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Autism, mercury and cover up???



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  #91  
Old Aug 25, 2005, 02:12 PM
mercyteapot's Avatar
I Like Pie&VDO
Join Date: Sep 2003

Originally Posted by judyblueeyes
Autistic 5-year-old dies during chelation.

The Pittsburgh Tribune-Review has reported that a 5-year-old boy went into cardiac arrest and died during chelation therapy for alleged lead and mercury toxicity. [Hasch M. Autistic boy, 5, dies after disputed therapy. Pittsburgh Tribune Review, Aug 26, 2005] http://pittsburghlive.com/x/tribune-.../s_367277.html
Chelation therapy for autism is a fraud. The state police and county coroner are investigating the boy's death.
I read this. Tragic.

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  #92  
Old Aug 25, 2005, 09:19 PM
Registered User
Join Date: Jul 2005

terrible. i heard it was an allergic reaction to the drug. the IV-EDTA is used for lead removal-which is FDA approved.

but this is why i used homeodetox on my child, rather than IV chelation therapy.

now if only all those deaths caused by vaccination would receive as much attention, we'd be getting somewhere.
http://www.medalerts.org/vaersdb/


Last edited by barbara44 : Aug 25, 2005 at 11:13 PM.
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  #93  
Old Aug 25, 2005, 11:52 PM
Registered User
Join Date: Jul 2005

1. Between 1990-2000, 186 reported deaths from Ritalin:

http://www.ritalindeath.com/

2. Children's deaths from vaccines, as recorded by the CDC:
(Keep in mind that, according to the FDA, only 10 percent of vaccine reactions/deaths are reported, so the number is probably much higher)
Chickenpox vaccine 1995-1998:
Between March 17, 1995 and July 25, 1998, 6580 adverse events -
including 14 deaths - were reported to the Vaccine Adverse Events
Reporting System in association with varicella vaccination---
Pediatric News 33(3):12, 1999.

For DPT vaccine 12,504 reports VAERS reports with 144 deaths per year
(1990-1993)
"In a year-long investigation of the Vaccine Adverse Reaction
Reporting System (VAERS) operated by the Food and Drug
Administration, NVIC/DPT analyzed VAERS computer discs used by the
FDA to store data on reports of deaths and injuries following DPT
vaccination. A total of 54,072 reports of adverse events following
vaccination were listed in a 39-month period from July 1990 to
November 1993 with 12,504 reports being associated with DPT vaccine,
including 471 deaths."Campaign Against Fraudulent Medical Research
(CAFMR)

MMR vaccine VAERS reports 7 deaths per year (1990-1994):
"From July 1990 thro' April 1994, 5799 ADRs following MMR vaccination
were reported to US Vaccine Adverse Events Reporting System (VAERS);
including 3063 cases requiring emergency medical treatment, 616
hospitalisations, 309 who did not recover, 54 children left disabled
and 30 deaths."--- John P Heptonstall

For OPV vaccine there were VAERS reports of 108 deaths per year over
a 5 year period.
"We commissioned an OPV Vaccine Report and started making all kinds
of other inquires. The OPV Vaccine report that we received was a
shocking report. It covered a recent period a little less than 5
years and the following is the summary for that period: The number of
Vaccine Associated events that occurred: 13,641 ..The number of
events resulting in death 540"--The Polio Connection of America &
Polio vaccine victims: http://village.ios.com/~w1066/poliov6.html

For Hep b vaccine there were VAERS reports of 54 deaths per year
(1990-98)
"The total 24,775 VAERS hepatitis B reports from July 1990 to October
31, 1998 show 439 deaths and 9673 serious reactions involving
emergency room visits, hospitalization, disablement or death."--
Michael Belkin http://www.whale.to/vaccines/belkin1.html

"Since July 1990, 17,497 cases of hospitalizations, injuries and
deaths in America following hepatitis B vaccination have been
reported to the Vaccine Adverse Event Reporting System (VAERS) of the
U.S. government. This figure includes 146 deaths in individuals after
receiving only hepatitis B vaccine without any other vaccines,
including 73 deaths in children under 14 years old. In 1996 alone
there were 872 serious adverse events in children under 14 years old
reported to VAERS. 658 of those injuries were following hepatitis B
vaccination in combination with other vaccinations and 214 of these
injuries were after hepatitis B vaccination alone. In these children
under 14 years old, there were 35 deaths after hepatitis B
vaccination in combination and 13 deaths after hepatitis B
vaccination alone, for a total of 48 deaths. Compare these statistics
with the total number of hepatitis B cases nationwide reported that
same year (1996) in children under 14, just 279, and the conclusion
is obvious that the risks of hepatitis B vaccination far outweigh its
benefits."---Incao's Hepatitis B Vaccination Testimony

