Bridging the Biochemistry of Down Syndrome to that Seen in Autism

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Bri dging the bio chem is try of Do wn s yndr om e to that see n in autism
Implications for the understanding of autism in the general population.
Laurette Ja nak Autis m One May 2008 Email: la urette.ja nak@ver izo n.n et
Overview
 Description of Down syndrome  Why discuss Down syndrome at an autism conference?  Might Down syndrome children be more sensitive to mercury?  Down syndrome and mitochondrial dysfunction.  Cancer and vaccines; is there a connection?
Common knowledge about DS
• • • • Characteristic facial features Learning challenges Increased risk of leukemia Advanced aging with early development of Alzheimer’s disease But what actually IS Down syndrome?
Genetics of Down syndrome
Extra chromosome 21
Why shed light on DS at an autism conference?
A 1979 study was published showing the extremely rare condition of having both DS and autism.
J Autism Dev Disord. 1979 Mar;9(1):31-6
Twenty years later in 1999, a new study found at least 7% of DS children had autism.
Dev med Child Neurol 1999 Mar;41(3):153-8
By 2001 a study reported that autism in DS is “by no means rare”.
Dev Med Child Neurol 2001 Nov;43(11):750-4
Why shed light on DS at an autism conference?
Because the incidence of autism is so elevated in the DS population it is worth asking if there are any similarities between children with autism and DS. It is also interesting to ask what changed in the 20 years from a 1979 report of autism being rare in DS to the 1999 report of a 7% co morbidity.
Comparing DS and Autism
   Metabolic biomarkers of increased oxidative stress and 
impaired methylation capacity in children with autism.
                                                  Am J Clin Nutr. 2004 Dec;80(6):1611­7.
“The current study was prompted by a serendipitous observation in a previous study that the metabolic profiles of dizygotic twins--one with Down syndrome and one with autism--were virtually identical with respect to methionine cycle and transulfuration metabolites.”
Comparing DS and Autism
Gloria’s twins
Gloria’s twins Justin has autism Kyle has DS
Comparing DS and Autism

Homocysteine metabolism in Children with Down Syndrome: In Vitro Modulation.
– Am J. Hum Genet. 69:88-95, 2001
– Full text available at:
– http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pubmed&pubmed

Metabolic biomarkers of increased oxidative stress and impaired methylation capacity in children with autism.
– Am J. Clin Nutr 2004;80:1611-7 – Full text available at:
– http://www.ajcn.org/cgi/reprint/80/6/1611
Gene loca ted on Chr 21
methionine L SAM L
B12 MS
THF
SAH homocysteine L CBS cystathionine cysteine L GSH
GST
CH3-THF
(Methyl THF)
“L” represent s de cr eased levels i n bo th DS and AS D children compare d to contr ols. SOD
H2O2
GPx
GR
H2O
GSSG
Comparing DS and Autism
Important notes
Both the DS study and the ASD study looked at the biology of these two disorders. Both studies looked at biological interventions and were not designed to investigate improvement in DS or autism behaviors. Neither the DS or Autism study was designed to look at issues having to do with mercury. (more on the mercury issues shortly)
Chicken or the Egg
Autism
Oxidative stress
Chicken or the Egg
Early oxidative stress in amniotic fluid of
pregnancies with Down syndrome.
Clin Biochem. 2007 Feb;40(3-4):177-80
Tested the hypothesis that oxidative stress occurs early in DS pregnancies. Measured Isoprostanes (IPs) in the amniotic fluid of DS pregnancies as a marker of free radical damage to lipids. A 9-fold increase in IPs was found in the amniotic fluid of pregnancies with DS fetuses.
Chicken or the Egg
Conclusion: “The study reveals that oxidative stress occurs early in pregnancy and supports the idea of testing whether prenatal antioxidant therapy may prevent or delay the onset of oxidative stress diseases in the DS population.”
Early oxidative stress in amniotic fluid of pregnancies with Down syndrome
Clin Biochem. 2007 Feb;40(3-4):177-80
Chicken or the Egg

Might oxidative stress in pregnant woman contribute to the risk of autism in their offspring? To investigate this possibility we will first look at DS moms then mothers of children with autism.

Comparing DS and Autism

“A significant increase in plasma homocysteine concentrations and lymphocyte methotrexate cytotoxicity was observed in the mothers of children with Down syndrome, consistent with abnormal folate and methyl metabolism.”

Am J Clin Nutr. 1999 Oct;70(4):495-501.

