japan Society for Occupational Health 47 1 1 21 doi 10 1539 joh 47 1 PMID 15703449 Treatment amp Management Monitoring Treatment Hemochromatosis for healthcare professionals Division of Nutrition and Physical Activity National Center for Chronic Disease Prevention and Health Promotion Centers for Disease Control and Prevention U S Dept of Health and Human Services 1 November 2007 archived from the original on 2008 02 24 retrieved 29 March 2008 a b Questions and Answers The NIH Trial of EDTA Chelation Therapy for Coronary Artery Disease National Center for Complementary and Alternative Medicine NCCAM National Institutes of Health U S Dept of Health and Human Services March 2007 Archived from the original on 2007 10 15 Retrieved 11 November 2007 a b American College for Advancement in Medicine Case Timeline FTC Case Timeline with links to documents Federal Trade Commission FTC 13 July 1999 Retrieved 1 July 2010 United States of America Federal Trade Commission In the Matter of American College for Advancement in Medicine a corporation File no 962 3147 Agreement Containing Consent Order Federal Trade Commission 12 January 1998 Retrieved 1 July 2010 Attachment A Notification letter Federal Trade Commission 8 December 1998 Medical Association Settles False Advertising Charges Over Promotion of Chelation Therapy Press release Retrieved 17 January 2014 Brown M J Willis T Omalu B Leiker R 2006 Deaths resulting from hypocalcemia after administration of edetate disodium 2003 2005 Pediatrics 118 2 e534 6 doi 10 1542 peds 2006 0858 PMID 16882789 S2CID 28656831 Archived from the original on 2009 07 27 Retrieved 2007 11 13 Baxter A J Krenzelok E P 2008 Pediatric fatality secondary to EDTA chelation Clinical Toxicology 46 10 1083 4 doi 10 1080 15563650701261488 PMID 18949650 S2CID 24576683 Centers for Disease Control Prevention CDC 2006 Deaths associated with hypocalcemia from chelation therapy Texas Pennsylvania and Oregon 2003 2005 Morbidity and Mortality Weekly Report Centers for Disease Control and Prevention 55 8 204 7 PMID 16511441 Drugs Committee on 1995 07 01 Treatment Guidelines for Lead Exposure in Children Pediatrics 96 1 155 159 doi 10 1542 peds 96 1 155 ISSN 0031 4005 PMID 7596706 S2CID 2477907 Van der Schaar Peter J 2011 Textbook of Clinical Metal Toxicology 10th ed Leende Netherlands International Board of Clinical Metal Toxicology unreliable medical source full citation needed Ernst E 2000 Chelation therapy for coronary heart disease An overview of all clinical investigations American Heart Journal 140 1 139 41 doi 10 1067 mhj 2000 107548 PMID 10874275 a b Weber W Newmark S 2007 Complementary and alternative medical therapies for attention deficit hyperactivity disorder and autism Pediatric Clinics of North America 54 6 983 1006 doi 10 1016 j pcl 2007 09 006 PMID 18061787 Boy with autism dies during chelation therapy Behavior News Behavior Analysis Association of Michigan 30 August 2005 Archived from the original on 29 November 2016 Retrieved 4 August 2010 a b American College of Medical Toxicology American Academy of Clinical Toxicology February 2013 Five Things Physicians and Patients Should Question Choosing Wisely an initiative of the ABIM Foundation American College of Medical Toxicology and American Academy of Clinical Toxicology retrieved 5 December 2013 a b Ernst Edzard 1997 Chelation therapy for peripheral arterial occlusive disease A systematic review Circulation 96 3 1031 3 doi 10 1161 01 CIR 96 3 1031 PMID 9264515 Seely D M Wu P Mills E J 2005 EDTA chelation therapy for cardiovascular disease A systematic review BMC Cardiovascular Disorders 5 32 doi 10 1186 1471 2261 5 32 PMC 1282574 PMID 16262904 Montana Board of Medical Examiners BME 14 May 2009 EDTA Chelation for Cardiovascular Disease PDF BME Position Paper Business Standard Div Montana Dept of Labor and Industry Archived from the original PDF on 2010 02 04 a b c Md Gervasio Lamas August 2013 Trial to Assess Chelation Therapy TACT ClinicalTrials gov U S National Library of Medicine National Institutes of Health U S Dept of Health and Human Services ClinicalTrials gov identifier NCT00044213 National Institutes of Health NIH National Center for Complementary and Alternative