Literature DB >> 26114777

Chelation for autism spectrum disorder (ASD).

Stephen James1, Shawn W Stevenson, Natalie Silove, Katrina Williams.   

Abstract

BACKGROUND: It has been suggested that the severity of autism spectrum disorder (ASD) symptoms is positively correlated with the level of circulating or stored toxic metals, and that excretion of these heavy metals, brought about by the use of pharmaceutical chelating agents, results in improved symptoms.
OBJECTIVES: To assess the potential benefits and adverse effects of pharmaceutical chelating agents (referred to as chelation therapy throughout this review) for autism spectrum disorder (ASD) symptoms. SEARCH
METHODS: We searched the following databases on 6 November 2014: CENTRAL, Ovid MEDLINE, Ovid MEDLINE In-Process, Embase, PsycINFO, Cumulative Index to Nursing and Allied Health Literature (CINAHL) and 15 other databases, including three trials registers. In addition we checked references lists and contacted experts. SELECTION CRITERIA: All randomised controlled trials of pharmaceutical chelating agents compared with placebo in individuals with ASD. DATA COLLECTION AND ANALYSIS: Two review authors independently selected studies, assessed them for risk of bias and extracted relevant data. We did not conduct a meta-analysis, as only one study was included. MAIN
RESULTS: We excluded nine studies because they were non-randomised trials or were withdrawn before enrolment. We included one study, which was conducted in two phases. During the first phase of the study, 77 children with ASD were randomly assigned to receive seven days of glutathione lotion or placebo lotion, followed by three days of oral dimercaptosuccinic acid (DMSA). Forty-nine children who were found to be high excreters of heavy metals during phase one continued on to phase two to receive three days of oral DMSA or placebo followed by 11 days off, with the cycle repeated up to six times. The second phase thus assessed the effectiveness of multiple doses of oral DMSA compared with placebo in children who were high excreters of heavy metals and who received a three-day course of oral DMSA. Overall, no evidence suggests that multiple rounds of oral DMSA had an effect on ASD symptoms. AUTHORS'
CONCLUSIONS: This review included data from only one study, which had methodological limitations. As such, no clinical trial evidence was found to suggest that pharmaceutical chelation is an effective intervention for ASD. Given prior reports of serious adverse events, such as hypocalcaemia, renal impairment and reported death, the risks of using chelation for ASD currently outweigh proven benefits. Before further trials are conducted, evidence that supports a causal link between heavy metals and autism and methods that ensure the safety of participants are needed.

Entities:  

Year:  2015        PMID: 26114777      PMCID: PMC6457964          DOI: 10.1002/14651858.CD010766.pub2

Source DB:  PubMed          Journal:  Cochrane Database Syst Rev        ISSN: 1361-6137


  53 in total

1.  Chelation for heavy metals (arsenic, lead, and mercury): protective or perilous?

Authors:  M J Kosnett
Journal:  Clin Pharmacol Ther       Date:  2010-07-21       Impact factor: 6.875

2.  Porphyrinuria in childhood autistic disorder: implications for environmental toxicity.

Authors:  Robert Nataf; Corinne Skorupka; Lorene Amet; Alain Lam; Anthea Springbett; Richard Lathe
Journal:  Toxicol Appl Pharmacol       Date:  2006-06-16       Impact factor: 4.219

3.  Change in autism symptoms and maladaptive behaviors in adolescents and adults with an autism spectrum disorder.

Authors:  Paul T Shattuck; Marsha Mailick Seltzer; Jan S Greenberg; Gael I Orsmond; Daniel Bolt; Sheilah Kring; Julie Lounds; Catherine Lord
Journal:  J Autism Dev Disord       Date:  2006-12-05

4.  Behavioral and emotional problems in young people with pervasive developmental disorders: relative prevalence, effects of subject characteristics, and empirical classification.

Authors:  Luc Lecavalier
Journal:  J Autism Dev Disord       Date:  2006-11

5.  A clinical trial of combined anti-androgen and anti-heavy metal therapy in autistic disorders.

Authors:  David A Geier; Mark R Geier
Journal:  Neuro Endocrinol Lett       Date:  2006-12       Impact factor: 0.765

6.  Diagnostic value of a chelating agent in patients with symptoms allegedly caused by amalgam fillings.

Authors:  J S Vamnes; R Eide; R Isrenn; P J Höl; N R Gjerdet
Journal:  J Dent Res       Date:  2000-03       Impact factor: 6.116

7.  A prospective study of mercury toxicity biomarkers in autistic spectrum disorders.

Authors:  David A Geier; Mark R Geier
Journal:  J Toxicol Environ Health A       Date:  2007-10

8.  Efficacy of DMSA Therapy in a Sample of Arab Children with Autistic Spectrum Disorder.

Authors:  Eleonor Blaucok-Busch; Omnia R Amin; Hani H Dessoki; Thanaa Rabah
Journal:  Maedica (Buchar)       Date:  2012-09

Review 9.  Chelation therapy for atherosclerotic cardiovascular disease.

Authors:  M V Villarruz; A Dans; F Tan
Journal:  Cochrane Database Syst Rev       Date:  2002

10.  The plausibility of a role for mercury in the etiology of autism: a cellular perspective.

Authors:  Matthew Garrecht; David W Austin
Journal:  Toxicol Environ Chem       Date:  2011-05-20       Impact factor: 1.437

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  7 in total

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Journal:  Clin Pediatr (Phila)       Date:  2019-04-02       Impact factor: 1.168

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Journal:  Mol Autism       Date:  2017-03-17       Impact factor: 7.509

5.  Assessing Risk of Bias in Randomized Controlled Trials for Autism Spectrum Disorder.

Authors:  Paola Matiko Martins Okuda; Cheryl Klaiman; Jessica Bradshaw; Morganne Reid; Hugo Cogo-Moreira
Journal:  Front Psychiatry       Date:  2017-11-29       Impact factor: 4.157

Review 6.  Evaluating Sensory Integration/Sensory Processing Treatment: Issues and Analysis.

Authors:  Stephen Camarata; Lucy Jane Miller; Mark T Wallace
Journal:  Front Integr Neurosci       Date:  2020-11-26

Review 7.  Practitioner's review: medication for children and adolescents with autism spectrum disorder (ASD) and comorbid conditions.

Authors:  Christian Popow; Susanne Ohmann; Paul Plener
Journal:  Neuropsychiatr       Date:  2021-06-23
  7 in total

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