Increased homocysteine is a risk factor for having a child with Down syndrome. Full text available at:
– http://www.ajcn.org/cgi/reprint/80/6/1611

methionine THF
B12 MS
SAM SAH H homocysteine H cystathionine cysteine ? GSH
GPx GST
CH3-THF
(Methyl THF)
“H” represents an increase in DS moms compared to controls. “?” = not measured. SOD
H2O2
H2O
? GSSG
GR
Comparing DS and Autism

Elevated homocysteine is a risk factor for neural tube defects.
 Report

of increase in NTD in DS families
Lancet. 2003 Apr 19;361(9366):1331-5.

This lends support to the idea that the mothers may have had elevated homocysteine (a marker of functional folate deficiency) prior to the conception of their DS baby.
Comparing DS and Autism

Let’s compare the biochemistry of the moms of children with DS to that of the moms with autistic children. 86 autism parents differ from 200 controls in the following:
 Higher

homocysteine  Higher SAH  Lower GSH (glutathione)  Increased GSSG (oxidized glutathione)  Unpublished data from the lab of Dr. Jill James
methionine THF
B12 MS
SAM SAH H homocysteine H cystathionine cysteine L GSH
GPx GST
CH3-THF
(Methyl THF)
High and low values of ASD parents compared to controls.
SOD
H2O2
H2O
H GSSG
GR
Comparing DS and Autism
46 Autistic Moms Homocsyteine SAH GSH GSSG 9.8 32.9 5.0 .32 200 Control Moms 7.4 23 7.3 .24
Personal correspondence with Dr. Jill James
Comparing DS and Autism

Is there any indication the elevated homocysteine found in the moms of autistic children may have existed prior to her pregnancy? Elevated homocysteine is associated with depression. Family histories of depression in autism.
 Am


J Psychiatry 1999 Apr;156(4):557-63
Comparing DS and Autism
Is there any evidence that alterations in homocysteine metabolism can increase the risk of having a child with autism? The antiepileptic drug Valproate has been used to induce an animal model of autism.



What does valproate do and how does this compare to the chemistry seen in the moms?
methionine THF
B12 MS
SAM SAH H homocysteine H cystathionine cysteine
CH3-THF
(Methyl THF)
Arrows indicate increases or decreases seen with valproate. Letters indicate increase or decrease in autism moms compared to control moms.
SOD
H2O2
GPx
L
GST
GSH
H2O
GSSG
H
GR
Comparing DS and Autism

There are many similarities between autism and the anticonvulsant syndrome seen in children whose mothers took valproate during pregnancy.

Fetal valproate syndrome and autism: additional evidence of an association Characteristics of fetal anticonvulsant syndrome associated autistic disorder. A clinical study of 57 children with fetal anticonvulsant syndromes. A new neurobehavioral model of autism in mice: pre- and postnatal exposure to sodium valproate. Maternal administration of thalidomide or valproic acid causes abnormal serotonergic neurons in the offspring: implication for pathogenesis of autism.




Comparing DS and Autism

I hypothesize the abnormal homocysteine metabolism seen in the moms of autistic children was present during her pregnancy and may act in a similar manner as valproate exposure. If so, I further suggest that this may have provided an in-utero environment of increased oxidative stress which might predispose toward autism when combined with additional postnatal oxidative stressors.

Mitochondria in Moms

Maternal hyperhomosysteinemia in animal models:
– Alters fetal brain development – Significantly reduced learning abilities in offspring – Caused increased lipid peroxidation in the brain of offspring (oxidative stress) – Increased brain DNA fragmentation in offspring

Folate deprivation promotes mitochondrial oxidative decay: DNA large deletions, cytochrome c oxidase dysfunction, membrane depolarization and superoxide overproduction in rat liver.
– Br J Nutr. 2007 May;97(5):855-63.
Mitochondria in Moms

J Biol Chem. 1998 Nov 13;273(46):30808-17.
– Study done in-vitro with human cells – “In this study, we demonstrate that homocysteine alters mitochondrial gene expression, function, and structure and provide evidence that homocysteine and H2O2 act synergistically to enhance mitochondrial damage.” – Inracellular glutathione was able to protect mitochondria from homocysteine and H2O2 induced damage. – Were study doses of homocysteine relevant?

