Last Updated:  Sep 25, 2009   

Mom and Dad	Sam, Jesse, Daddy, Ashley and Stevie
Stevie and Sammy (First school pic)	Stevie, Jesse, Ashley, Dad and Sam.

Welcome to our website. We are the Gillespie family...Steven Sr., Michelle,  Ashley, Jesse and twins, Stevie Jr. and Samuel Noah. Our three older children are now young adults. Amanda is in the army, recently married and is currently stationed in Washington. Amanda and her husband are currently serving in Iraq. Christopher attends Towson State. Gregory is in the army and is deployed to Afghanistan. Please visit us at our other websites located at;   www.caringbridge.org/visit/samuelandstevengillespie  and

http://themanyfacesofautism.blogspot.com/

You can also read an article regarding our family at, http://www.examiner.com/a-125244~Walk_for_Autism_research_raises_awareness_of_condition.html   

AUTISM STATISTICS.

Here are some stats on autism today: Did you know....... 1 in 150 children are diagnosed with autism. 1 in 104 boys are on the autism spectrum 67 children are diagnosed per day A new case is diagnosed almost every 20 minutes More children will be diagnosed with autism this year than with Aids, diabetes and cancer COMBINED Autism costs the nation over $90 billion per year, a figure expected to double in the next decade Autism is the fastest-growing serious developmental disability in the United States. Autism receives less than 5% of the research funding of many less prevalent childhood diseases There is no medical detection or cure for autism Boys are four times more likely to have autism than girls INCIDENCE VS. PRIVATE FUNDING Leukemia affects 1 in 25,000/ funding:$310 million Muscular Dystrophy affects 1 in 20,000/ funding: $175 million Pediatric Aids affects 1 in 8,000/ funding:$394 million Juvenile Diabetes affects 1 in 500/ funding: 4310 million Autism affects 1 in 150 / Funding : $15 million.  NATIONAL INSTITUTES OF HEALTH FUNDS ALLOCATION Total 2005 NIH budget $29 billion Of this only $100 million goes towards autism research. This represents only 0.3% of the total NIH funding!

Our twins, Steven Jr. and Samuel were diagnosed with Mercury Induced Autism . *Stevie and Sammy were   NOT born with Autism. They recieved 2 flu vaccines containing Thimerosal 27 days apart (at the tender age of 6 months then again at just shy of 7 months) by our "previous" pediatrician. Mercury aka Thimerosal is the second known neurotoxin to man. [The CDC says on it's website that "mercury is a neurotoxin and to avoid eating fish because it may contain mercury. They state as an example a person weighing 110 pounds should have no more than 5 micrograms of mercury." The flu vaccine contains 25 micrograms of mercury. You need to weigh at least 550 pounds for this vaccine to be safe.] Had someone told us this, in the winter of 2004, our boys would have NEVER recieved these shots! Do the research...[MERCURY WAS TAKEN OUT OF ANIMAL VACCINES OVER 10 YEARS AGO!]

Ashley is now in the 12th grade in the "Lifeskills" program at her local high school. Ashley's favorite interests are art, music and learning sign language. Ashley's art can be seen throughout our home. Ashley enjoys a variety of music including but not limited to Carrie Underwood, Rascal Flatts, Akon, Fergie and Reba. She also enjoys Highschool Musical, Bratz and soap operas. Jesse  is now in the ninth grade and is in the Protective Services program at YCST. Jesse enjoys swimming and playing XBOX 360. Both Ashley and Jesse help quite a bit with their twin brothers. Stevie and Sammy are currently in an "Autistic Support" classroom. Both are adjusting well. The twins' currently see many medical professionals due their complicated medical issues. They are currently being worked up for a mitochondrial/metabolic disorder. We are hoping for answers in the near future.

*** We owe a great deal of gratitude to the following people who are currently involved in the twins' care; Susan Brousseau (Director of Special Education), Brenda Hartman and Dawn Dull (LIU, Autistic Support) Missy Skimski; (Bev, Pam and Amanda) with ValleyView Center. Sara Czolba with Gateway Healthcare. Allison Laird with MHMR/Autism side. Cindy Corbin with MHMR. Dr. Amanda Pearl, Dr. Dorgan, Dr. Musunuri and Michele O. with Philhaven Center for Autism and Developmental Disabilities. Dr. Ventura, Kristen, Val, Shelley, Tracey and Keesha with Pediatric Health Associates. Dr. Benny Kerzner with Children's National in D.C. (G.I.) Dr. Shapiro (ENT) Andrea Raffensberger with the ARC of York County***

 Stop in and sign our guest book and let us know what you think...you may also email us anytime with questions regarding this information and if we do not know the answer, we will direct you to someone who does gillespies62599@msn.com    & can you please remember to vote for our site so we stay on the "most favorites list." Thank you.   

