MERCURY,
SMALLPOX VACCINES,
AND DEATH BY WORLD HEALTH ORGANIZATION DESIGN
Here is something to consider carefully before having you kids vaccinated with smallpox vaccine. There is one rather morbid but practical consideration. If you decline to vaccinate your kids and yourself, and if as many as 70% of the population comply and are vaccinated, you chances of getting smallpox are greatly reduced. This is because all those people who were vaccinated will not pass the disease to you since they will be immune and not get sick. Thus, you will have only a chance to be infected by 30% of the population or less. Of this 30%, only possibly 20% will get sick and be contagious. Figure the odds, and let the wicked and ignorant take the risks.
The single most deadly aspect of using vaccines is the consideration that immunity is easily acquired by getting the disease in childhood. Obviously, there are several diseases one does NOT want to get, but many of the common diseases, like measles, chicken pox, and mumps, are very minor on a child. If the child is protected from the disease by a vaccine, yet later the child gets the disease, the affects in an adult of most of these childhood diseases is horrific. Shingles in an adult is far more terrible than chicken pox in a child. Whooping cough in a teen or young adult male will often result in sterility. The Salk vaccine has proven to be a deadly blessing to certain people, and the vaccine itself should be reinvented. It is a medical killer weapon all too often. So, parents must weigh the choices very carefully.
In retrospect, let us not be mindlessly reactionary. Polio is obviously a terrible disease, and any SAFE way of eradicating it would be a great blessing. Also, I would NEVER go to the equatorial world without getting cholera and yellow fever vaccinations. The side effects and the risk of contamination at the manufacturer, are far less worrisome than to actually get the diseases, and do NOT let anyone tell you that cholera is not deadly, and do NOT let them tell you that it is less an issue today than in the past. With Third World cities growing to enormous population numbers, and sanitation getting WORSE rather than better in most Third World nations, you do have a very good chance of getting sick there. Cholera can be cured very easily, IF you receive antibiotics and IV fluids within 24 hours of contracting the disease. If you can get the antibiotics, but the IV is far away, YOU WILL DIE. A baby, after contracting cholera, will die in as little as eight hours. There is nothing you can do but stand and watch the fluids run our of his rectum like a faucet running.
Again, in retrospect, and to show how confusing this is, the vast majority of statistics on deaths by small pox, and other diseases that can kill the victim, are from Bangladesh and Africa. This is due to lack of medical resources and poverty of governments. The cause of death with many small pox diseases is from complications like electrolyte imbalance and skin rashes which become infected. This would never happen in the USA. Also, the statistics are VERY old, and they take NO consideration for the modern antibiotics and even invasive mechanical methods of keeping a patient alive. These resources were NOT available in the 1930s through 1950s when much of the data now in use was gathered. So, the horror statistics are very faulty, for we have not had one small pox epidemic since about 1970 anywhere on earth. Also, if cholera were to break out in the USA, it would be contained easily due to the Federal coffers which would quickly be used to buy only two simple things-- very common antibiotics and fluid IVs. The statistics on cholera are absolutely useless if we are talking about the USA. If you are traveling to Bangladesh, the story is 1000% the opposite.
The best thing you can do about these fearful diseases is the following:
1. Quarantine YOUR own family and home so you don't infect other people.
2. Do not go to the hospital where other diseases can easily be contracted and weaken the little immune system you already have.
3. Call a doctor to make a house call and diagnose the disease.
4. Demand immunization of all other family members at once.
This was done in India and Bangladesh and an epidemic was stopped. You may have to shop for a medical provider to help you since most doctors are supercilious fools and believe all the official information provided them by the Federal Health sources. Remember, it was Dr. Everett Koop who told us the AIDS was not dangerous to women, that it could not be passed by using public toilets, and that heavy kissing was not dangerous. Time has made a wretched fool of the idiot. He killed many stupid gullible fools who acted upon his advice. So, shop for medical help until you find someone who has a brain. In the Southwest USA, this may be as simple as a ride across the border to Mexico.
So, let us weigh the evidence against the pharmaceutical companies who will kill you if they can make a dollar doing it, and consider that fact against the risk. If the risk is low, or exposure in childhood is actually a better choice, then help your child GET the minor diseases so they will have the immunity to go through life disease free. If a real killer is on the loose, get the vaccination and ask God for mercy from the NWO and drug peddlers.
Here is how serious the WHO is about their obsession with your child. I for one do NOT believe this is all being done out of pure compassion. I know that small pox vaccine was laced with AIDS virus for the sole purpose of killing off most of Africa, and high placed US officials master minded it. I can prove that the Aspen Institute and Henry Kissinger have called for the reduction of the world's population "by pestilence." The following is the most frightening paragraph in the article with follows below.
Vaccine researchers are seeking $500 million from all the world's governments to create a genetically engineered "supervaccine" that will be given orally at birth. This supervaccine - the CDC and CVI call it the "Holy Grail" - will contain raw DNA from 20 to 30 viruses, parasites, and bacteria that will insert itself directly into the cells of babies. The vaccine will be time-released over several months. Disease organisms scheduled to be included in the supervaccine, many containing multiple strains or types of each virus, bacteria, or parasite, are pneumonia (three viruses), AIDS (two viruses), dengue haemorrhagic fever (four viruses), diarrheal disease (several viruses and bacteria), diphtheria, hepatitis, malaria (two parasites), measles, meningitis (six viruses and bacteria), polio (three viruses), schistosomiasis (one parasite), tuberculosis, typhoid fever, and pertussis.
This from a reader:
From: Stumpy
Date: Wednesday, July 17,
2002 16:42:39
To: Stumpy Patriot
Subject: think vaccines/methyl mercury
are good? you might be surprised...
I especially recommend reading "Vaccine Scene 2000.htm," which I found at www.woodmed.com. It's rather long, but quite a comprehensive eye-opener. It has great information as a basis for research on thimerosal and mercury levels in mass government- mandated vaccination programmes. Share this information with anybody who has or will have children receiving vaccinations or anyone you know who receives influenza shots.
This sure opened my eyes to many of the vaccinations that are mandated by many governments in many countries. And given the following positive step from France's health minister, I wouldn't trust the World Health Organization judging by their immediate next-day response either:
"Government officials have also been on the defensive since last October, when France became the first country to end hepatitis B vaccine requirements for schoolchildren. France's health minister acted after numerous reports of arthritis- and multiple sclerosis-like symptoms. Pending citizen lawsuits against SmithKline Beecham and Pasteur-Merieux, which make and sell the hepatitis B vaccine, may also have influenced the French decision. In addition, attorneys representing 15,000 French citizens are suing government health officials for understating the vaccine's risks and exaggerating its benefits.
The day after France withdrew the vaccine mandate, a dismayed World Health Organization stated that "the decision taken yesterday may lead to loss of public confidence in this vaccine, and decisions by other countries to suspend or delay introduction of hepatitis B vaccine. . . . WHO strongly recommends that all countries already using hepatitis B vaccine as a routine vaccine in their national immunization programs continue to do so, and that countries not yet using the vaccine begin as soon as possible."
Vaccinations are big business and big revenue for well-known companies like Merck, Eli Lilly, and Pasteur-Merieux.
"Mercury is widely known to cause neurological damage, often permanent. Current clinical and epidemiological research suggests that the mercury-laden thimerosal so widely given to children by the drug companies in the 1990's might cause a range of neurological and neurodevelopmental injuries, including autism. Compounding this public health disaster is that the toxic exposure was entirely avoidable. The thimerosal was added merely as product packaging for the multi-dose vials, and is not needed as a preservative when the vaccines are packaged in single-dose vials or single-use syringes. Thimerosal had nothing to do with vaccine safety, and everything to do with the profits and convenience of packaging for the pharmaceutical companies."
It would make any normal person wonder why the government does not demand thimerosal- free vaccines and does not demand that the mercury levels are eliminated or reduced to safe levels.
There are also very high levels of methyl mercury in some fish. "The Food and Drug Administration (FDA) is announcing its advice to pregnant women and women of childbearing age who may become pregnant on the hazard of consuming certain kinds of fish that may contain high levels of methyl mercury. The FDA is advising these women not to eat shark, swordfish, king mackerel, and tilefish. As a matter of prudent public health advice, the FDA is also recommending that nursing mothers and young children not eat these fish as well. Fish such as shark, swordfish, king mackerel, and tilefish contain high levels of a form of mercury called methyl mercury that may harm an unborn baby's developing nervous system. These long- lived, larger fish that feed on smaller fish accumulate the highest levels of methyl mercury and therefore pose the greatest risk to the unborn child. Mercury can occur naturally in the environment and it can be released into the air through industrial pollution and can get into both fresh and salt water. (January 12, 2001)"
From the US Food and Drug Administration's Center for Food Safety and Applied Nutritition, Office of Seafood (May 2001):
Table 1
Fish With Highest Mercury
Levels
SPECIES MEAN (PPM) RANGE (PPM) NO. OF SAMPLES
Tilefish 1.45 0.65-3.73
60
*Swordfish 1.00 0.10-3.22 598
King Mackerel 0.73 0.30-1.67 213
*Shark 0.96 0.05-4.54 324
Vaccine Scene 2000: |
---|
Date: 01/01/2000 |
SOURCE:
Woodlands Healing Research Center Family,
Environmental & Preventive Medicine
5724 Clymer Rd.
Quakertown, PA 18951
215-536-1890
800-517-9545
Fax 215-529-9034
Email: foffice@woodmed.com
Web Page- http://www.woodmed.com
Introduction:
We are frequently asked our opinion and position on vaccination in both children
and adults. This lengthy monograph is an attempt to express a minority view and
position that is contrary to current government, public and medical opinion on
the subject. However, whatever position on the vaccination decision one chooses
to adopt, we feel the under riding, most important point is Parental Choice! Therefore,
we ardently believe the best approach to this very controversial subject is to
present both the pro and con, good and bad, known and unknown about immunizations
and then help guide the patient or parents to choose what is best for them or
their children. This is termed "informed consent" and should be the
basis of every medical test or treatment; vaccinations being no exception. Consequently,
our Healing Research Centers honor and respect the patient's or parent's choice
in this matter and will immunize or not immunize accordingly.