Medicine National Heart Lung and Blood Institute 7 August 2002 NIH Launches Large Clinical Trial on EDTA Chelation Therapy for Coronary Artery Disease NIH News Press release NIH Archived from the original on 28 December 2014 Retrieved 28 December 2008 a href Template Cite press release html title Template Cite press release cite press release a CS1 maint multiple names authors list link a b Government probes chelation heart disease study Washington Post Washington DC Associated Press 2008 09 25 Retrieved 2008 09 26 dead link Jones Valerie 2009 07 09 NIH Awards 30 Million Research Dollars To Convicted Felons Cliff s Notes Version Science Based Medicine Retrieved December 5 2014 Gervasio D Lamas 2013 Effect of Disodium EDTA Chelation Regimen on Cardiovascular Events in Patients With Previous Myocardial Infarction The TACT Randomized Trial JAMA 309 12 1241 1250 doi 10 1001 jama 2013 2107 PMC 4066975 PMID 23532240 Escolar E Lamas G A Mark D B Boineau R Goertz C Rosenberg Y Nahin R L Ouyang P Rozema T Magaziner A Nahas R Lewis E F Lindblad L Lee K L 2014 The Effect of an EDTA based Chelation Regimen on Patients With Diabetes Mellitus and Prior Myocardial Infarction in the Trial to Assess Chelation Therapy TACT Circulation Cardiovascular Quality and Outcomes CircoutComes 7 1 15 24 doi 10 1161 CIRCOUTCOMES 113 000663 PMC 4111470 PMID 24254885 Bauchner H Fontanarosa PB Golub RM 2013 Evaluation of the Trial to Assess Chelation Therapy TACT The Scientific Process Peer Review and Editorial Scrutiny JAMA 309 12 1291 1292 doi 10 1001 jama 2013 2761 PMID 23532245 Atwood Kimball 4 November 2012 The Trial to Assess Chelation Therapy Equivocal as Predicted Science Based Medicine Gorski David 5 November 2012 The result of the Trial to Assess Chelation Therapy TACT As underwhelming as expected Science Based Medicine Chelation therapy doesn t alter quality of life in heart attack patients American Heart Association 4 November 2012 Archived from the original on 9 November 2012 Retrieved 30 November 2012 Why Chelation Therapy Should Be Avoided Quackwatch 15 May 2004 Retrieved 7 October 2013 a b Davis Tonya N O Reilly Mark Kang Soyeon Lang Russell et al 2013 Chelation treatment for autism spectrum disorders A systematic review Research in Autism Spectrum Disorders 7 1 49 55 doi 10 1016 j rasd 2012 06 005 However given the significant methodological limitations of these studies the research reviewed here does not support the use of chelation as a treatment for ASD a b Stokstad E 2008 Stalled trial for autism highlights dilemma of alternative treatments Science 321 5887 326 doi 10 1126 science 321 5887 326 PMID 18635766 S2CID 206581219 FDA links child deaths to chelation therapy NBC News Associated Press February 3 2006 Archived from the original on August 30 2018 Retrieved August 30 2018 Aspies For Freedom Aspies For Freedom Archived from the original on 2010 01 17 Retrieved 24 February 2009 Blakeslee Sandra 19 May 2004 Panel finds no evidence to tie autism to vaccines New York Times Retrieved 2008 02 01 Blaucok Busch E Amin O R Dessoki H H Rabah T 2012 Efficacy of DMSA therapy in a sample of Arab children with autistic spectrum disorder Maedica 7 3 214 21 PMC 3566884 PMID 23400264 Adams J B Baral M Geis E Mitchell J et al 2009 Safety and efficacy of oral DMSA therapy for children with autism spectrum disorders Part B Behavioral results BMC Clinical Pharmacology 9 17 doi 10 1186 1472 6904 9 17 PMC 2770991 PMID 19852790 Adams J B Baral M Geis E Mitchell J et al 2009 The severity of autism is associated with toxic metal body burden and red blood cell glutathione levels Journal of Toxicology 2009 532640 doi 10 1155 2009 532640 PMC 2809421 PMID 20107587 Adams J B Baral M Geis E Mitchell J et al 2009 Safety and efficacy of oral DMSA therapy for children with autism spectrum disorders Part A Medical results BMC Clinical Pharmacology 9 16 doi 10 1186 1472 6904 9 16 PMC 2774660 PMID 19852789 External links editChelation Therapy Unproven Claims and Unsound Theories Quackwatch Retrieved from https en wikipedia org w index php title Chelation therapy amp oldid 1212920412, wikipedia, wiki, book, books, library,

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