David Kirby

Is Aluminum the New Thimerosal?
By Robert W. Sears
Issue 146, January/February 2008

Vaccines have become the most controversial parenting topic of the decade. When parents are considering whether or not to vaccinate their children, one of the things that must be considered is aluminum toxicity.

Aluminum is added to a number of vaccines to help them work better. Normally, one wouldn't consider aluminum to be a problem. It's a naturally occurring element that is present everywhere in our environment-in food, water, air, and soil. It's also a main ingredient in over-the-counter antacids. And because the body doesn't absorb aluminum, it's harmless when swallowed.

I didn't think much about aluminum when, 13 years ago, I began researching vaccines. In fact, the early seminars on vaccine education that I offered to parents included a brief statement that aluminum was nothing to worry about. But as I read each product insert and saw the number of micrograms (mcg) of aluminum contained in several vaccines, I wondered, "Has anyone determined what a safe level of injected aluminum actually is?" I didn't have to wonder for long, because the answer is easy to find; go to www.fda.gov, search on "aluminum toxicity," and you'll find several documents about aluminum.

The first document I came across discusses the labeling of aluminum content in injected dextrose solutions (the sugar solutions added to intravenous fluids in hospitals): "Aluminum may reach toxic levels with prolonged parenteral administration [ i.e., injected into the body] if kidney function is impaired. Research indicates that patients with impaired kidney function, including premature neonates [ i.e., babies], who received parenteral levels of aluminum at greater than 4 to 5 micrograms per kilogram of body weight per day, accumulate aluminum at levels associated with central nervous system and bone toxicity. Tissue loading [ i.e., toxic buildup in certain body tissues] may occur at even lower rates of administration." ¹ For a tiny newborn, this toxic dose would be 10 to 20 mcg; for an adult, it would be about 350 mcg.

The second document discusses aluminum content in IV feeding solutions, or Total Parenteral Nutrition (TPN) solutions. The FDA requires these solutions to contain no more than 25 mcg of aluminum per liter of solution. A typical adult in the hospital would get around 1 liter of TPN each day, thus about 25 mcg of aluminum. The FDA document also states, "Aluminum content in parenteral drug products could result in a toxic accumulation of aluminum in individuals receiving TPN therapy. Research indicates that neonates and patient populations with impaired kidney function may be at high risk of exposure to unsafe amounts of aluminum. Studies show that aluminum may accumulate in the bone, urine, and plasma of infants receiving TPN. Many drug products used routinely in parenteral therapy may contain levels of aluminum sufficiently high to cause clinical manifestations [ i.e., symptoms]. . . Aluminum toxicity is difficult to identify in infants because few reliable techniques are available to evaluate bone metabolism in premature infants. . . Although aluminum toxicity is not commonly detected clinically, it can be serious in selected patient populations, such as neonates, and may be more common than is recognized." ²

Elsewhere, I found a relevant 2004 statement by the American Society for Parenteral and Enteral Nutrition (ASPEN), a group that monitors oral and injectable nutritional products for safety and side effects. It reiterated the cited FDA warnings to the letter, and recommended that doctors purchase IV products with the lowest aluminum content possible, "and should monitor changes in the pharmaceutical market that may affect aluminum concentrations." ³

The source of the daily limit of 4 to 5 mcg of aluminum per kilogram of body weight quoted by the ASPEN statement seems to be a study that compared the neurologic development of about 100 premature babies who were fed a standard IV solution that contained aluminum, with the development of 100 premature babies who were fed the same solution with almost all aluminum filtered out. The study was prompted by a number of established facts: that injected aluminum can build up to toxic levels in the bloodstream, bones, and brain; that preemies have decreased kidney function and thus a higher risk of toxicity; that an autopsy performed on one preemie whose sudden death was otherwise unexplained revealed high aluminum concentrations in the brain; and that aluminum toxicity can cause progressive dementia. The infants who were given IV solutions containing aluminum showed impaired neurologic and mental development at 18 months, compared to the babies who were fed much lower amounts of aluminum. Those who got aluminum received an average of 500 mcg of the metal over a period of 10 days, or about 50 mcg per day. The other group received only about 10 mcg of aluminum daily-4 to 5 mcg per kilogram of body weight per day. ⁴ This seems to be the source of this safety level.

However, none of these documents or studies mentions vaccines; they look only at IV solutions and injectable medications. Nor does the FDA require labels on vaccines warning about the dangers of aluminum toxicity, although such labels are required for all other injectable medications.