Any medical therapy must balance the "effectiveness" versus the "safety"
of its actions on the human body. For instance, aspirin therapy is effective in
preventing a second heart attack after having a first heart attack and it is quite
safe, only having a very small incidence of stomach or intestinal bleeding as
a potential long-term side effect. As you read the following monographs, please
keep these key points in mind in terms of "effectiveness" versus the
"safety" of vaccinations:
In early August of this year Congressional hearings were held in Washington D.C.
dealing with questions of vaccine safety. Congressman Dan Burton, Chairman of
the U.S. House Government Reform Committee, called the hearings. On the weekend
of October 2nd and 3rd, 1999, an autism conference was held at Cherry Hill, New
Jersey, sponsored by the Autism Research Institute of San Diego, California. Over
l,000 people were in attendance, the great majority of whom were parents of autistic
children. At one point in the meeting, when those parents who thought their child's
autism was caused by vaccines were asked to stand, a large majority of the audience
stood. With these and other indications of growing public concerns about current
childhood immunization programs, it is hoped that this review will be of timely
interest.
Inadequate
Proof of Benefit of Vaccines
It is true that there may be situations where extreme
measures may be justified to preserve life and health as the lesser of two evils.
The basic question, therefore, is whether the benefits of current childhood vaccines
outweigh the harm, or whether the reverse is true. As to the benefits of vaccines,
polio has been eliminated from the Western Hemisphere; smallpox may have been
eliminated worldwide, although there are disturbing reports that it is still to
be found in parts of the Far East.
Vaccine proponents would have us believe that vaccines have been largely responsible
for controlling virtually all of the former epidemics of killer diseases in the
U.S.A. With the exceptions cited above, the facts do not bear this out. According
to the records of the Metropolitan Life Insurance Company, from 1911 to l935 the
four leading causes of childhood deaths from infectious diseases in the U.S.A.
were diphtheria, pertussis (whooping cough), scarlet fever, and measles. However,
by l945 the combined death rates from these causes had declined by 95%, before the implementation of mass immunization programs1. By far the greatest factors in this decline were sanitation
through public health measures, improved nutrition, better housing with less crowded
conditions and the introduction of antibiotics. Also, the virulence of microorganisms
tends to become weakened or attenuated with the passage of time and serial passages
through human hosts2, one example of which is whooping cough (pertussis) which
is clearly a much milder disease today in Western nations than it was l00 or so
years ago3.
Safety
Not Proven
It should be pointed out that today's children receive
22 or more vaccines before school age, whereas today's senior citizens received
only one, the smallpox vaccine. Some of these vaccines contain mercury, although
the impact of this potentially toxic metal remains unknown as concerns the vaccines.
With growing public concerns about potential adverse reactions of these heavy
burdens of foreign immunologic materials on the immature immune systems of children,
it is reasonable to ask ourselves what is known about these reactions.
A small but growing minority of physicians and scientists are becoming aware that safety testing for the various vaccines has been woefully inadequate. As one of many examples, a l994 special committee of the National Academy of Sciences published a comprehensive review of the safety of the hepatitis B vaccine. When the committee, which carried the responsibility for determining the safety of vaccines by Congressional mandate, investigated five possible and plausible adverse effects, they were unable to come to conclusion for four of them because they found that relevant research had not been done4.
The clear implication of this and other revelations5 concerning a general deficiency of safety testing in the vaccine field, especially as concerns possible long-term side effects, is that adverse reactions may be taking place on a large scale without being recognized as to their true nature.
There is a school of thought that the so-called minor childhood illnesses of former times, including measles, mumps, rubella (German measles) and chicken pox), which entered the body through the mucous membranes, served a necessary and positive purpose in challenging and strengthening the immune system of these membranes6. In contrast, so the theory goes, the respective vaccines of these diseases are injected by needle directly into the system of the child, thereby bypassing the mucosal immune system. As a result, mucosal immunity remains relatively weak and stunted in many children, complications of which may be the rapid increase in asthma and eczema now being seen, both in terms of frequency and severity7.
This concept tends to be confirmed by four controlled studies, widely separated geographically, in which vaccinated children were found to have significantly more atopic disorders than controls8, 9, 10, 11. In commenting on the increased incidence of asthma and other atopic disorders in the United Kingdom in the article, "Measles and atopy in guinea-Bissau," cited above, the authors made the following comment:
"The rise of allergic disease among children in the UK over the past 30 years remains unexplained. One hypothesis is that infections in early childhood prevent allergic sensitization, and that successive generations of children have lost his protection as their exposure to infectious disease in early life has declined. Consequently the prevalence of atopy and concomitant allergic disease has risen."
It
is true that in former times there were occasional serious complications from
these childhood diseases, but this is an area in which nutritional approaches
and homeopathy traditionally have been at their best. If these approaches were
made widely available, it is probable that most of these complications could be
eliminated. No one wants to see serious complications in our children, but the
vaccine route may in time prove to be the worst possible choice that could have
been made, as concerns the minor childhood diseases.
Threat of Brain damage from the Vaccines
Perhaps the greatest concern with vaccines today rests
with their possible causal relation to the growing epidemic of childhood autism,
developmental delay and attention deficit hyperactivity disorder (ADHD). Regarding
the latter, recent news item stated that ADHD has increased from 900,000 in l99l
to nearly 5 million today12.
Parenthetically, statistics may be open to question, but one cannot question the
observations of veteran elementary school teachers who, in our experience, unanimously
and emphatically report a marked increase in this disorder in recent years. Regarding
autism, a recent survey mandated by the California state legislature found an
increase of 273 percent in California in the past eleven years13. Reports from education departments of several states and
reports to the U.S. Congress on the rapidly increasing needs of classrooms for
developmentally delayed children reflect comparable changes throughout the nation14.
At present primary suspicion for this epidemic of neurobehavioral disorders rests with the MMR (measles-mumps-rubella) vaccine. Although scientific evidence has not yet reached the standards of scientific proof, one pioneer researcher in this area, Dr. Vijendra Singh with the Department of Pharmacology, University of Michigan, has published the report of a study in which he found that a large majority of autistic children tested had antibodies to brain tissue in the form of antibodies to myelin basic protein. He also found a strong correlation between myelin basic protein antibodies and antibodies to measles (almost all of the children had been immunized with the MMR vaccine, and none had had these diseases)15.
This study tends to confirm the results of a similar study published in The Lancet in l998 by Dr. Andrew Wakefield and coworkers of the Royal Free Hospital in London, indicating a possible link between MMR vaccination and Crohn's disease of the bowel and autism16.
If
the MMR vaccine were causing an autoimmune reaction involving the brains of autistic
children, what would be the mechanism? Although research in this area is in its
infancy, we do know some things. Both the measles and mumps fractions of the MMR
vaccine are cultured in chick embryo tissue. As purely genetic material, viruses
are highly susceptible to the process of "jumping genes," in which they
may incorporate genetic material from tissue in which they are cultured17. Furthermore, protein sequences in the measles virus have
been found to have similarities to those found in brain tissues18. As a result, once this foreign genetic material is introduced
into the child, it may set in motion an immunologic battleground, a process, which
the work of Dr. Singh would tend to confirm.
Stealth
Virus
A similar process may have taken place with the oral
(Sabin) polio vaccine, which is cultured in monkey kidney tissue. Years ago Dr.
John Martin, then serving as director of the viral oncology branch within the
U.S. Food and Drug Administration, found foreign DNA in contemporary polio vaccines.
He later learned that a simian (monkey) cytomegalic virus had been found in all
of the eleven African green monkeys imported for production of the polio vaccine19.
After leaving the FDA Dr. Martin took a position as professor of pathology with the University of Southern California. There he tested blood samples from patients with chronic fatigue syndrome, autism and other nervous system disorders. This work led to his discovery of unique cell-destroying viruses that were not recognized by the immune system. Termed "stealth viruses," some of which he thought had clearly originated from the simian cytomegalic virus, these viruses were missing specific genes, which, if expressed, would induce immune responses from the host20, 21. It should be admitted that this work is preliminary. No definitive conclusions can be drawn from it, but the need for further intensive investigation should be apparent.
Overdue in the opinion of many, on June l7, l999 US government officials voted to withdraw their recommendation for the use of the live oral polio vaccine and to recommend exclusive use of the inactive (Salk) polio vaccine, because the former has been the only remaining source of polio cases, though rare, in the USA since l979.
In
summary, it is possible that either the MMR or the oral polio vaccines, by mechanisms
described above, may induce a process of encephalitis or brain inflammation, which
may be highly prevalent but as yet rarely recognized for its true nature.
Genetic
Implications of "Live Virus" Vaccines
In a letter-to-the-Editor of Science magazine in October
l967, Joshua Lederberg, Department of Genetics, Stanford University School of
Medicine, warned about live-virus vaccines:
"In point of fact, we (are practicing) biological engineering on a rather large scale by use of live viruses in mass immunization campaigns …Crude virus preparations, such as some in common use at the present time, are also vulnerable to frightful mishaps of contamination and misidentification.22"
With
this sobering warning, made over 3 decades ago, it may sadly prove to be prophetic
for what we are seeing today.
Damage
May Yet Escalate
As another concept, it is highly pertinent that many
of today's children are second-generation vaccines; that is, they are born to
mothers previously vaccinated with the measles, mumps, and/or rubella vaccines.
It is possible that the reaction rates in the second-generation vaccines may be
happening on a much large scale due to previous sensitization of mothers from
their vaccines, this sensitization being transmitted in turn to the fetus during
pregnancy23. If this process is taking place, something we cannot know
until appropriate research is done, there predictably will be additional increases
in autism beyond that already taking place, should the process be continued into
yet another, a third generation.
Time may prove that vaccine programs went awry when they deviated from the most basic of all medical ethics, the right of parents to accept or reject vaccines for their children. Freedom-of-choice provides a system of checks and balances now lacking. At the very least, this would provide the parents the power to compel better safety screening of vaccines. The remedy? Parents should be allowed the right of informed consent, or the right to accept or reject vaccines for their children based on full and uncensored disclosure of pros and cons.
Today
we have a system in which vaccine production by the pharmaceutical companies is
largely self-regulated. Naturally these companies are interested in profits from
their products which, in itself, is not wrong. However, when arbitrary decisions
in the mandating of vaccines are made by government bureaucracies, who are highly
partisan to the pharmaceutical companies, with no recourse open to parents, we
have all the potential ingredients for a tragedy of historical proportions.