Mitochondrial dysfuntion is well documented with valproate exposure.
– Elevated homocysteine – Low glutathione – Similar set up in moms of children with DS and/or ASD

Environmental exposures and infections can increase H2O2 production.
While you cannot have a genetic epidemic, dietary deficiencies can unmask a genetic predisposition to injury from an environmental exposure.
The percentage of energy from eating energy dense, nutrient poor foods was an independent positive predictor of serum homocysteine in adult Americans. Serum concentrations of vitamins A, E, C, and folate were inversely related to consumption of energy dense, nutrient poor foods. Am J Clin Nutr 2000;72:926-36
Comparing DS and Autism
Justin
Autism, tethered cord, tongue tied and hypothyroidism
Kyle
Down syndrome and hypothyroidism
Lauren
Celiac and JRA
Comparing DS and Autism
 
Twinning
 Increased
in both DS and ASD
Biochemistry
 In
DS and ASD children
– Decreased Methionine, SAM, Hcy, GSH – Increased GSSG
 In
DS and ASD moms
– Increased SAH and Hcy – Similar pattern seen in valproate exposure

Celiac
1
in 14 DS individuals have celiac  Reports of increased celiac in ASD families
– Does not appear to be supported by current studies
Comparing DS and Autism

Autoimmune disorders
 In
DS - increased occurrence of autoimmune disorders with target organs including pancreas, thyroid, joints, adrenal gland, gastric mucosa and brain.  In autism there is a familial presence of autoimmune diseases including pancreas, thyroid, joints, brain.
 