All of these studies and label warnings seem to apply mainly to premature babies and kidney patients. What about larger, full-term babies with healthy kidneys? Using the 5 mcg/kg/day criterion from the first document as a minimum amount we know a healthy baby could handle, a 12-pound, two-month-old baby could safely receive at least 30 mcg of aluminum per day. A 22-pound one-year-old could receive at least 50 mcg safely. Babies with healthy kidneys could probably handle much more than this, but we at least know that they can handle this much. However, these documents don't tell us what the maximum safe dose would be for a healthy baby or child, and I can't find such information anywhere. This is probably why the ASPEN group suggests, and the FDA requires, that all injectable solutions be limited to 25 mcg; we at least know that that level is safe.

Calculating Aluminum in Vaccines
Here are the current levels of aluminum per shot of the following vaccines, as listed on each vaccine's packaging:

• DTaP (for Diphtheria, Tetanus, and Pertussis): 170-??625 mcg, depending on manufacturer
• Hepatitis A: 250 mcg
• Hepatitis B: 250 mcg
• HIB (for meningitis; PedVaxHib brand only): 225 mcg
• HPV: 225 mcg
• Pediarix (DTaP-??Hepatitis B-??Polio combination): 850 mcg
• Pentacel (DTaP-??HIB-??Polio combination): 330 mcg
• Pneumococcus: 125 mcg

In other words, a newborn who gets a Hepatitis B injection on day one of life would receive 250 mcg of aluminum. This would be repeated at one month with the next Hep B shot. When, at two months, a baby gets its first big round of shots, the total dose of aluminum could vary from 295 mcg (if a non-aluminum HIB and the lowest-aluminum brand of DTaP are used) to a whopping 1225 mcg (if the Hep B vaccine is given along with the brands with the highest aluminum contents). These doses are repeated at four and six months. With most subsequent rounds of shots, a child would continue to get some aluminum throughout the first two years. But the FDA recommends that premature babies, and anyone with impaired kidney function, receive no more than 10 to 25 mcg of injected aluminum at any one time.

As a medical doctor, my first instinct was to worry that these aluminum levels far exceed what may be safe for babies. My second instinct was to assume that the issue had been properly researched, and that studies had been done on healthy infants to determine their ability to rapidly excrete aluminum. My third instinct was to search for these studies. So far, I have found none. It's likely the FDA thinks that the kidneys of healthy infants work well enough to excrete aluminum before it can circulate through the body, accumulate in the brain, and cause toxic effects. However, I can find no references in FDA documents that show that using aluminum in vaccines has been tested and found to be safe.

So I did what any pediatrician would do. I turned to the American Academy of Pediatrics (AAP), who in 1996 published a policy statement, "Aluminum Toxicity in Infants and Children," that made the following points:

• Aluminum can cause neurologic harm.
• A study from 30 years ago showed that human adults increase their urine excretion of aluminum when exposed to higher levels of the metal, which suggests that adults can clear out excess aluminum.
• Adults taking aluminum-containing antacids don't build up high levels of aluminum in their bodies.
• Reports of infants with healthy kidneys show elevated blood levels of aluminum from taking antacids.
• People with kidney disease who build up bloodstream levels of aluminum greater than 100 mcg per liter are at risk of toxicity.
• The toxic threshold of aluminum in the bloodstream may be lower than 100 mcg per liter.
• The buildup of aluminum in tissues has been seen even in patients with healthy kidneys who receive IV solutions containing aluminum over extended periods. ⁵

To put this in perspective: Because the body of the average adult contains about 5 liters of blood, receiving more than 500 mcg of aluminum in the bloodstream all at once will be toxic if the kidneys aren't working well. (Toxicity has also been seen in patients with healthy kidneys.) Because a newborn's body contains about a liter (300 milliliters) of blood, more than 30 mcg of aluminum floating around in the bloodstream could be toxic if the baby's kidneys aren't working well. The body of a toddler or preschool-age child contains about 1 liter of blood, so more than 100 mcg in his system could be toxic-and, as we've seen, babies can receive more than 1000 mcg of injected aluminum all at one time. Fortunately, this amount doesn't all go into the blood at once, but is slowly diffused into the bloodstream over a period of time from the muscle or skin where it was injected.

But that is the main point of this article. No one has measured the levels of aluminum absorption by the bloodstream when it is injected into the skin and muscle of infants, or the levels of excretion from the body via urination. All of the FDA and AAP documents that I've read state that aluminum might be a problem, but that they haven't studied it yet, so we should limit the amount of aluminum included in injectable solutions. But, again, no one is talking about the levels of aluminum in vaccines.