Conclusion
In closing, it may be appropriate to cite an item which,
though seemingly small in itself, may be indicative of the problems with which
we are faced. In January l993 a scientific journal published the results of a
study of 89 children with adverse clinical reactions following administrations
of various combinations of vaccines24.
Detailed case histories were taken and blood tests were done to examine various
parameters of cellular and humoral immunity. It was found that children with adverse
reactions had marked increases in abnormal blood parameters as compared with children
who had had no reactions.
The
first study of its kind as far as we are aware, perhaps the most striking and
significant feature of the report is not the results of the tests, which might
have been anticipated, so much as the fact that it came from a foreign country,
Czechoslovakia. American science has been foremost in the development and promotion
of vaccines. That it should be laggard in basic safety testing, of which this
study may represent one of the modest beginnings, is a sad reflection on the American
scientific community. Do we not have a right to expect better?
THE WORLDWIDE ACCEPTANCE OF MASS VACCINATION TO SUPPRESS INFECTIOUS childhood
diseases - once fiercely resisted - is one of the most successful public relations
stories in the history of medicine. As a result, epidemics of smallpox, which
once swept through 18th- and 19th-century port cities such as Halifax, New York,
and Boston without warning and cut down entire families, are now dry facts relegated
to medical books. Images of children struggling through whooping cough, walking
down the street coughing spasmodically, and stopping at curbs to spit up sticky
mucus are only fading memories for grandparents alive to talk about what their
parents told them. Baby boomers and their parents still remember lining up in
school in 1955 for polio vaccinations, with the hope that this magic bullet would
keep them out of the dreaded iron lung.
Mass vaccination has dramatically
suppressed childhood diseases. In Canada, recorded diphtheria cases dropped from
9,000 in 1924 to two to five by 1994. When measles vaccination began in the United
States between 1963 and 1965, doctors reported more than 400,000 cases annually;
by 1995, that number had dwindled to 309. Cases of tetanus are almost unheard
of in North America and Europe. Yet the universal use of vaccines as a worthy
goal that prevents needless suffering and that benefits all mankind has begun
to be challenged.
The voices of critics are heard in the living rooms of families whose children
have been injured or have died from reactions to routine childhood vaccinations,
and in courtrooms, where parents are suing vaccine makers and challenging mandatory
vaccination laws. In the U.S. Congress, legislators who have heard them have set
up a vaccine injury compensation program. At scientific conferences and in the
pages of prestigious medical journals, researchers and physicians are risking
their careers by discussing vaccine side effects. On network TV, millions are
watching parents, who say vaccines hurt their children, square off with policy
makers, who say vaccines rarely hurt anyone at all.
At the heart of the controversy lies a scientific challenge to the very premise
that mass vaccination with multiple vaccines safely and effectively controls diseases
and improves individual and public health. Simultaneously, ethical and legal arguments
challenge the right of government health officials to force vaccination on everyone.
Wrapped up in this scientific, legal, and political battle are beleaguered pediatricians
losing the trust of parents and a booming pharmaceutical industry with billions
of dollars invested in new vaccine development.
How
it all began
IN 1796, BRITISH PHYSICIAN EDWARD JENNER, ACTING ON
A HUNCH, SCRAPED cowpox pus onto the arm of an eight-year-old boy. He theorized
that a mild bout of cowpox would prevent a more virulent case of smallpox, and
he was right. The procedure, which he dubbed inoculation, enjoyed limited success
at first. But it failed in Jenner's own 11-month-old son, and bad reactions to
smallpox inoculation, which eventually used lymph from the cow itself, were legendary.
One mother in England bitterly complained in 1883 about mandatory vaccination
laws that allowed public health officials to issue summons, threaten parents with
imprisonment, and impose stiff fines for refusing to vaccinate their children.
She said, "In no country has the cry of the mothers been allowed a hearing.
They who see and realize that their children suffer from this practice have never
been consulted as to its initiative or its continuance. If the will of the mothers
could be made potent and effective, this cruel legislation would be at once and
universally repealed."
But 19th-century physicians quickly adopted and
promoted Jenner's new procedure despite public protests. Physicians and politicians
were desperate for anything that appeared to keep epidemic pestilences from invading
the overcrowded, filthy cities of Europe and the New World. They failed to realize
that eliminating the root causes of poor health - poverty, malnutrition, water
contaminated by human and animal waste, spoiled food, and industrial air pollution
among others - would help prevent the spread of many diseases.
Government-enforced vaccinations led to burgeoning chemical/pharmaceutical industries
in France, Germany, and Britain. The Pasteur Institute, founded in 1887 by the
famed inventor of the rabies vaccine, eventually created Canada's largest vaccine
manufacturer: Pasteur Mérieux Connaught. Today, vaccinations are big business.
In 1995, an international high-technology research firm, Frost & Sullivan,
projected that the worldwide human vaccine market will increase from $2.9 billion
to more than $7 billion by the year 2001.
Public health officials in every country assist the industry's growth, often by
force of laws that ensure citizens use about a dozen different viral and bacterial
vaccines, including ones to suppress even generally mild childhood diseases such
as chicken pox. Traditional public health measures - improving sanitation, nutrition,
living conditions, health education, and access to affordable medical care, especially
in underprivileged populations - often take a backseat to achieving a 100 per
cent vaccination rate.
Most medical doctors consider vaccines their single
most important tool in protecting public health. "Few would question the
profound importance of vaccines to public health," wrote Richard B. Johnston,
Jr., MD, medical director of the March of Dimes and chairman of the Institute
of Medicine Vaccine Safety Committee, in a 1994 National Academy of Sciences report,
Adverse Events Associated with Vaccines. "Not only have deaths from the most
common childhood infections been almost eliminated, but so have the devastating
morbidities of diseases like measles, paralytic polio, and congenital rubella.
This revolution has . . . led to major savings in medical costs and gains in work
productivity, as well as to reductions in deaths and suffering."
Questioning authority
BUT CRACKS ARE APPEARING IN THE united front that the
medical establishment has maintained for two centuries. In industrialized countries,
dissatisfied patients and alternative health care proponents are questioning orthodox
medicine's basic foundations, especially its heavy reliance on surgery and synthetic
drugs. The proliferating number of vaccines are just one more target for increasingly
well-educated and Internet-savvy health care consumers, who are wary of the many
magic bullets drug companies promote.
Remembering when doctors wanted every child's tonsils out, mothers wonder why
doctors now insist that they should stay in. Where doctors once prescribed antibiotics
for every sore throat, prescription-dependent patients are now being blamed for
new strains of antibiotic-resistant bacteria. A new drug promoted as a lifesaver
today is sometimes pulled off the market tomorrow for killing those who took it.
In the April 15, 1998, issue of the Journal of the American Medical Association
(JAMA), an analysis of drug side effects found that toxic reactions to correctly
prescribed medications make more than two million Americans seriously ill every
year and kill 106,000, putting drug side effects among the top 10 causes of death
in the United States. Among children, antibiotics and vaccines cause more adverse
reactions than any other prescribed medicines, according to a Canadian study presented
at the annual meeting of the American Academy of Allergy and Asthma in 1998. Sandra
K. Knowles and her colleagues at the Sunnybrook Health Sciences Centre in Toronto
reviewed Canadian data on more than 1,500 cases of drug reactions between 1985
and 1995. The antibiotics amoxicillan and ampicillin accounted for 24 per cent
of total adverse reactions, with vaccines coming in second at 19 per cent. Baby
boomers wonder what and who to believe.
Many believe health requires better nutrition, exercise, managing stress, a positive
attitude, and a less intrusive approach. A 1997 study in the Canadian Journal
of Public Health estimated that 15 per cent of Canadians had seen an alternative
therapy practitioner in the preceding 12 months. A 1998 survey in JAMA found 39
million Americans made more than 600 million visits to alternative health care
practitioners in 1997, more than to primary care physicians. The patients paid
most of the $21.2 billion cost themselves because health insurance plans generally
don't reimburse patients for alternative health care. The patients wanted alternative
therapies primarily to "prevent future illness from occurring or to maintain
health and vitality."
Embracing the more spiritual concept of achieving
better health through better living rather than through better chemistry, members
of the Me generation - who challenged every institution and social more as teenagers
- continue to exercise their counterculture instincts as adults by asserting their
right to make independent health care choices. Their demand to make vaccination
choices puzzles and worries MDs, including some outspoken alternative health care
advocates.
Andrew Weil, MD, a respected leader in the alternative health
care movement, defends mass vaccination. Sparring with Richard Moscowitz, MD,
in Natural Health magazine in 1997, Weil asserted, "The debate about immunization
could only be going on in a country where the people are mostly immunized. If
people in this country lived with these diseases, you wouldn't hear them questioning
immunization." Moscowitz, a clinician who specializes in homeopathy, countered,
"For us to bombard a newborn baby with a whole battery of vaccines as, in
effect, their very first immunological experience I think is reckless beyond measure.
I would say it borders on the criminal."
VACCINES ARE SUPPOSED TO fool the body's immune system into producing antibodies
to resist viral and bacterial infection in the same way that actually having the
disease usually produces immunity to future infection. But unlike natural recovery
from many infectious diseases, which stimulates lifetime immunity, vaccines only
provide temporary protection. That's why booster doses are often required.
Vaccination raises two equally contentious questions. First, is it better to protect
children against infectious diseases early in life through temporary immunity
from a vaccine or are they better off contracting certain contagious infections
in childhood and attaining permanent immunity? Second, do vaccine complications
cause more injury and death than diseases do? Both questions essentially pit trust
in human intervention against trust in nature.
The rise of asthma and other autoimmune diseases
PHYSICIANS AND PUBLIC HEALTH OFFICIALS PROMOTING CHILDHOOD
vaccination insist that vaccines do not harm the immune system in any way. They
defend the use of vaccines - made in the laboratory from altered viruses and bacteria
as well as chemicals, such as formaldehyde, mercury, aluminum, monosodium glutamate,
sulfites, and antibiotics - as necessary weapons for shielding vulnerable newborns
from the suffering caused by viral and bacterial infections.
Visitors to
the U.S. Centers for Disease Control and Prevention (CDC) web site (www.cdc.gov)
learn that "vaccines give your baby's immune system the chance to practice
and make protective antibodies before real germs invade. If left totally to chance,
your baby's first exposure to a disease may be from a germ too strong for your
baby to fight. That's why before parents had vaccines for their children, many
children died from whooping cough, measles, diphtheria and other diseases. Those
same germs exist today, but today's babies are protected by vaccines."