"If adverse drug reactions were tabulated as a cause of death, this would be
between the fourth leading and sixth cause of death In the United States."
Sources: Centers for Disease Control Fastats estimated 2000 causes of death;
To Err Human, National Institute of Medicine, 1999; Bates et al., Incidence
of adverse drug events and potential adverse drug events. JAMA 274:29, 1995;
Porter. Jick, Drug-related deaths among medical inpatients. JAMA
237:879-281, 1977."

http://www.drugintel.com/pharma/cause_of_death.htm


Last edited by barbara44 : Aug 26, 2005 at 12:04 AM.
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  #94  
Old Aug 27, 2005, 06:32 PM
Registered User
Join Date: Jul 2005

Autism and Chelation: Where is the Science?
Nearly four years ago, the Institute of Medicine recommended
research into chelation therapy and autism. But that never happened,
and now a little boy in Pennsylvania is dead.

The heartrending tragedy of Abubakar Tariq Nadama, an autistic five-
year-old who died while undergoing chelation this week, is one of
the saddest chapters in the very sad saga of autism in America.

But even as the grieving immigrant mother makes funeral arrangements
for her beloved boy, opponents of the theory that drew the family to
America (the theory that mercury triggers autism, and removing it
through chelation may improve symptoms) are holding his death up as
proof that the idea is bogus. They claim that the use of chelation
to treat autism is foolishly dangerous, and should be shut down at
once.

Some people have come perilously close to exploiting this tragedy to
further their own political or personal agendas. Some blame the
boy's death on his mother, who has been labeled as reckless
and "desperate." Others blame the Pennsylvania doctor -- and any
autism doctor willing to try chelation (the use of certain chemicals
to remove heavy metals from the body) – for the tragedy. Some fault
me, for writing a book that dared to include the topic of chelation
and autism within its pages.

It's time to take a deep breath and look at the facts.

First of all, only an autopsy will reveal the actual cause of death,
and I think it is prudent to wait before jumping to any conclusions
about the general safety of chelation and autism. That said, the boy
did die while undergoing the procedure, and it's possible the
controversial treatment is what killed him.

But here is where things get more complicated. Abubakar was given a
substance known as EDTA, and he was receiving it intravenously. EDTA
is used mostly (and legally, I might add) for the treatment of lead
poisoning. EDTA is not typically used in mercury cases, and it is
not clear why it was used to treat autism here.

In fact, I am unaware of any autistic child who's been chelated with
EDTA, nor am I familiar with any autism cases where IV chelation was
employed. The chelation methods I have written about (I do not, and
cannot recommend treatments, for the record, I only report on them)
were either oral or trans-dermal, and they used substances that are
significantly different than EDTA.

Furthermore, I cannot find any reference in the medical literature
about any patient dying from chelation. (Please post them if you
have them).

Does chelation therapy work? We just don't know. Could it be
dangerous, even deadly, for children with autism? Perhaps, but
there's no hard science available one way or the other. And if
chelation does improve symptoms, what are the best agents, at what
doses and timing, and through which route of administration? No one
can say, of course, because no one has bothered to study these
questions in double-blinded trials.

Which brings us back to the IOM recommendation of 2001. The
committee assigned to look into thimerosal (the mercury containing
vaccine preservative) noted that some autism practitioners
report "clinical improvements following chelation." And though the
committee said that chelation "is not a benign treatment," it
nonetheless recommended "careful, rigorous, and scientific
investigations of chelation when used in children with
neurodevelopmental disorders, especially autism."

That report was issued on October 1, 2001, nearly four years ago.
But few paid attention to the recommendation, and no one did the
hard science on chelation. This left parents and doctors flying half-
blind in pursuit of chelation -- not out of "desperation," but out
of strong evidence their children had suffered from mercury exposure.

Just think, if the government had listened to the very IOM report it
commissioned back in 2001, we might know a lot more about chelation
and autism than we know today. If clinical trials had gotten
underway then, we would know with certainty whether chelation could
heal, or kill.