Zinc status
 Reports
of low zinc status in both DS and ASD
Thyroid disorders
 High
occurrence of antibodies to thyroid gland in DS  Familial autoimmune thyroid disease is a risk factor for ASD regression
– J Autism Dev Disorder 2006 Apr;36(3):317-24
Comparing DS and Autism
 Altered
 DS
immune system
– – – – –
Immune suppression Decreased NK cell activity Disruptions in CD4, CD8, and CD26 Decreased IL-2 T and B cell derangement
 Autism
– Immune system skewed toward Th2 – Decreased NK cell activity – Abnormal CD4/CD8 ratios
Comparing DS and Autism
 Response
 DS
to MethylB12
- in vitro study shows a positive metabolic response to MeB12  Autism - shows positive metabolic response to MeB12
 MeB12
 Be
has been shown to:
useful in RA  Increase NK cell activity  Positively alter the CD4/CD8 ratio  Increase methionine synthase activity
• My discussion on mercury can be extended to the many environmental exposures our high tech society has brought into our life. • This should not be construed into thinking I believe mercury is the sole cause of autism; as I do NOT believe that to be true. • I further believe that other components in vaccines (especially viruses) may be problematic for children with DS.
– Additional material is included for your consideration after my closing slide.
DS and environmental exposures
IOM 2004
With respect to the hypothesis that there may be a subgroup of children who are genetically more sensitive to the toxic effects of thimerosal (a mercury preservative found in vaccines), the IOM had this to say:
“This hypothesis cannot be excluded by epidemiological data from large population groups that do not show an association between a vaccine and an adverse outcome. Depending upon the frequency of the genetic defect, a rare event caused by genetic susceptibility could be missed even in large study samples.”
Glutathione Utilization
Over expressed in Down syndrome
cysteine
SOD
H2O2
GPx
L
GST
Detoxification of drugs and chemicals
GSH
GR
Up-regulated by metal exposure
H2O
GSSG
GSH: glutathione GSSG: oxidized glutathione GR: glutathione reductase GPx: glutathione peroxidase
GST: glutathione transferase SOD: superoxide dismutase H2O2: hydrogen peroxide
DS and Mercury
• Studies showing the overexpression of SOD and increased oxidative stress in Down syndrome are plentiful and predated the IOM 2004 investigation. • The fact that heavy metals (including mercury) increase oxidative stress and upregulate SOD was known prior to the IOM 2004 investigation.
DS and Mercury
• Studies showing decreased levels of GSH in DS predated the IOM 2004 investigation.
• J Pediatr. 2003 May;142(5):583-5. • Am J Hum Genet. 2001 Jul;69(1):88-95.
• It is a well established fact that mercury and other metals deplete GSH in a dose dependent manner. This fact has been shown in many studies that predated the IOM 2004 investigation.
• Immunopharmacol Immunotoxicol. 1993 Mar-Jun;15(23):273-90.
DS and Mercury
• An animal model of DS which showed decreased GSH in hippocampal neurons stated: – “Additional lowering of GSH levels led to enhanced cell death…..Based on these results we suggest that a GSH level which is decreased under a specific threshold by increased consumption, reduced synthesis or lack in precursor contributes to cell loss and neurodegneration in Down syndrome.”
– Brain Res 1997 Aug 15;765(2):313-8
DS and Mercury
• Animal models and human studies have found cholinergic dysfunction in DS.
• Eur J Neurosci. 2000 Sep;12(9):3259-64. • Brain Res. 1994 Sep 26;658(1-2):27-32. • Neurosci Lett. 1997 Feb 7;222(3):183-6.
• It has been shown that exposure to mercury can induce cholinergic dysfunction.
• J toxicol Sci 1979 Nov;4(4):351-62 • Res Commun Chem Pathol Pharm 1980 Nov;30(2):381-4 • Brain Res Dev Brain Res 1995 Mar 16;85(1):96-109
Mitochondria in DS
• It is extremely well documented that Down syndrome individuals have mitochondrial dysfunction. • The nature of this dysfunction is multifactorial & includes:
– Impaired mitochondrial enzyme activities
• • • • Cytochrome oxidase (complex IV) Isocitrate dehydrogenase (Krebs cycle enzyme) Decreased protein levels of complex I Decreased gene expression of ATPase6 (effects functioning of complex V)
Mitochondria in DS
– Accumulation of toxic free radicals
• Begins in-utero (Clin Biochem. 2007 Feb;40(3-4):177-80) – Studies on fetal DS brain and in fetal DS amniocytes demonstrate mitochondrial dysfunction occurs prior to birth.
• J Neural Transm Suppl. 2001;(61):109-16. • Mol Cells. 2003 Apr 30;15(2):181-5.
– DS mitochondria have a lower mitochondrial membrane potential which, is “underlying the presence of an increasing susceptibility of these organelles to damaging agents”.
• FEBS Lett. 2007 Feb 6;581(3):521-5. Epub 2007 Jan 17.
Mitochondria in ASD
• Nov. 9, 2007 the US. government conceded a vaccine-autism case in the Court of Federal Claims. • Claim: vaccinations aggravated an underlying mitochondrial disorder resulting in features of ASD. • Media Spin: this was an unusual case and mitochondrial disorders are rare.
Mitochondria in ASD
• As early as 1998, mitochondrial dysfunction was hypothesized to be related to autism.
– Autism: a mitochondrial disorder? Med Hypotheses. 1998 Jun;50(6):497-500
• Since that time, a number of other studies have noted this association in a subset of children with autism.
– – – – – – – – J Child Neurol. 2002 Jun;17(6):435-9. Ann Neurol. 2003 Jun;53(6):801-4. J Child Neurol. 2004 May;19(5):379-81. J Autism Dev Disord. 2004 Dec;34(6):615-23. Dev Med Child Neurol. 2005 Mar;47(3):185-9. J Autism Dev Disord. 2006 Nov;36(8):1137-40. J Child Neurol. 2007 Sep;22(9):1121-3. Dev Med Child Neurol. 2007 Oct;49(10):726-33.
Mitochondria in ASD
• “data suggest that further metabolic evaluation is indicated in autistic patients and that defects of oxidative phosphorylation might be prevalent.”
– Developmental regression and mitochondrial dysfunction in a child with autism.
• J Child Neurol. 2006 Feb;21(2):170-2. • Poling JS, Frye RE, Shoffner J, Zimmerman AW.
• It is estimated that up to 20% of children with autism may have mitochondrial disease.
http://osdir.com/ml/culture.autism/2005-07/msg00093.html
Mitochondria in DS/ASD
• What about DS children who are all known to have mitochondrial dysfunction that exists even before birth? • Are vaccines also aggravating the underlying mitochondrial dysfunction in DS children? • Might this explain the vastly higher incidence of autism among DS children?
Mitochondria in DS/ASD
• Recall from an earlier slide:
– DS mitochondria have a lower mitochondrial membrane potential which, is “underlying the presence of an increasing susceptibility of these organelles to damaging agents”.
• FEBS Lett. 2007 Feb 6;581(3):521-5.
• Can thimerosal be one of the “damaging agents” described above?
Mitochondria, mercury and homocysteine
• Mercury induces SOD and increases H2O2. The presence of homocysteine and H2O2 combined has been shown to cause mitochondrial damage. • Are study doses relevant to in-vivo findings? •
– J Biol Chem. 1998 Nov 13;273(46):30808-17.
• Who might have elevated homocysteine?