The CDC warns that "Immunizations must begin at birth and most vaccinations
[be] completed by age 2. . . . Children under 5 are especially susceptible to
disease because their immune systems have not built up the necessary defenses
to fight infection."
YET A GROWING BODY OF SCIENTIFIC EVIDENCE SUGGESTS
THAT VACCINES MAY have inadvertently done more than just suppress infectious childhood
diseases. Vaccine critics point out that the increase in autoimmune and neurological
disorders in the past three decades in industrialized countries coincides with
the addition of new vaccines to the childhood vaccination schedule as well as
rapidly increasing vaccination rates.
Between 1964 and 1992, the U.S. added six new vaccines to the mandatory vaccination
schedule, including five doses of live virus polio; two doses of MMR (measles,
mumps, and rubella); four doses of Hib (haemophilus influenzae type b, which is
a type of meningitis); and three doses of hepatitis B vaccine, while more strictly
enforcing existing laws mandating five doses of DPT (diphtheria, pertussis- also
known as whooping cough - and tetanus). Vaccination coverage hepatitis B, and
Hib vaccines.
Asthma is an autoimmune disorder, an allergic condition that
tops the list of chronic respiratory diseases found in children in Western societies
today. A 1997 study published in Science reported that "the prevalence of
asthma in westernized societies has risen steadily this century, doubling in the
last 20 years. Asthma now affects one child in seven in Great Britain, and in
the United States it causes one-third of pediatric emergency room visits."
Another study found that between 1964 and 1980, asthma in children aged six to
11 years increased 50 per cent. In 1995, the CDC reported that, between 1982 and
1992, asthma increased 52 per cent for persons between the ages of five and 34
years old, and deaths from asthma increased 42 per cent.
The 1978 Canada Health Survey found that only 2.3 per cent of Canadians 15 years
and over reported having asthma. By 1991, its prevalence was at 6 per cent. More
than 1.5 million Canadians of all ages suffer from asthma. Even more worrisome,
however, are the findings of a large survey of Canadian school children in 1995-96
that found a 13 per cent prevalence of asthma. From the early 1970s to the late
1980s, the number of Canadian patients under 35 years discharged from hospital
with a diagnosis of asthma tripled. The greatest increase has been in children
under four years of age. As in the U.S., asthma deaths in Canada have climbed
along with its increased prevalence.
Asthma's economic burden is formidable.
According to Canada's 1994 National Population Health Survey, the long-term disability
costs associated with asthma, emphysema, and chronic bronchitis in 1993 totaled
$1.8 billion, without counting costs associated with treating asthma in children
under 11 years old. In the U.S., the total cost of illness related to asthma in
1990 was estimated at $6.2 billion.
Although public health officials attribute the recorded increases in asthma to
better case diagnoses, more air pollution indoors and outdoors, and smoking, some
scientists find evidence that vaccination and lack of contagious infectious diseases
in early childhood may later encourage the development of asthma and other allergic
conditions.
In 1996, the British medical journal, The Lancet, published Danish
and British findings concerning child health, lung function, and allergy. Noting
that the incidence of early childhood diseases in Britain has fallen this century
while those of allergic diseases such as asthma, hay fever, and eczema rose sharply,
the researchers hypothesized that certain childhood infections, specifically measles,
may protect against allergy.
They compared evidence of atopy (allergy) in two groups of young adults, aged
14 to 21, in Guinea-Bissau, West Africa. One group had recovered from measles
during a 1979 epidemic (before the measles vaccine was introduced); the other
did not get measles as children and were later vaccinated.
The researchers confirmed their hypothesis: About 26 per cent of the vaccinated
young adults had allergic conditions, twice the rate of those who had recovered
from measles. After adjusting for breast-feeding and other variables, they concluded
that their findings may indicate that "measles infection prevents allergic
sensitization." Because this was the first population-based study to relate
reduced allergies to a specific childhood viral infection, they urged further
studies in developing countries, where childhood diseases are still widespread
due to low vaccination rates.
Vaccine promoters point out that measles complications
kill one million children annually, mostly in underdeveloped countries. In Guinea-Bissau's
1979 measles epidemic, the case-fatality rate in children under 3 was 25 per cent:
it is better to have asthma for the rest of your life that die from measles.
Mass vaccination critics counter that West Africa's health and living conditions,
which could account for the high death rate, don't apply to Europe and North America,
where toddlers who get measles usually recover without complications. Why not
eliminate poverty, malnutrition, poor sanitation, and substandard medical care
in developing countries so that measles-related death rates come down, as in industrialized
countries even before vaccination?
Another study, this time comparing the
prevalence of asthma and other allergic disorders in child populations throughout
the world, appeared in The Lancet in 1998. The authors found that the wealthier,
more developed countries in Western Europe and North America and Australia and
New Zealand had higher incidences of asthma than did the poorer countries in Eastern
Europe, Asia, and Africa.
The authors of the 1997 Science article "Asthma: An Epidemic in the Absence
of Infection?" tentatively answered yes to their own question, concluding
that "childhood infections may, therefore, paradoxically protect against
asthma." In a 1997 issue of Epidemiology, New Zealand researchers hypothesized
that "it is theoretically possible that immunization may contribute to the
development of allergic disease." Of 1,265 New Zealanders born in 1977, 23
received no childhood vaccinations, and none suffered childhood asthma. Among
the 1,242 who got polio and DPT shots, 23 per cent later had episodes of asthma,
23 per cent had asthma consultations, and 30 per cent had consultations for other
allergic illness. Their conclusion was, "The findings presented here are
consistent with the hypothesis that some component of infant immunization may
increase the risk of developing asthma in childhood."
A
tripling of diabetes
DIABETES, A CHRONIC AUTOIMMUNE DISORDER THAT DISRUPTS
THE blood's glucose levels, afflicts some 125 million people worldwide. That number
is expected to double by 2025. In the U.S., where 600,000 new cases are diagnosed
every year, the number of diabetics has increased a record threefold since 1958,
to nearly 16 million, and millions more may unknowingly have it. Now the fourth
leading cause of death in the U.S., diabetes can cause blindness, kidney failure,
stroke, and heart disease and lead to amputations. In 1992, the U.S. National
Institute of Diabetes and Digestive and Kidney Diseases estimated that diabetes
cost the U.S. $45 billion for medical treatment plus $47 billion for lost work
time, disability payments, and premature death. In Canada, the Laboratory Centre
for Disease Control found that the 1993 cost burden of diabetes exceeded $1 billion,
including $565 million in drug, physician, and hospital costs and $559 million
in mortality-related costs.
As early as 1949, the medical literature reported
that some children injected with the pertussis vaccine had reduced blood glucose
levels. The pertussis vaccine can cause diabetes in mice. In recent decades, scientists
have suggested that viral infections may be a co-factor in causing diabetes. Because
both rubella and mumps infections have been associated with juvenile diabetes,
the introduction of the live virus vaccines for measles, mumps, and rubella in
the 1960s and 1970s also raised questions about whether live vaccine virus could
be a contributing co-factor to the onset of diabetes.
In the May 24, 1996, New Zealand Medical Journal, J. Barthelow Classen, MD, a
former researcher at the U.S. National Institutes of Health (NIH) and the founder
and CEO of Classen Immunotherapies in Baltimore, reported that juvenile diabetes
increased 60 per cent following a massive hepatitis B vaccination campaign for
babies six weeks or older in New Zealand from 1988 to 1991. In the October 22,
1997, Infectious Diseases in Clinical Practice, Classen showed that Finland's
incidence of diabetes increased 147 per cent in children under five after three
new vaccines were introduced in the 1970s, and that diabetes increased 40 per
cent in children aged 5 to 9 after the addition of the MMR and Hib vaccines in
the 1980s. He concluded that "the rise in IDDM [juvenile onset diabetes]
in the different age groups correlated with the number of vaccines given."
Classen discounts the conclusions of many vaccine safety trials, especially
48-hour or several-day vaccine reaction follow-ups, which can miss the development
of autoimmune dysfunction that can take years to develop. According to Classen,
"Previous vaccine trials are flawed because they are not designed to detect
associations between vaccination and autoimmune diseases, such as diabetes. Prospective
clinical trials are needed."
Government health officials dispute Classen's research, and that of others concerned
about mass vaccination policies. In 1997, U.S. federal health officials did admit
that one of their own studies showed that "the possibility that hepatitis
B vaccination, particularly at older ages, may increase IDDM risk cannot be ruled
out and will require larger more detailed studies." Nevertheless, in 1998,
they told the public in a report written to rebut Classen's findings, "Dr.
Classen's results are not consistent with current scientific thinking and have
not been verified by other researchers. . . . Comparison of diabetes rates between
countries with different vaccination policies also provides weak evidence because
many factors, including different vaccination schedules, may differ by country.
Many factors, including genetic predisposition and a number of possible environmental
exposures unrelated to vaccines, may influence the development of diabetes in
different countries."
Last year, after Classen discussed the possible
link between diabetes, certain vaccines, and the timing of early childhood vaccinations
on ABC's World News Tonight, he was summoned to a closed meeting at Johns Hopkins
University chaired by Neal Halsey, MD, chairman of the American Academy of Pediatrics
Committee on Infectious Diseases, AAP liaison member of the CDC's Advisory Committee
on Immunization Practices, and Director of the Institute of Vaccine Safety at
Johns Hopkins University. Officials from NIH, the Food and Drug Administration
(FDA), and the CDC, as well as representatives from several vaccine manufacturers
also attended the meeting. There, they criticized Classen for speaking publicly
about his findings. Later, World Health Organization officials joined U.S. health
officials in berating Classen.
Undaunted, Classen and a colleague appealed
to vaccine policy makers in a letter published in the January 16, 1999, British
Medical Journal. "We believe that the public should be fully informed that
vaccines, though effective in preventing infections, may have long-term adverse
effects," he said. "An educated public will probably increasingly demand
proper safety studies before widespread immunization. We believe that the outcome
of this decision will be the development of safer vaccine technology."
Autism soars
OTHER SCIENTISTS RESEARCHING HEALTH PROBLEMS ASSOCIATED
WITH vaccines have also felt the ire of public health officials. In 1998, an unsuspecting
young British gastroenterologist suddenly found himself in the eye of a hurricane
for discovering a possible connection between the MMR vaccine and autism.