What I think may have happened is that because aluminum used to be found in only one vaccine-DTP, an older version of the current DTaP vaccine-no one thought much about it. Then, in the 1980s, the PedVaxHib brand of HIB meningitis vaccine was released, which also included aluminum; but other brands of HIB vaccine did not, so again, no one thought much about it. In the 1990s, the Hepatitis B vaccine began to be widely used; in the 2000s, the Pneumococcus vaccine; and, more recently, the Hepatitis A vaccine. Administering one aluminum-containing vaccine at a time involves only a small amount of the metal; administering four such vaccines simultaneously is a different story. It seems this issue has simply escaped everyone's attention. Or has it?

Limited Studies limit thinking
Several years ago, some suspected cases of aluminum toxicity resulted in various neurologic and degenerative problems. The Cochrane Collaboration, a group that studies health-care issues around the world, wanted to look at a very large study group to see if there was a real correlation between neurologic problems and the aluminum in vaccines. They investigated all the reported side effects of one aluminum-containing vaccine, DTP (no longer used), and looked for any evidence that such vaccines caused more side effects than non-aluminum vaccines. Other than more redness, swelling, and pain at the injection site, they found no indication that an aluminum-containing vaccine caused any more problems, and concluded that no further research should be undertaken on this topic. ⁶ That is a very bold statement. Most researchers will draw conclusions from the findings of their own research; it's unusual to say that no one else should do any more research into the matter.

This is especially surprising because of the limitations of the Cochrane Collaboration's study. They looked at the effects of only one standard aluminum-containing vaccine, rather than the effects of all four being administered at once. They didn't study aluminum metabolism itself. They didn't test aluminum levels in children after vaccination, nor did they explore whether or not the amount of aluminum in vaccines builds up in the brain or bone tissues. They looked only for evidence of external symptoms of aluminum toxicity, not internal effects. Nor did they do their own research; instead, they reviewed all available studies conducted by other investigators. Despite all this, the Cochrane Collaboration study essentially closed the book on investigating aluminum toxicity from vaccines, without really having opened it in the first place.

The most obvious way to study this matter would be to inject various amounts of aluminum into children and see what happens to them internally. We know from the FDA documents that aluminum toxicity does occur from other types of injectable treatments; that it accumulates in the brain and bones in toxic amounts; that this may occur more commonly than is recognized; and that aluminum toxicity is hard to detect by looking for external symptoms. The question remains: What happens when these amounts of aluminum are injected via vaccines? Vaccine manufacturers may have begun to wonder about the same thing; I found some interesting research in the product insert of the new HPV vaccine, Gardasil. In researching the safety of Gardasil, Merck & Co., Inc., the vaccine's developer and manufacturer, added a step to their testing procedure by injecting aluminum into a separate group of test subjects used as a safety control group. They then compared the side effects of the Gardasil vaccine with a saline placebo that contained neither Gardasil nor aluminum, as well as with the placebo containing no Gardasil but the same amount of aluminum as the vaccine. They found that the placebo containing aluminum was much more painful than the saline placebo, and about as painful as the full HPV shot. The aluminum placebo also caused much more redness, swelling, and itching than the saline placebo, though not quite as much as the full HPV shot.

Unfortunately, Merck looked only at the effects of aluminum at the injection site. Nor did they state in the Gardasil product insert what role the aluminum placebo played in all the other standard side effects, such as fever and flu-like symptoms. Nor did they study the body's internal metabolism of aluminum. However, their research did show how irritating aluminum can be when injected into the muscles. It was a good first step. If aluminum can be toxic, why not just remove it from vaccines, as is being done with the preservative thimerosal, which contains the neurotoxin mercury? It's not that simple. Aluminum is an adjuvant; in other words, it helps vaccines work more effectively. When the metal is mixed with a vaccine, the body's immune system more easily recognizes the vaccine and creates antibodies against the disease. Thimerosal was easy to omit, because it has nothing to do with the efficacy of the vaccine itself. But the pharmaceutical companies would need good evidence that aluminum is harmful before they would invest in coming up with new, aluminum-free vaccines. (The Cochrane Collaboration report pointed out that removing aluminum from vaccines would then require extensive trials of the reformulated vaccines. ⁷)

What, exactly, does a toxic level of aluminum do to the brain? While no one has studied healthy babies to see how much, if any, aluminum builds up in the brain from the amounts of aluminum used in vaccines, the study on IV feeding solutions in premature babies mentioned above revealed that aluminum impaired their neurologic and mental development. ⁸ But that was in premature babies, not healthy, full-term infants. I found several animal studies involving aluminum and/or aluminum-containing vaccines that did show neurologic harm. Not only did aluminum build up in the brain and cause damage, but some of the damage looked similar to what is seen in the brains of Alzheimer's patients. ^{9-13 14} However, it's hard to draw conclusions about aluminum's effects on humans from studies of animals. What we need are more studies of human infants.