– – – – – Persons who use valproate Mothers of Down syndrome children Mothers of autistic children Persons with depression Persons with cardiovascular disease, etc. etc….
Mitochondria, mercury and homocysteine
• Has thimerosal (the mercury component found in flu vaccines) been tested for its ability to cause mitochondrial damage? • Thimerosal induces neuronal cell apoptosis by causing cytochrome c and apoptosis-inducing factor release from mitochondria.
– Int J Mol Med. 2005 Dec;16(6):971-7.
• Have thimerosal studies looked at vulnerable subsets such as Down syndrome children or persons with elevated homocysteine?
DS and Mercury
• Other abnormalities that are noted in DS and may be impacted by mercury exposure include:
• • • • Calcium dysregulation Alterations in glutamate metabolism Autoimmune disorders Leukemia
Cancer (DS, Autism & Mercury)
• Cancer/glutathione connection
– DS - low glutathione – Autism - low glutathione – Cancer - low glutathione levels can make people more sensitive to DNA damage from a variety of mutagenic environmental exposures. Thus, one might expect to see more cancer in both DS and autism.
Cancer (DS, Autism & Mercury)
• Cancer in DS and ASD – DS - it is well documented that children with DS have 15-20 fold increase occurrence of leukemia. – Autism - There is an increased mortality from cancer in individuals with autism.
– J Autism Dev Disord 2001 Dec;31(6)569-76 » (this was a small study)
– “We have seen the co-occurrence in families of autism and leukemia”
– NIH Autism Research Network
http://www.autismresearchnetwork.org/AN/IACC/wfAim.aspx?Aim=4
Cancer (DS, Autism & Mercury)
• Cancer in DS and ASD – It has been clearly demonstrated that mercury at low levels is a mutagen. – The mutagenic property of mercury has been shown to be causally related to its ability to induce H2O2.
– Environ Mol Mutagen 1998;31(4):352-61
– Therefore: children with low glutathione may be at higher risk for cancer from exposure to heavy metals and other environmental toxins.
Cancer (DS, Autism & Mercury)
• Mercury induces the formation of H2O2 via the enzyme CuZn-SOD which is overexpressed in DS.
• “The mechanism of carcinogenesis in Down syndrome could be explained by our findings: SODs enhance metalmediated DNA damage induced by H2O2. We conclude that SODs may increase the frequency of mutations due to oxidative DNA damage in cells, increasing carcinogenic potential.” » FEBS Lett. 2001 Apr 27;495(3):187-90.
A skillet study
• You pick up a hot skillet with your bare hands. • You yell and then drop it after 1 second. • Authorities say you have no damage to your hand because you only touched the pan for 1 second.
Thimerosal: A skillet study?
• Mercury levels in newborns and infants after receipt of thimerosal-containing vaccines.
– Pediatrics. 2008 Feb;121(2):e208-14 – Principle investigator: Michael Pichichero – Pichichero has served as a consultant to several vaccine manufacturers including GSK Biologicals, sanofi Pasteur, Wyeth Pharmaceuticals and MedImmune. – Study sought to compare the half-life of mercury in blood after receiving thimerosal containing vaccines (ethyl mercury) verses that of oral methyl mercury.
Thimerosal: A skillet study?
• Points of interest:
– Mandatory vaccines contained thimerosal.
• “Although considerable information is available regarding oral exposures to methyl mercury, relatively little is known about the pharmacokinetics of ethyl mercury, particularly when administered intramuscularly.”
– Findings: half-life in blood for thimerosal was 3.7 days while that of methyl mercury is 44 days.
• “The significant difference in blood half-life of intramuscular ethyl and oral methyl mercury suggests that exposure guidelines based on oral methyl mercury may not be appropriate for use in risk assessments of thimerosal in vaccines.” • “The importance of blood levels of ethyl mercury for assessing toxicity is unknown, but blood levels have been shown to be a predictor of toxicity for methyl mercury exposure.”
Thimerosal: A skillet study?
• “our measurements are unable to determine the fate of the mercury after it leaves the blood.” • A University of Rochester release quotes Pichichero as saying, “ Now it’s obvious that ethyl mercury’s short halflife prevents toxic build-up from occurring. It’s just gone too fast.” http://www.urmclabs.com/pr/news/story.cfm?id=1848 • Metaphoric implication: touching a hot skillet with your bare hands will not burn your skin because you only touched it for 1 second. We don’t need to look at your skin; it is undamaged because we said so.
MEDIA
“The findings bolster the argument that a mercury-based vaccine preservative doesn't cause autism in children”
Associated Press January 30, 2008 - 9:31pm
“WASHINGTON, Jan 30 (Reuters) - The mercury in a vaccine preservative is pumped out of a baby's body too quickly for it to do any damage, researchers reported on Wednesday in a study they say should further absolve shots of causing autism.” “New studies in infants show that the mercury used as a preservative in vaccines is cleared from the body at least 10 times faster than researchers had previously believed, a finding that casts further doubt on the theory that the preservative causes autism.” Los Angeles Times January 31, 2008
DS and Mercury
• Epidemiology vs biological studies
• IOM is correct; you cannot determine subgroups of mercury sensitive persons from large epi studies
• The biology of DS is consistent with what the medical literature indicates for increased toxicity with exposure to mercury. • If one group of genetically sensitive individuals is found, it is likely that there are others.
Future directions
» Conduct DS cell culture and animal studies to determine thimerosal sensitivity. » If increased sensitivity is found, a biological look at how thimerosal may contribute to autism in this highly susceptible group of children should be pursued.
Future directions
» Studies should be conducted by independent researchers with no conflict of interest. » Emphasis should be on biological mechanisms not epidemiology. » DS/autism studies should receive the same level of vigor as those of DS/Alzheimer’s and DS/leukemia.
How confident do I feel that sufficient mechanistic studies have been done on mandatory vaccines?
Thank you for touching my life!
Leukemia and vaccines
Vaccination history and risk of childhood leukaemia.
Int J Epidemiol. 2005 Oct;34(5):1100-9
Quote from the abstract: Vaccinations against DPT, tetanus, MMR, and polio “were not associated with the risk of leukemia.”
Quote from the full text: “It is possible that the present study had limited power in detecting an effect even if one was present because almost all children received these vaccines and followed very similar schedules"
Leukemia and vaccines
What does the media tell us?
Flu Jabs for mums-to-be to protect children from leukemia
by FIONA MACRAE and BOB OSMAN 24th October 2006
The following wording appeared below a picture of a pregnant women: “Cancer warning: Pregnant women will receive a flu jab because of a leukaemia risk to an unborn child.”
http://www.dailymail.co.uk/pages/live/articles/news/news.html?in_article_ id=412187&in_page_id=1770&ct=5
Leukemia and vaccines