In the February 27, 1998, issue of The Lancet, Andrew Wakefield, MD, and 13 colleagues
reported on a new syndrome involving inflammatory bowel disease and autism in
children. Eight out of 12 normal children who developed severe intestinal disorders
soon after an MMR vaccination also became autistic. Previously, five of those
eight children had reacted adversely to vaccinations.
The team of British scientists, who had inadvertently stumbled upon the connection
while studying Crohn's disease and other inflammatory bowel dysfunction in children,
emphasized that they had not proved a cause-and-effect relationship. They called
for more studies to investigate whether persistent viral infection, either from
natural disease or live virus vaccines, can lead to central nervous system damage
in some children.
Nevertheless, in the same issue of The Lancet, CDC officials Robert Chen, MD,
and Frank DeStefano, MD, charged in an editorial that "vaccine safety concerns
such as that reported by Wakefield and colleagues may snowball" when the
public and the media "confuse association with causality and shun immunization."
Other CDC officials discounted the study's importance, saying that the children's
health problems were "coincidental" and not caused by vaccination.
Soon after, a Reuters newswire story quoted Johns Hopkins's Halsey saying it was
"highly inappropriate" for Wakefield and his colleagues to discuss a
possible connection between the children's health problems and measles or MMR
vaccines. Wakefield was later called before the Medical Research Council where
British, U.S., and WHO health officials criticized his report for unnecessarily
scaring the public.
In contrast, autism experts defended Wakefield. Bernard Rimland, who has a PhD
in experimental psychology and is founder and director of the Autism Research
Institute in San Diego, said, "It is ludicrous to claim that the link between
many causes of autism and vaccination is just coincidental. Dr. Wakefield's group
has greatly expanded our understanding of one possible mechanism. The blunt truth
is that some children are harmed by vaccinations. Research, not denial, is the
proper response to this report."
Portia Iverson, founder and president of CAN, the Cure Autism Now foundation in
Los Angeles, also took issue at the government-led criticism: "Approximately
one-half of the hundreds of parents who call our office each month report that
their child became autistic shortly after receiving a vaccination. Isn't it the
responsibility of the government to take a pro-active position on behalf of these
children rather than a defensive one?"
Like incidences of asthma and diabetes, the incidence of autism has climbed dramatically
in the past 30 years. Although the medical literature identified only a handful
of cases in the 1940s, by the mid-1960s, after the DPT vaccine had been widely
used and the measles vaccine introduced, autistic children began flooding doctors'
offices. (Parents in the U.S. and Canada who report vaccine-associated autism
most often mention that their children's autistic behaviors followed DPT or MMR
vaccination.) Today, 1 in 1,000 children are diagnosed as autistic, making autism
more prevalent among children than cancer, multiple sclerosis, or cystic fibrosis.
A recent California study put the figure at 1 in 312 children, a 273 per cent
increase between 1987 and 1998.
Hepatitis B vaccine takes a hit
CANADIAN PHYSICIANS HAVE ALSO FACED CRITICISM FROM
GOVERNMENT HEALTH officials who dismiss vaccine side effects. Byron Hyde, MD,
chairman of the Ottawa-based Nightingale Research Foundation and an internationally
recognized authority on myalgic encephalomyelitis (chronic fatigue syndrome),
has accumulated data on several hundred cases of serious immune and neurological
dysfunction following hepatitis B vaccination. His first case reports, in the
early 1990s, came from Quebec nurses who reported a constellation of autoimmune
symptoms, including pain, fatigue, and mental dysfunction, and were unable to
work.
Hyde, a vaccination advocate, spoke out publicly about the side effects in September
1997 at the First International Public Conference on Vaccination sponsored by
the National Vaccine Information Center in Washington, D.C. He told more than
500 parents and doctors that in the early 1990s, both the vaccine manufacturer
and the Canadian health authorities repeatedly rebuffed his requests for an investigation
into signs of demyelinating disease, measurable loss of IQ, loss of stamina, intractable
pain, blindness, skin lesions, and other problems affecting health care workers
following their hepatitis B vaccinations.
Hundreds of cases later, he has
concluded that "almost all of these people who had adverse reactions after
the first immunization, after the second immunization were individuals who had
immunological side effects and who told their physicians, and the physicians did
nothing about it but continued to proceed with immunization. . . . I think part
of the problem is the pharmaceutical companies and the governments themselves
have attempted to say, 'Here, take this sugar pill, it is danger-free, it is a
wonderful thing, it has no risk, no problems,' and doctors have become lazy and
actually believed this dangerous philosophy put out by the pharmaceutical companies
and the governments."
Researchers like Hyde are at the centre of a growing controversy about the recombinant
DNA hepatitis B vaccine licensed in the U.S. in 1986. Although health officials
estimate that more than 300 million people worldwide have chronic hepatitis B,
both Canada and the U.S. have historically had among the world's lowest rates,
even before the vaccine was introduced. Unlike in parts of Asia and Africa, where
the disease often affects 5 to 20 per cent (and sometimes more) of the population,
in Canada and the U.S., less than 1 per cent have hepatitis B, and about 95 per
cent of those infected recover and get permanent immunity. However, health officials
emphasize that those who become chronically infected suffer dire consequences:
poor health, liver disease, and sometimes liver cancer.
Unlike whooping cough, a respiratory disease that can kill babies and small children,
which the pertussis vaccine was designed to prevent, hepatitis B is not a childhood
disease. Spread through infected body fluids, primarily blood, it is most prevalent
in high-risk adult populations such as intravenous drug users, prisoners, individuals
with multiple sexual partners, those undergoing blood transfusions, and health
care workers exposed to infected blood. Doctors reported about 10,000 hepatitis
B cases in the U.S. in 1997 with only 306 occurring in children under 14.
The only babies at risk are those born to hepatitis B-infected mothers, but because
few hospitals screen pregnant women for hepatitis B infection, in 1991, the CDC
recommended vaccinating all newborns before discharge from the hospital nursery.
The CDC maintains its recommendation despite this 1997 admission: "Hepatitis
B continues to decline in most states primarily because of a decrease in the number
of cases among injecting drug users and, to a lesser extent, because of a decline
in cases associated with both male homosexual practices and heterosexual practices."
Widely touted as almost risk-free, health care workers in the U.S. and Canada
were among the first to get this, the first genetically engineered recombinant
DNA vaccine. Soon after, nurses and doctors in both countries reported postvaccination
symptoms like those described by Hyde, ranging from rashes and fevers that come
and go, debilitating fatigue, muscle weakness, joint pain, and memory loss to
paralysis and death. Many were diagnosed with rheumatoid arthritis, multiple sclerosis,
lupus, and other autoimmune disorders, although most often they did not suffer
from classic forms of these diseases. As the U.S. passed laws and Canada recommended
children get three vaccine doses or be barred from school, children began to report
the same reactions.
Recombinant hepatitis B vaccine is also being challenged by Bonnie Dunbar, PhD,
professor of Cell Biology, Baylor College of Medicine in Houston, who has spent
most of her 25-year career in academic and laboratory science in new vaccine development.
After reactions to hepatitis B vaccinations disabled both her brother and a research
assistant, she intensively investigated the vaccine. With several other U.S. scientists,
Dunbar is investigating whether the genetically engineered hepatitis B vaccine
"tricks" the immune systems of genetically susceptible individuals into
attacking their own bodies, causing debilitating autoimmune and brain dysfunction.
Recombinant hepatitis B vaccines contain polypeptide sequences similar to those
present in human brain tissues such as myelin while viral polypeptides can induce
autoimmune diseases resembling multiple sclerosis and rheumatoid arthritis.
"The drug companies report safety studies that monitored children and adults
for only four or five days after vaccination," said Dunbar. "It takes
weeks and sometimes months for autoimmune disorders such as rheumatoid arthritis
to develop following vaccination. In fact, a study group on hepatitis B vaccine
with members from the CDC, WHO, NIH, Merck & Co., SmithKline Beecham, Pasteur
Mérieux Connaught, and Pasteur-Merieux, MSD Joint Venture reported that
'a reasonable time limit to use for the onset of MS postvaccination is about 60
days."
Dunbar is most critical of the science: "No basic science research to determine
the biological mechanism of vaccine injury or long-term studies into the side
effects of this vaccine have ever been conducted in babies or children. In adults,
only limited follow-up has been carried out in genetically restricted populations."
Dunbar and her colleagues have applied twice for government funding to investigate
the role that genetic factors may play in hepatitis B vaccine reactions or in
vaccine failures. Their goal of identifying high-risk markers to screen susceptible
children and adults out of the mass vaccination program will have to wait. The
NIH has twice turned them down.
To continuing reports that the hepatitis B vaccine negatively affects children
and adults, U.S. government officials respond, "there is no confirmed scientific
evidence that hepatitis B vaccine causes chronic illness, including multiple sclerosis,
chronic fatigue syndrome, rheumatoid arthritis, or autoimmune disorders. . . .
Surveillance of adverse events in the United States after hepatitis B vaccination
have shown no association between hepatitis B vaccine and the occurrence of serious
adverse events including Guillain-Barre syndrome, transverse myelitis, optic neuritis
and seizures."
The CDC insists on vaccinating all newborns and young children on the grounds
that they may act irresponsibly later in life. "While most hepatitis B vaccine
infections occur among older adolescents and young adults, vaccination of persons
in high-risk groups has generally not been a successful public health strategy."
Yet the vaccine manufacturers themselves don't know how long vaccine-induced immunity
will last. Merck & Co. stated in its 1996 product insert, "The duration
of the protective effect of [the vaccine] in healthy vaccines is unknown at present,
and the need for booster doses is not yet defined."
Government officials have also been on the defensive since last October, when
France became the first country to end hepatitis B vaccine requirements for schoolchildren.
France's health minister acted after numerous reports of arthritis- and multiple
sclerosis-like symptoms. Pending citizen lawsuits against SmithKline Beecham and
Pasteur-Merieux, which make and sell the hepatitis B vaccine, may also have influenced
the French decision. In addition, attorneys representing 15,000 French citizens
are suing government health officials for understating the vaccine's risks and
exaggerating its benefits.