A Call for Better Research
There is good evidence that large amounts of aluminum are harmful to humans. Because no meaningful research has specifically been done on aluminum in vaccines, there is no existing evidence that the amount in vaccines is harmful to infants and children. However, no one has actually studied aluminum levels in healthy human infants after vaccination to make sure it is safe. Should we now stop and research this matter? Or should we just go on, continuing to hope that it is safe to use aluminum as an adjuvant in vaccines?

Vaccine policy makers and advocates may read this article, review my perspective, and initiate research studies to explore the risks of aluminum. I would hope that those researchers do not conduct a retrospective review of all the old vaccine safety studies and journal articles to look for the side effects of aluminum. As the FDA, AAP, and others have stated, aluminum toxicity can't be detected by external observation alone. It would be a waste of time, and a grave disservice to the health of America's children, to have several such reports show up in the medical literature. The only way the issue of aluminum safety can be put to rest is to conduct real-time studies on thousands of infants and measure aluminum levels after vaccination.

In such a study, the researchers should look not only at blood levels. They should also find out whether or not aluminum accumulates in the body, where it accumulates, how the body eliminates it, and at what rate. Once I see such research, and have determined to my satisfaction that aluminum has been proven safe, I will post an update on www.thevaccinebook.com, and revise future editions of the book accordingly. If such research finds that aluminum may not be safe, then I would expect a new vaccine schedule to be adopted in which the administering of vaccines is spread out to minimize the amount of aluminum a child receives at any given time. I would also expect vaccine manufacturers to begin finding ways to reduce or remove aluminum from vaccines without compromising their effectiveness. We need to know the answers to many questions: Why does one brand of HIB vaccine require aluminum to make it work while another brand does not? Why does one brand of DTaP vaccine contain four times as much aluminum as another?

Learning from the Past
I worry that aluminum may end up being another thimerosal. I am relieved that, as of 2002, the mercury-containing preservative had been removed from most vaccines. But according to an article in the Los Angeles Times, Merck & Co., the makers of several vaccines, knew in 1991 that the cumulative amount of mercury in vaccines given to infants by six months of age was about 87 times the level then thought to be safe.14 The article includes a copy of an internal memo, written by one of Merck's research doctors and sent to the president of Merck's vaccine division, clearly stating the doctor's worry about mercury overload. What was done with that information back in 1991? We'll never know. What we do know is that vaccine manufacturers knew that we were overdosing babies, but that the mercury wasn't removed from vaccines until 10 years later. This was because few paid attention to the potential problems with mercury. When we did find out, we hoped it wasn't harmful, we did extensive research to try to show that it wasn't, and we slowly removed it from most vaccines.

The issue of mercury toxicity from vaccines is moot for infants receiving vaccines today, as long as doctors and parents choose a flu shot without mercury, know which brands of vaccines still contain barely detectable traces of mercury, and are aware that some plain Tetanus and Diphtheria-Tetanus vaccines still contain mercury (though these last vaccines are not parts of the routine vaccine schedule). [ For a current list of vaccines and their thimerosal contents, go to  www.vaccine safety.edu/thi-table.htm-Ed

What isn't moot is the question of aluminum toxicity. As doctors, we can choose certain vaccine brands that contain less or no aluminum. We can be careful about giving only one aluminum-containing vaccine at a time. And we can talk about it instead of sweeping the issue under the rug. I pray that my fears about aluminum are unfounded, and that objective studies performed by completely independent groups with no ties to vaccine manufacturers or political organizations show that it is safe. If not, I would hope that manufacturers would start to reduce or eliminate the aluminum content of their vaccines as soon as possible. I know this won't be an easy task, but our children are worth it.

Excerpted from The Vaccine Book ? 2007 by Robert Sears, MD. Reprinted by permission of Little, Brown and Company. New York, NY. All rights reserved. For more information, see www.thevaccinebook.com . For the notes to this article, see www.mothering.com/ articles/growing_child/vaccines/aluminum-new-thimerosal-notes.html 

http://www.lifesitenews.com/ldn/printerfriendly.html?articleid=09072106

 

Tuesday July 21, 2009

Is Aborted Fetal DNA in Vaccines Linked to Autism?

 

 

By Theresa A. Deisher, Ph.D.