If hard scientific proof had been uncovered that chelation was 100-
percent worthless in the treatment of autism, no parent or doctor
would still be pursuing the therapy today. If evidence had surfaced
in clinical trials that children could be harmed or even killed by
chelation, no one would be using it today. The doctor in
Pennsylvania would have halted chelation therapy long ago, and this
poor grieving family would never have crossed the ocean from the UK
in pursuit of its false promise.

But what if the opposite were true? What if the "rigorous science"
recommended by the IOM had yielded proof that chelation can indeed
help some kids -- provided that it's done with the safest agents, at
the safest doses, and through the safest routes of administration
(not to mention in combination with other therapies)?

Either way, if America had done its scientific homework, as
recommended by its top science professors, Abubakar might still be
alive today.

If chelation is quackery that kills, let's outlaw it today. But if
it can be done safely, with demonstrated clinical benefit to some
autistic patients at a minimum of risk, then it should be approved
by the FDA for the treatment of autism.

Does chelation in autism kill or cure? Only hard science will answer
that question. What a shame we have wasted four long years not
finding out.

http://www.huffingtonpost.com/david-...and-chelation-
whe_b_6286.html

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  #95  
Old Aug 27, 2005, 06:43 PM
mercyteapot's Avatar
I Like Pie&VDO
Join Date: Sep 2003

Thank you, barbara, for posting these stories.


Last edited by mercyteapot : Aug 28, 2005 at 09:55 AM.
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  #96  
Old Sep 10, 2005, 10:44 PM
Registered User
Join Date: Sep 2005
Autism/Mercury toxicity

Originally Posted by Seren21
Well, why do some kids get autism and some don't? They all get the shots. Do vaccines even still have thimerosol in them? Is this still a problem today?
Well I have heard in addition to the mercury toxicity one or both parents have an auto- immune disorder. You can ask why some get autism and some don't. I worked with mercury toxic patients. Some were really sick others mildly sick and the range of mercury varied no correlation? It effects everyone differently. I did see children with "autism" improve when the mercury was taken out by DMPS chelation. The other chelation is EDTA which is used for lead toxicity and is much more dangerous. I don't know the facts of the child that died. I only saw progress with the patients treated for "autism"
Amy

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  #97  
Old Oct 06, 2005, 01:28 PM
Spidey's mom's Avatar
SAHM wannabe
Join Date: Dec 2002

A friend who knows the scientist involved in the following study sent this to me and I found it fascinating and hopeful. Genetics studies are close to finding the causes of autism and linked diseases and also possible cures or treatments.

Here is the link:

http://www.boston.com/news/science/a...agile_promise/


Here is another article -

http://web.mit.edu/giving/spectrum/s..._progress.html

steph


Last edited by Spidey's mom : Oct 06, 2005 at 01:32 PM.
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  #98  
Old Oct 06, 2005, 04:09 PM
Registered User
Join Date: Sep 2005
Thanks

interesting


Originally Posted by stevielynn
A friend who knows the scientist involved in the following study sent this to me and I found it fascinating and hopeful. Genetics studies are close to finding the causes of autism and linked diseases and also possible cures or treatments.

Here is the link:

http://www.boston.com/news/science/a...agile_promise/


Here is another article -

http://web.mit.edu/giving/spectrum/s..._progress.html

steph

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  #99  
Old Oct 07, 2005, 04:05 AM
Senior Member
Join Date: Oct 2004

Originally Posted by stevielynn
A friend who knows the scientist involved in the following study sent this to me and I found it fascinating and hopeful. Genetics studies are close to finding the causes of autism and linked diseases and also possible cures or treatments.

Here is the link:

http://www.boston.com/news/science/a...agile_promise/


Here is another article -

http://web.mit.edu/giving/spectrum/s..._progress.html

steph
Hey guys,

Just wanted to say thanks for this forum, my son has Autism.

I am going to look at hormonal influence and autism. I have several scientific articles if anyone is interested as part of my literature review (for my dissertation, I am a PhD neuroscience student). PM me if yu want them.

Mike

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  #100  
Old Oct 07, 2005, 09:31 AM
Registered User
Join Date: Sep 2005
Research

You may want to research Glutathione.
Amy


Originally Posted by mwbeah
Hey guys,

Just wanted to say thanks for this forum, my son has Autism.

I am going to look at hormonal influence and autism. I have several scientific articles if anyone is interested as part of my literature review (for my dissertation, I am a PhD neuroscience student). PM me if yu want them.

Mike

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Autism, mercury and cover up???

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