The day after France withdrew the vaccine mandate,
a dismayed World Health Organization stated that "the decision taken yesterday
may lead to loss of public confidence in this vaccine, and decisions by other
countries to suspend or delay introduction of hepatitis B vaccine. . . . WHO strongly
recommends that all countries already using hepatitis B vaccine as a routine vaccine
in their national immunization programs continue to do so, and that countries
not yet using the vaccine begin as soon as possible."
Canadian
parents take on the establishment
IN CANADA, THE HEPATITIS B VACCINE CONTROVERSY IS ALSO
HEATING UP. Although only three provinces (Manitoba, Ontario, and New Brunswick)
actually mandate vaccines for school entry, parents can refuse on medical, philosophical,
or religious grounds. Even with these informed consent protections, Mary James,
co-founder of the Association for Vaccine Damaged Children (AVDC) in Winnipeg,
points out that "vaccination is never presented as a choice to parents. Most
parents are told that their child must be vaccinated. Since most parents are not
aware of vaccine risks or their rights, they comply without questioning."
When parents were told last year that their children had to get three doses of
the new hepatitis B vaccine, James and her AVDC co-founder Leona Rew fought for
a court injunction to stop the program, arguing that Winnipeg public health officials
were inadequately informing parents of potential risks. Although they lost their
bid to stop the program, members of AVDC joined members of Parents for Informed
Consent and the Eagle Foundation in Winnipeg to raise their objections through
television and radio appearances.
To better monitor vaccine risks, the federal government's Laboratory Centre for
Disease Control operates a vaccine reaction reporting system called Vaccine Associated
Adverse Events (VAAE). Although most doctors are not required to report health
problems following vaccination (except in Ontario, where AVDC activists got a
law passed), the system does receive about 4,000 to 5,000 voluntary reports every
year. Laboratory Centre for Disease Control officials stress that these reports
only reflect "any event that is felt to be temporally related to the administration
of an immunization but not necessarily absolutely causally related." They
state, "Over 12 million doses of vaccine are distributed every year and very
few concerns arise despite intense searching. Until diseases are eradicated, immunization
remains our best defense."
Rew disagrees: "Doctors and nurses still do not report adverse reactions.
We need a reporting system that has some teeth in it so that doctors are compelled
to do their job and report serious health problems that occur after someone gets
vaccinated."
James, whose five-month-old daughter was partially paralyzed
and died in 1984 following two polio vaccinations, and Rew, whose infant son had
bouts of high-pitched screaming and a seizure within hours of a DPT shot, emphasize
that AVDC does not advocate banning vaccines. Says James, "The vaccines should
be available like any other health care product, but parents should know the risks
as well as the benefits and be able to make an informed choice. Right now, they
are just getting one side of the story - the one that the government and drug
companies want everyone to believe."
American protest forces acknowledgment
CANADA'S GRASSROOTS MOVEMENT RESEMBLES ITS U.S. PREDECESSOR.
In 1982, a television documentary, DPT: Vaccine Roulette, prompted a handful of
parents, whose children had been injured by or died from the DPT vaccine, to found
an organization known today as the National Vaccine Information Center (NVIC).
Soon after, manufacturers threatened to stop producing vaccines unless they were
immune to lawsuits. Although most vaccine injury lawsuits were then either won
by drug companies or settled on the courthouse steps by weary, cash-poor parents
(with all evidence sealed from public view), plaintiffs had won large enough punitive
damages in the late 1970s and early 1980s to worry vaccine producers about their
liability.
The U.S. Congress immediately began writing legislation for a vaccine injury compensation
system and asked physician organizations, vaccine manufacturers, and the co-founders
of NVIC to present their concerns. The physicians and manufacturers wanted Congress
to remove all liability and to guarantee protection from lawsuits for vaccine
injury and death. Congress's final decision required parents to first file for
federal compensation by suing the secretary of the Department of Health and Human
Services. But parents won the right to sue vaccine manufacturers or negligent
physicians if vaccine-injured children were offered too little financial support
for their catastrophic vaccine injuries or were turned down entirely - although
bringing a lawsuit would then be more difficult. Parents also retained the right
to sue for unlimited punitive damages where manufacturers engaged in "fraud
or intentional wrongful withholding of information relating to the safety or efficacy
of the vaccine," or engaged in "other criminal or illegal activity relating
to the safety and effectiveness of vaccines."
Government health agencies opposed the proposed federal compensation legislation,
maintaining that vaccinated children who developed serious health problems had
an "underlying genetic disorder" or a health problem that would have
spontaneously occurred even without a vaccination. It was only after the book
DPT: A Shot in the Dark (Coulter and Fisher, Harcourt Brace Jovanovich, 1985)
was published and parents held public demonstrations at the CDC in Atlanta and
in front of the White House the following year, that President Ronald Reagan signed
the National Childhood Vaccine Injury Act into law in 1986. (Pressure by parents
eventually led to the FDA licensing of a purified pertussis vaccine in 1996, which
has been associated with fewer reactions.)
Today, parents of vaccine-injured children and their lawyers criticize the law's
implementation because three out of four applicants are turned away. With government
lawyers and health officials fighting every claim, more than $1 billion lies idle
in a vaccine injury trust fund. Still, under the act, more than $1 billion has
been paid to 1,000 families whose members, the U.S. Court of Claims in Washington,
D.C., has judged, were harmed by routine vaccinations. The majority of the awards
have been for DPT-vaccine related brain damage or death, with a lesser number
for MMR and polio vaccine reactions. (NVIC's web site, www.909SHOT.com, describes
some of the vaccine injury cases.)
The 1986 law, which mandated the Institute of Medicine (IOM) of the prestigious
National Academy of Sciences (NAS) to review the medical literature for evidence
that vaccines can cause injury and death, was historic societal acknowledgement
that vaccines can be harmful. In 1991 and 1994, NAS published the evidence in
three landmark reports.
One high-level physician committee examining the medical literature wrote, "the
lack of adequate data regarding many of the adverse events under study was of
major concern. . . . The committee encountered many gaps and limitations in knowledge
bearing directly or indirectly on the safety of vaccines." Nevertheless,
the IOM did find enough scientific evidence to confirm that the DPT vaccine can
cause acute brain inflammation and permanent brain damage that ranges from learning
disorders to severe and profound retardation; the DT (diphtheria and tetanus)
vaccine can cause Guillain-Barre syndrome, including death, as well as brachial
neuritis; the rubella vaccine can cause acute and chronic arthritis; the live
oral polio vaccine can give polio to the person being vaccinated or to someone
who comes into contact with that person's body fluids; and the MMR vaccine can
cause shock as well as a potentially fatal infection from a vaccine strain of
measles virus.
Because scientific studies did not exist, physician committees could not properly
evaluate a long list of other vaccine-associated health problems, including some
of the chronic autoimmune and neurological disorders - such as diabetes and multiple
sclerosis - at the centre of the vaccine safety controversy. The big news, though,
was that the medical community had told the public that vaccines can injure and
kill. While health officials stressed anew that "the benefits [of vaccines]
outweigh the risks," parents of healthy children better understood the cry
of parents of vaccine-injured children: "When it happens to your child, the
risks are 100 per cent."
Under the 1986 law, the federal government also set up an improved vaccine reaction
reporting system, which, like Canada's reporting system, depends on physicians'
reports. The U.S. Vaccine Adverse Event Reporting System receives between 12,000
and 14,000 reports of hospitalizations, injuries, and deaths following vaccination
every year, but as in Canada, parent groups claim that less than 10 per cent of
doctors report vaccine-associated health problems and that the government does
not adequately follow up.
A
matter of law
UNLIKE CANADA, HOWEVER, EVERY U.S. STATE LEGALLY REQUIRES
vaccinations, and public health officials vigorously enforce these laws. Refusing
to vaccinate one's children can result in denial of an education, including enrolment
in day care, elementary school, high school, college, and graduate school; denial
of health insurance; denial of employment; and threatened denial of government
benefits for poor children, including food and medical care. In addition, parents
who don't comply with vaccination laws have been charged with child medical neglect
and threatened with having their children taken from them.
All 50 states provide a medical exemption to vaccination laws that doctors licensed
to prescribe drugs can write. All but two states allow exemptions for religious
beliefs, but some states require that parents belong to a religion that has a
written tenet opposing vaccination (several state high courts have found this
requirement unconstitutional). Some 16 states provide for philosophical or "personal
belief" exemption, but most parents are unaware of these exemptions and fewer
than 1 per cent in most states exercise them.
Although American vaccine laws fall under state, rather than federal, jurisdiction,
as soon as the CDC licenses a new vaccine and recommends it for "universal
use," state health officials automatically make it mandatory. So, while state
health officials only required children to show proof of smallpox vaccination
to enter school in 1949, in 1999, most states require children to be injected
with 33 or 34 doses of nine or 10 different vaccines.
Tracking
system to enforce vaccination
TO ENCOURAGE HIGH VACCINATION RATES, FEDERAL OFFICIALS
GIVE GRANTS and other financial incentives to state health and education agencies,
or withhold them. In 1993, the Clinton administration launched an "Immunization
Initiative," and Congress authorized more than $400 million for states that
enforced mandatory vaccination by using social security numbers to track children
from birth. Simultaneously, a grant program rewards state health departments with
up to $100 for each fully vaccinated child.
The government eventually plans to link state vaccine tracking systems together
to create a government-operated centralized electronic database monitoring everyone's
medical records, including vaccination status, from birth. One federal proposal
would link a national ID "smartcard" to obtaining a driver's license
and other societal privileges, such as health care or getting a job. Individual
legislators, at both the state and federal levels, have already proposed tax penalties
for citizens who don't fully vaccinate their children.
In addition to government grants, the Robert Wood Johnson Foundation (Johnson
& Johnson) has awarded nearly $10 million to states to set up vaccine tracking
systems to enforce vaccine laws. In 1989, Johnson & Johnson joined with Merck
& Co., the U.S. manufacturer of the MMR, chicken pox, and hepatitis B vaccines,
to form Worldwide Consumer Pharmaceuticals Company, with the goal of becoming
"one of the premier worldwide consumer products companies." By 1997,
Merck's vaccine sales had reached $1 billion.
Tracking system would eventually become global
A NUMBER OF PRIVATE COMPANIES AND ORGANIZATIONS ARE
ALREADY WORKING with governments around the world to ensure "the integration
and harmonization of immunization registries" through the promotion, standardization,
and acceptance of computerized patient records systems that would monitor the
health status of every citizen.