July 21, 2009 (LifeSiteNews.com) - Just when the pharmaceutical industry thought the vaccine-autism controversy had been resolved, the National Vaccine Advisory Committee has recommended further study of vaccine safety. A perceived fear of the safety of the U.S. vaccination schedule has led increasing numbers of parents to opt out of full compliance. The numbers of children who are not fully vaccinated has now reached a point where "herd" immunity may be compromised, compelling the Centers for Disease Control to hold town-hall meetings and convene a Vaccine Safety Working Subgroup. Despite research ruling out mercury (Thimerosal) or the measles portion of one specific vaccine, autism continues to rise to a level of one in every 64 children in the UK.

The NVAC draft report recommends further study of the potential for vaccines to contribute to autism in children who have underlying mitochondrial disease, a worthwhile study given the clinical history of such children developing autism after vaccinations (see Poling case). What the NVAC has overlooked, however, in their recommendations, is that epidemic regressive autism is associated with the switch from using animal cells to produce vaccines to the use of aborted human fetal cells for vaccine production. Now when we vaccinate our children, some vaccines also deliver contaminating aborted human fetal DNA. The safety of this has never been tested.

Autism and autism spectrum disorder are polygenic diseases, meaning that multiple genes have been shown to be associated with these diseases. Studies have also clearly shown that there is an environmental component, a trigger, that is required. Vaccines are an obvious potential environmental trigger for autism because of the almost universal childhood exposure to vaccines in first world countries. The vaccine-autism connection was first hypothesized following the introduction of a new measles, mumps and rubella (MMR) vaccine to the U.S. in 1979, with complete U.S. market share by 1983, and to the UK in 1988. Autism rates began to rise in the U.S. after 1979 and rose dramatically after 1983, and likewise rose in the UK after 1988, leading physicians to suspect a link. Initially, the measles component of this vaccine, MMR II, was suspected to be the culprit. Subsequent studies have also focused on the presence of mercury in vaccines, which incidentally, the MMR II vaccine did not contain.

Those studies have largely ruled out the new measles portion of the MMR II or mercury as the environmental trigger for autism. However, the compelling temporal association between this new MMR vaccine and autism cannot be ignored or explained away. What has been ignored is the fact that this new MMR vaccine introduced the use of aborted fetal cells for vaccine production. At one point, as much as 94 percent of children in the U.S. and 98 percent of children in the UK were given this vaccine.
Today, more than 23 vaccines are contaminated by the use of aborted fetal cells. There is no law that requires that consumers be informed that some vaccines are made using aborted fetal cells and contain residual aborted fetal DNA. While newer vaccines produced using aborted fetal cells do inform consumers, in their package inserts, that the vaccines contain contaminating DNA from the cell used to produce the vaccine, they do not identify the cells as being derived from electively aborted human fetuses.

In other words, they tell you what is in the vaccine, but they don't fully inform you where it came from. The earliest aborted fetal cell-produced vaccines such as Meruvax (rubella) and MMR II do not even inform consumers that the vaccines contain contaminating DNA from the cell used to produce them. Furthermore, it is unconscionable that the public-health risk of injecting our children with residual contaminating human aborted fetal DNA has been ignored.

How could the contaminating aborted fetal DNA create problems? It creates the potential for autoimmune responses and/or inappropriate insertion into our own genomes through a process called recombination. There are groups researching the potential link between this DNA and autoimmune diseases such as juvenile (type I) diabetes, multiple sclerosis and lupus. Our organization, Sound Choice Pharmaceutical Institute (SCPI), is focused on studying the quantity, characteristics and genomic recombination of the aborted fetal DNA found in many of our vaccines.

Preliminary bioinformatics research conducted at SCPI indicates that "hot spots" for DNA recombination are found in nine autism-associated genes present on the X chromosome. These nine genes are involved in nerve-cell synapse formation, central nervous system development and mitochondrial function.

Could genomic insertion of the aborted fetal DNA, found in some of our childhood vaccines since 1979, be an environmental trigger for autism? Could the fact that genes critical for nerve synapse formation and nervous system development are found on the X chromosome provide some explanation of why autism is predominantly a disease found in boys? Could the "hot spots" identified in these autism-associated genes be sites for insertion of contaminating aborted fetal DNA?

These questions must be answered, and quickly. Recent literature suggests that autism spectrum disorder may now impact one out of every 100 children. The pharmaceutical industry is also currently moving to replace more animal-produced vaccines with aborted-fetal-cell production and also to produce biologic drugs using aborted fetal cells.

The practice of using aborted fetal cells for vaccine and drug production creates wrenching moral dilemmas for parents and consumers, ignores informed consent rights, and exposes our children and ourselves to contaminants lacking safety evaluations. We cannot ignore this issue in good conscience, and we cannot afford to wait.