Maternal illness and drug/medication use during the period surrounding pregnancy and risk of childhood leukemia among offspring.
Am J Epidemiol. 2007 Jan 1;165(1):27-35

Media jumps to false conclusion
 
The study did not even mention the word “vaccine”. Study acknowledges:  the problem of recall bias  influenza was self-reported; not laboratory confirmed  3 other studies (2 based on medical records) found no association or a decreased risk of leukemia with maternal influenza surrounding pregnancy
Leukemia and vaccines

Other concerns include:

Contamination of MMR with avian leukosis virus (ALV) from being attenuated on chicken eggs

Working in chicken slaughter houses is a risk factor for leukemia.

Chromosomal breaks have been documented in patients receiving attenuated measles vaccine.

Am J Hum Genet. 1966 Jan;18(1):81-92
Leukemia and vaccines

Other concerns include:

“Patients with Down’s syndrome show more chromosomal breaks after virus infection than do normal control subjects.”

Pediat Res 7: 582-587 (1973)

“It is determined that antimeasles vaccination causes considerable changes in the leucocyte chromosome apparatus of children affected with Down’s syndrome not affecting any cytogenetic structure of healthy children.” N. N. Ilyinskikh 1981 Leukamoide Reaktion oder Leukose nach MMRSchutzimpfung translates to “Leukemoid reaction or leukosis after MMR preventive vaccination”


Kinderaztl Praxis 61(1993) 118-119
Leukemia and vaccines

Other concerns include:

“Further study is essential to unveil the exact mechanism of the clastogenic action of different vaccines on the hereditary materials of the inoculated organisms.”

Int J Genet, 3(1): 51-58 (2003)

Do upcoming vaccines undergo testing on the clastogenic properties of the vaccine prior to public release?
Leukemia and vaccines

sanofi pasteur


Influenza Virus Vaccine, H5N1
HIGHLIGHTS OF PRESCRIBING INFORMATION
http://www.fda.gov/cber/label/h5n1san041707LB.pdf




Safety and effectiveness have NOT been established in pregnant or lactating women, and in pediatric and geriatric populations. Each dose contains 50 ug mercury; you get 2 doses over a 28 day time frame. The clinical trials used an “investigational” vaccine that did NOT contain any mercury. “Influenza Virus Vaccine, H5N1, has NOT been evaluated for carcinogenic or mutagenic potential, or for impairment of fertility.”

great info. I think I shall

great info.

I think I shall send it to a friend.

Thank you

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