The Children's Vaccine Initiative (CVI),
launched in 1990 at the World Summit for Children in New York City, wants to develop
global strategies for "the development and utilization" of vaccines
by all the world's children. Headquartered in Geneva, CVI receives money from
the United Nations Children's Fund, the United Nations Development Programme,
the World Bank, WHO, and the Rockefeller Foundation. CVI is also financially supported
by the world's largest manufacturers and marketers of vaccines. To conform to
CVI goals, in 1994, CDC health officials developed a National Vaccine Plan for
the U.S., which "provides a framework in which diverse domestic and international,
public and private-sector activities in immunization and vaccine development can
be effectively coordinated" and "describes the way in which the United
States should promote immunization to protect the health of all people, including
"accelerating the development and use of promising new and improved vaccine
candidates."
An
HIV vaccine for children?
IN A FEBRUARY 12, 1997, MEETING OF THE CDC's Advisory
Committee on Immunization Practices, which makes vaccine policy for the U.S.,
committee member Neal Halsey reminded HIV vaccine researchers and developers that
the government plans to target preteens for universal application of an HIV vaccine.
Halsey told them, "One of the things that's happened in the past with vaccines
is that sometimes the manufacturers have developed them and tested them primarily
in an age group or a population which may not be the final target population that
this committee has considered. . . . We really see age 11 to 12 as the target
age for introduction vaccines for prevention of sexually transmitted diseases.
. . . It would be nice if there were studies that were planned in parallel when
you move another step in the direction of actually having a candidate vaccine,
realizing where we think we would want to use universal application of such a
vaccine."
As the number of reported AIDS cases in the U.S. continues to drop (about 58,000
in 1997 compared with 103,691 in 1993) and the number of AIDS cases in the Third
World veers out of control, vaccination supporters have accelerated their push
to put an AIDS vaccine on the market. In 1997, President Bill Clinton challenged
scientists and industry to make an AIDS vaccine available within 10 years and
added more money to the yearly $150 million already committed to this purpose.
The U.S. media compared his call to President John F. Kennedy's challenge to American
scientists to put a man on the moon.
At least three dozen different experimental HIV vaccine trials are underway in
the U.S., using numerous approaches. Pasteur Mérieux Connaught has created
one vaccine from a weakened, genetically engineered canarypox virus. Researchers
are testing it as an injection, and it also will be swabbed or dripped onto the
genital and urinary tracts and nose and throat. Another experimental vaccine uses
a new strategy based on genetically engineered salmonella bacteria. In 1998, the
Chicago-based International Association of Physicians in AIDS Care called for
use of an experimental live HIV vaccine, although physician advocates admitted
that a live HIV vaccine could theoretically mutate into an AIDS-causing strain.
A report on monkey tests from the 12th World AIDS Conference last July confirmed
that many monkeys or their offspring died or developed AIDS symptoms after receiving
live HIV vaccines.
Last June, the FDA gave VaxGen, Inc., a San Francisco biotechnology company, permission
to start Phase III human clinical trials of a genetically engineered vaccine containing
recombinant forms of two HIV strains. VaxGen, which "is committed to making
an HIV vaccine for worldwide use," is testing its vaccine on 5,000 volunteers
in Thailand and North America, including cities such as Philadelphia and Los Angeles.
Most HIV-negative volunteers who get an HIV vaccination in experimental AIDS vaccine
trials will test HIV-antibody-positive for life. In New York City, technicians
now ask those getting blood drawn if they have volunteered in an AIDS vaccine
trial - stark acknowledgement of a new generation of vaccine-induced HIV positives
who, researchers insist, are not HIV infected.
As public health officials
increasingly define disease control in global, rather than national, terms, mass
vaccination proponents and vaccine makers must find ways to finance delivery of
newer and more expensive vaccines to poor countries. They accomplish this by first
making the vaccinations mandatory in rich countries, as HIV vaccine developer
Stanley Plotkin, MD, of Pasteur Mérieux Connaught explained in 1996: "The
keystone of the [global mass vaccination] system is that the research costs [of
drug companies] are recouped in North America and Europe, and the vaccines are
sold in the developing world at much, much lower margins. . . . The relatively
high rate of childhood vaccination seen lately in most parts of the world is the
result of that system."
Just last year, the CDC illustrated this funding formula by recommending that
all American babies under six months receive three doses of the newly licensed
live rotavirus vaccine for diarrhea. Although a serious health problem in the
Third World, where 870,000 babies lacking adequate nutrition or medical care die
from dehydration caused by severe diarrhea every year, most American and Canadian
babies fully recover from bouts with rotavirus and are left with permanent immunity.
About 20 to 40 babies die of rotavirus infection in the U.S. every year.
Vaccine
production problems and new epidemics
THE ROTAVIRUS VACCINE, WHICH WILL cost $40 a shot in
the U.S., is the first rhesus-human reassortment vaccine, created by co-cultivating
rhesus monkey rotavirus strains with human rotavirus strains to create a genetic
human-monkey hybrid strain of rotavirus. This production process, while more sophisticated,
recalls the use of rhesus monkeys to produce the original Salk polio vaccine.
In the rush to put a polio vaccine on the market in 1955, polio vaccine pioneer
Jonas Salk unknowingly used rhesus monkey kidney tissues contaminated with monkey
viruses. In the late 1950s, after lab technology advances could screen for monkey
viral contaminants, scientists identified simian virus 40 (the 40th monkey virus
identified in the vaccine). SV40 was found to cause cancer in lab animals in 1959,
but by then, some 98 million American children had already received the vaccine.
Today, Michele Carbone, MD, a molecular pathologist at Chicago's Loyola University
Medical Center, and other researchers around the world are culturing out SV40
from cancerous brain, bone, and lung tumors in adults and children in an effort
to understand the inexplicable rise of these rare cancers.
After they discovered the SV40 contamination, polio vaccine makers in the U.S.
switched from the rhesus monkey to African Green monkey kidney tissues to produce
live polio vaccine. However, African Green monkeys can be infected with simian
immunodeficiency virus (SIV) and not appear sick. In 1992, Walter S. Kyle, whose
article "Simian retroviruses, polio vaccine and origin of AIDS" was
published in The Lancet, hypothesized that SIV contaminated both experimental
and general use oral polio vaccines using African Green monkey kidney tissues.
"There could have been multiple crossovers of the SIV virus from monkeys
into the human population at different points in time where, in humans it took
the form of HIV," he wrote. "This may explain why different populations
have been affected at different times with HIV during the past 30 years"
- a time span that correlates perfectly with the dates that those populations
were vaccinated in their respective countries during different phases of the worldwide
polio vaccination campaigns.
At the 1996 Eighth Annual Houston Conference on AIDS in America, a retrospective
scientific analysis by California microbiologist Howard B. Urnovitz, PhD, supported
the thesis that SIV, which is highly similar in genetic structure to HIV-2, may
have contaminated experimental live oral polio vaccines. In some African children
given this contaminated vaccine in the Congo between 1957 and 1959, says Urnovitz,
SIV could have recombined with their own normal genes to create the monkey-human
hybrid now known as HIV-1.
There is no scientific consensus on HIV's origin. Earlier this year, Beatrice
Hahn, MD, and Anthony Fauci, MD, pointing to chimpanzees that Congolese were slaughtering
and eating, announced that they had solved the mystery. Hahn reported that three
West African chimps were infected with SIV strains that very strongly resembled
three HIV subgroups.
Kyle and Urnovitz both challenge these findings. "They
have been eating monkeys in Africa for thousands of years," said Urnovitz.
"Why did HIV only crop up in the late 1950s? The buffet theory of the origins
of HIV just doesn't hold any water. . . . There are many confounding theories
being forwarded, but they all come back to contaminated polio vaccines."
Adds Kyle, "Hahn's discovery could as easily be explained by the fact that
chimps also eat African Green monkeys."
A
Brave New World
IN 1997, CDC OFFICIAL WALTER ORENSTEIN, MD, TESTIFYING
BEFORE THE U.S. Congress, painted a picture of the future in his annual appeal
for more vaccine funding. "On the horizon are vaccine technologies that would
have been considered science fiction just a decade ago but are now reported at
scientific meetings," he said. "Snippets of synthetic DNA have worked
as experimental vaccines in animals. Edible plants have been bioengineered to
become vaccine factories. . . . Vaccines have been enclosed in microscopic capsules,
permitting them to be released slowly over time."
Vaccine researchers are seeking $500 million from all the world's governments
to create a genetically engineered "supervaccine" that will be given
orally at birth. This supervaccine - the CDC and CVI call it the "Holy Grail"
- will contain raw DNA from 20 to 30 viruses, parasites, and bacteria that will
insert itself directly into the cells of babies. The vaccine will be time-released
over several months. Disease organisms scheduled to be included in the supervaccine,
many containing multiple strains or types of each virus, bacteria, or parasite,
are pneumonia (three viruses), AIDS (two viruses), dengue haemorrhagic fever (four
viruses), diarrheal disease (several viruses and bacteria), diphtheria, hepatitis,
malaria (two parasites), measles, meningitis (six viruses and bacteria), polio
(three viruses), schistosomiasis (one parasite), tuberculosis, typhoid fever,
and pertussis.
In all, vaccine manufacturers and U.S. government researchers are developing more
than 150 different viral and bacterial vaccines. A nasal spray flu vaccine targeting
children will be ready by the fall of 2000; adhesive skin patch vaccines and high
technology jet guns will deliver vaccines designed to prevent ear infections,
strep throat, asthma, genital herpes, gonorrhea, stomach ulcers, and even cancer
and the common cold. If the microbe fighters have their way, the "Brave New
World" of the future will truly be infection-free.
Or will it? In 1993, scientists at the American Society of Microbiology annual
meeting reported that diseases such as tuberculosis, meningitis, and gonorrhea
have become resistant to antibiotics because of their overuse in the past decades.
One study shows that pediatricians are prescribing antibiotics to 44 per cent
of children with common colds. In 1998, evidence of penicillin-resistant strep
bacteria caused worry that more people will suffer or die from severe pneumonia,
bacteremia, and meningitis.
Last year, a U.S. Public Health Report warned that the overuse of antibiotics
in animals, which transfers resistant microbes from livestock to humans through
the food chain, is producing resistant bacteria, including antibiotic-resistant
salmonella, enterococci, and E. coli. Health officials warn food producers that
antibiotics should never substitute for "inadequate hygiene."