(Dr. Deisher is president of Sound Choice Pharmaceutical Institute (www.soundchoice.org), as well as a cofounder and the research and development director for Ave Maria Biotechnology Company (www.avmbiotech.com), which promote pro-life biotechnology. This article is an adaptation and update of SCPI's June 2009 newsletter and is published with its kind permission.)

 

URL: http://www.lifesitenews.com/ldn/2009/jul/09072106.html

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02/26/2008

LES INCOMPETANTS: OPEN LETTER TO THE AAP

By K. Paul Stoller, M.D.

"Diet, injections, and injunctions will combine, from a very early age, to
produce the sort
of character and the sort of beliefs that the authorities consider
desirable, and any serious
criticism of the powers that be will become psychologically impossible.
Even if all are
miserable, all will believe themselves happy, because the government will
tell them that
they are so."

-Bertrand Russell, The Impact of Science on Society p50, 1953

As a pediatrician, who has been a fellow of the AAP for two decades, I find
the AAP's
approach to the autism epidemic to be deeply disturbing.

Not only have they allowed the myth of better diagnosing (as the reason for
all the notice
given to affected children) to be perpetuated, but when they were put on
notice at the
CDC's Simpsonwood meeting in 2000, that the mercury in the pre servative
Thimerosal
was causing speech delays and learning disabilities, they obfuscated and
hide that
information. They never made good on their 1999 pledge to have Thimerosal
eliminated
from vaccines and almost a decade later joined in the protest against a
fictitious TV show
(Eli Stone) because it was critical of mercury being in vaccine.Out of 132
million doses of
the worthless1 flu vaccine for the 2007-08 flu season, 8 million doses are
Thimerosal
free. That means 94% contain the full amount of Thimerosal.

If a pregnant woman got a flu shot in 2001 and her child followed the flu
shot
recommendations, the baby/fetus would have received six flu shots with the
full amount
of Thimerosal by the year 2005.

Today, flu vaccine for those under 3 year of age supposedly do not contain
Thimerosal,
but with no government agency testing vaccines for mercury, the only ones
who know
whether these Thimerosal f ree vaccine (flu or otherwise) actually are
mercury free are the
manufacturers themselves.

Vaccines with "trace" amounts of Thimerosal are supposed to contain less
than 1
microgram of mercury per 0.5 ml dose (1 microgram (ug) Hg per 0.5 ml is the
same as 2
ug Hg per ml which is the same as 2000 ug/liter. Micrograms per liter is
parts per billion
[ppb]2)

0.5 parts per billion (ppb) mercury = Kills human neuroblastoma cells
(Parran et al.,
Toxicol Sci 2005; 86: 132-140).

2ppb mercury = U.S. EPA limit for drinking water
(   http://www.epa. gov/safewater/ contaminants/ index.html# mcls  )

20 ppb mercury = Neurite membrane structure destroyed (Leong et al.,
Neuroreport 2001;
12: 733-37).

200 ppb mercury = level in liquid the EPA classifies as hazardous waste
( http://www.epa. gov/epaoswer/ hazwaste/ mercury/regs. htm#ha zwaste )

25,000 ppb mercury = Concentration of mercury in multi-dose, Hepatitis B
vaccine vials,
administered at birth from 1991-2001 in the U.S.

50,000 ppb mercury = Concentration of mercury in multi-dose DTP and
Haemophilus B
vaccine vials, administered 8 times in the 1990's to children at 2, 4, 6,
12 and 18 months
of age. Current "preservative" level mercury in multi-dose flu,
meningococcal and tetanus
(7 and older) vaccines.

For years the Infectious Disease division at the CDC (and others) have said
the reason for
the dramatic increase in autism is due to "better diagnosing" and "greater
awareness."
They have encouraged those like the AAP to manufacture uncertainty by
publishing articles
that were less than truthful. The AAP shamefully played along, perhaps
encouraged by the
largesse of vaccine manufacturers who significantly contribute to the AAP's
yearly budget.

There is another budget to co nsider for eighty percent of autistic
Americans under the age
of 18, and we will soon begin to see a dramatic impact on Social Security
in coming years
as these children become dependent adults. There are no studies that have
found the
previously undiagnosed or misdiagnosed autistic individuals among older
Americans. They
simply aren't there. So what is coming will significantly impact on society.

As there are no genetic epidemics, which leaves an epidemic linked to some
sort of
exposure. Now, the increase of autism has been linked to the increase in
mercury
exposure through fish and industrial sources, amalgam and additionally,
through
increased parenteral exposure to Thimerosal - no controlled, randomized
study regarding
the safety of amalgam or Thimerosal exists.

A recently released Scientific Consensus Statement on Environmental Agents
Associated
with Neurodevelopmental Disorders (by the Collaborative on Health and the
Environment' s
Learning and Developmental Disabilities Initiative) concludes that
environmental
contaminants are an important cause of learning and developmental
disabilities.

Delayed detoxification of mercury severely impairs methylation reactions
(required for the
correct expression of DNA, RNA, and neurotransmitters) , which further
adversely affects
growth factor derived development of the brain and attention abilities.
Phospholipid
methylation, which is crucial for attention, is impaired in autistic and
attention deficit
hyperactivity disorders.

In a first analysis of the VSD datasets, Verstraeten (et al) had described
a 7.6 to 11.4 fold
increase of autism risk in children at one month, with the highest mercury
exposure levels
compared to children with no exposure. In four subsequent separate
generations of the
analysis, which involve the exclusion of children with no Thimerosal exposure and less
than two polio vaccines, the statistical significance disappeared. This is
what was
published by the AAP even though they knew the truth. How did they know the
truth?

Again, they were presented at the Simpsonwood meeting in June 2000, a
meeting that
was illegal to hold. No Federal agency is allowed to call a meeting
together with
representatives of private industry (all the vaccine manufacturers were
represented at this
meeting) without opening the meeting to the public.

Thimerosal was tested only once, by Eli Lilly on 22 adult patients
suffering from
meningitis. There was no chance for follow- up to observe long-term
effects, as all of the
patients in this "study" died. Even if follow-up had been possible, damage
to the
developing brains of very young children would have remained an unknown.
Eli Lilly said it
was safe and the medical community accepted it. After the creation of the
FDA, its use was
simply continued. The federal government has never tested the type of
mercury in
vaccines for toxicity. This is an unconscionable oversight failure at best,
at worse it is an
example that we have left consensus reality to be created by the liars,
thieves, cheats,
killers, and the junk scientists they employ.

How it came to pass the AAP joined these rogues and became an active
participant in this
skullduggery is beyond reason - is even beyond greed. They have remained
silent as
mercury laden vaccine continue to be exported and used in all third world
and second
world countries.

We are living in a time where an incredible overplay and lies and
self-aggrandizing
behavior and non-science is the norm. We have tolerated the junk science
that has
covered up the true cause of this epidemic at a considerable cost to
science, the public,
and our very way of life in this country. Is it stretch to realize that by
putting our collective
heads in the sand about the autism epidemic we have made it possible for
the destruction
of our very civilization?

Not something easy to contemplate? Then ask why haven't pediatricians come
forward to
demand the end of the use of Thimerosal once and for all, and to advocate
for the
treatment of these children before it is too late? Why are they not at the
front of the line
protesting the amounts of mercury allowed to come out of coal-fired power
plants? Why
aren't they leading the charge to stop the use of mercury amalgam dental
fillings that are
placed in the mouths of young children and pregnant women?

The very Federal agencies that should have been sounding the alarm bell about
environmental pollution creating future generations of mentally disabled
citizens did less
than remain silent because they have become arms of the very corporations
that profit
from sel ling and distributing poisons. Just look who sits on the FDA's
Scientific Advisory
Boards - the conflicts of interest are so glaring as to suggest that the
FDA has become a
trade arm of big pharma.

Nevertheless, the hand writing is on the wall as the US government has
quietly conceded a
vaccine-autism case in the Court of Federal Claims.3 Pediatricians will no
longer be able
to hide behind the skirts of "Standard of Care" if they are giving autistic
children heavy-
metal laden vaccines. That is only one step away from giving vaccines and
making normal
children autistic.

The AAP should proactively be bringing in risk management specialists and
be proactive
towards how this could affect pediatricians in civil litigation for
following the CDC
recommendations on vaccinations after a diagnosis of any type of
neurodevelopmental
delay in a child. This is what they are afraid of and this is what the law
of attra ction will
bring in upon the AAP and the minions of those that just followed the
recommendations
and drank the Kool-Aid that Big Pharma wanted them to drink.

For all the above reasons, I will no longer enable the AAP to be party to
the damage that is
being done to the world's children by sending in my dues for a third
decade. It is a token
protest, but it has to begin with someone.

1 BMJ 2006;333:912- 915 (28 October), doi:10.1136/ bmj.38995. 531701.80

2 http://www.ajph. org/cgi/eletters /AJPH.2007. 113159v

3 http://www.huffingt onpost.com/ david-kirby/ government- concedes-
vacci_b_88323. html

K. Paul Stoller, MD is the President of International Hyperbaric Medical
Assoc and Medical
Director of the Hyperbaric Medical Center of New Mexico.

WHY THE AUTISM SPEAKS BLACKOUT ON JENNY AND DAN!?

http://www.ageofautism.com/2008/04/why-the-autism.html

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