Now
there are signs that viruses and bacteria, eager to survive, may be outsmarting
vaccines. A 1998 British Medical Journal study found that B. pertussis infection
(whooping cough) is occurring in vaccinated populations in the Netherlands, Norway,
and Denmark despite vaccination rates as high as 96 per cent. Among other causes
of the whooping cough outbreaks, scientists have found an increasing incidence
of strains of B. pertussis with a mutated surface protein.
Last year, a CDC
study identified eight distinct genotypes of a wild-type measles virus in populations
around the world, possibly because the vaccine put pressure on the virus to mutate.
In January of this year, the CDC reported a 1998 measles outbreak in Alaska in
which 51 per cent of the children had received one or more doses of measles vaccine.
Will health officials add yet another booster dose, as they did during measles
outbreaks in the late 1980s when they realized that one dose failed to do the
job?
While the global village gets smaller and smaller, our health officials warn parents
that terrible diseases killing children in the Third World are "just a plane
ride away." The only way to protect yourself and your children, say the doctors,
is to do what we say and use all the vaccines we have created to keep everyone
safe. Yet some parents and doctors, concerned about the future, are looking beyond
the present. "What we forget is that millions of years of evolution have
taken place on this planet, and up until the last 100 years, humans have lived
in relative harmony with microbes. Yes, there have been epidemic infectious diseases
in history, but they have always resolved themselves," said Richard Moscowitz,
MD. "I don't think there is any real appreciation for what we may be doing
by using so many vaccines to try to eradicate so many organisms."
If
we stay the present course, will mankind be free from infectious disease but crippled
by chronic disease? Will eradication of feared diseases, such as AIDS, through
mass vaccination be one of man's greatest triumphs or will we live in fear of
deadly mutations of microbes that have outsmarted man's attempt to eradicate them?
We may look back at the crossroads we are at today and wish we had decided to
make peace with nature instead of trying to dominate it.
Whatever government
and industry decide to do, public support for mass vaccination programs may continue
to erode if public policy precedes science and individual health is dismissed
as less important than the public health. Perhaps the peace we need to make is
not as much with nature, as with ourselves.
References:
1Dublin, L. Health Progress, l935-l945, New York: Metropolitan Life Insurance Company, l948, Page l2.
2Diodati, CJM, Immunization: History, Ethics Law an Health, Integral Aspects Incorporated, Windsor, Ontario, l999, pp. 104-l06.
3In the text,Vaccination, l00 Years of Orthodox Research Shows that Vaccines Represent a Medical Assault on the Immune System, by Vera Scheibner, Ph.D.,l993, available from New Atlantean Press, PO Box 9638-925, Santa Fe, NM 87504, pp. 33-46. (The Swedish experience with pertussis exemplifies the relative mildness of this disease today in Western nations compared with earlier times. In l979 Sweden banned the pertussis vaccine because of a return of the disease in fully vaccinated children and also because of unacceptable side effects, including brain damage. In spite of this ban, which remains in effect today, Sweden has one of the lowest infant mortality rates in the world. Pertussis remains mildly endemic in Sweden, but complications remain uncommon and virtually unchanged since l979.)
4Stratton, KR, CJ Howe, and RB Johnston, Jr., Editors, Adverse Events Associated with Childhood Vaccines; Evidence Bearing on Causality, Institute of Medicine, National Academy Press, Washington, DC, l994, pp. 2ll-236.
5Buttram, HE, The National Childhood Vaccine Injury Act: A Critique, The Townsend Letter for Doctors and Patients, Oct. l998, pp. 66-68.
6Incao, Philip, Supporting children's health,, Alternative Medicine Digest, Issue l9, pp. 54-59.
7One survey showed a 46% increase in death rate nationwide from asthma between l977 an l99l (Phildelphia Inquirer, December 8, l994, A22). In some areas, the incidence of asthma has increased 200% in the past 20 years (The Human Ecologist (National HEAL), fall l992, (55):6.
8Shaneen, SO et al, Measles and atopy in Guinea-Bissau, Lancet, Vol 347, June l9, l996, pp. l792-l796.
9Odent, MR, Pertussis vaccination and asthma: is there a link? J Am Med Ass'n,, Vol 27l, l994, pp. 229-23l
10Alm, JS et al, Atopy in children of families with an anthroposophic lifestyle, Lancet, Vol 353, May l, l999, pp. l485-l488.
11Kemp, T et al, Is infant immunization a risk factor for childhood asthma or allergy? Epidemiology, Vol 8(6), Nov. l997:pp. 678-680.
12Lisa Jennings, Increasing Ritalin doses in school children questioned, The Intelligencer (newspaper, Doylestown, PA), September 2l, l998, pp. Dl-D2.
13Changes in the Population of Persons with Autism and Pervasive Developmental Disorders in California's Developmental Services System: l987 through l998, a Report to the Legislature, March l, l999, Department of Developmental Services, l600 North Street, Room 240, Sacramento, CA 958l4.
14Assessment, Evaluation and Support Unit, Special Education
Division, California Department of Education.
Total Enrollment and Percent
of Pupils with Disabilities by Federal office of Special Education Programs, New
Jersey State Department of Education.
Illinois State Board of Education Report
(8/20/98). Rhode Island Department of Elementary and Secondary Education, annual
Statistical Reports.
Sixteenth through Twentieth Annual Reports to Congress
on the implementation of The Individuals with Disabilities Education Act, <http://www.ed.gov/offices/OSERS/OSEP/OSEP94-98AnlRpt/>
15Singh, V & Yang, V. Serological association of measles virus and human herpes virus-6 with brain autoantibodies in autism, Clinical Immunology and Immunopathology, Vol 88(l):l998, pp. l05-l08.
16Wakefield, AJ et al, Ileal-lymphoid-nodular hyperplasia, non-specific colitis, and pervasive developmental disorder in children, The Lancet, Vol 35l, Feb. 29, l998, pp. 637-64l.
17Kumar, S & LK Miller, Effects of serial passage of Autographa California nuclear poly hedrosis virus in cell culture, Virus Reseach, Vol 7, l987: pp. 335-349.
18Jahnke, U et al, Sequence homology between certain viral proteins and proteins related to encephalomyelitis and neuritis, Science, Vol 29, July l9, l985, pp. 242-284.
19Horowitz, Leonard, DMD, MA, MPH, Emerging Viruses, AIDS and Ebola, tetrahedron Publishing Group, Rockport, MA, l997, pp. 488-493.
20Martin, WJ et al, African green monkey origin of the atypical cytopathic "stealth virus" isolated from a patient with chronic fatigue syndrome, Clinical and Diagnostic Virology,Vol 4, l994, pp. 93-l03.
21Martin, WJ et al, Stealth virus epidemic in Mohave Valley, I: Initial report of virus isolation, Pathobiology, Vol 65(l), l997, pp.35l-356.
22Lederberg, Joshua, Letter-to-the-Editor, Science, Oct. 20, l967, p. 3l3.
23Gupta S et al, Dysregulate immune system in children with autism, beneficial effects of intravenous globulin on autistic features, J of Autism and Developmental Disorders, Vol 26(4);l996, pp. 439-452. (In this article on page 450 it is stated, "We theorize that the high titers of rubella antibody…presented in mothers of children with autism would be transplacentally transferred and may persist for a prolonged period in the child. When such a child gets MMR immunization, rubella antigen may complex with preexisting antibodies, and such complexes might play a role in pathogenesis of autistic features.")
24Immunologic findings in children with abnormal reactions after vaccination, Czechoslovakia Pediatrics, Vol 48(l), January, l993, pp. 9-l2.
VACCINES
MADE FROM ABORTED BABIES
AND ALTERNATIVES
SOURCE:
http://www.dgwsoft.co.uk/homepages/vaccines/usvaccines.html
We have also had an increasing number of queries from other parts of the world, in particular from the USA, and as a result I have prepared this page of information for US readers. For more information and to join the campaign to make ethical vaccines available in the US please go to www.cogforlife.org
Disease | Brand name | Manufacturer | Cell lines (Human fetal) |
Polio | Poliovax (polio-E-IPV) | Pasteur Merieux Conaught Labs USA | MRC5 |
Measles, mumps, rubella | MMR II | Merck Sharp & Dohme | WI-38 |
Rabies | Imovax
HDCV DCO | Pasteur Merieux Connaught Pasteur Merieux Conaught | MRC5 ? |
Hepatitis A | Havarix VAQTA | Smithkline
Beecham MSD | MRC5 MRC5 |
Chickenpox | Varivax | MSD | WI-38 |
Disease | Brand name | Company | Cell line |
Polio | IPOL (L)
Orimune (L) | Pasteur-Merieux Connaught Lerderle Labs | Monkey kidney & calf serum Monkey Kidney cells |
Mumps | Mumpsvax (L) | Provaccine, Switzerland Merck Sharpe & Dohme USA | Chick embryo |
Measles | Attenuvax (L) | Merck sharpe & Dohme USA | |
Rubella | Takahashi Strain (UL) | Kitasato Institute | Rabbit Kidney |
Rabies | (RVA )(L)
RabAvert (PECE) (L) | Smithkline -Beecham
Chirion Bering Gmbl & Co | Rhesus Monkey Chick embryo |
Hepatitis A | Aimmugen (UL) | Chemo-therapeutic Institute Japan (Kaketsuken) | Monkey Kidney |
Flu | All brands (L) | All manufacturers | Chick embryos |
Yellow Fever | YF-Vax (17D) (L) | Pasteur Merieux Connaught | Chick embryo |
Japanese Encephalitis | JE-Vax (L) | Biken Osaka, Distributed by Connaught | Mouse derived |
Smallpox | (L) | Supplied
by CDC For Laboratory Workers and Military | Calf Lymph |
The following diseases are bacterial and are made on
nutrient solutions and not on living cells . As no fetal cells are used
there is no ethical problem from a prolife point of veiw .( Whether all vaccines
required for school entry are medically advisable is debatable and not an
issue I am covering in this site)
Whooping cough,tetanus,diptheria , bacterial
meningitis, typhoid, tuberculosis and anthrax.
Influenza vaccines are usually
made on chicken cells although this is a viral disease.Hepatitis B
is grown
on yeast cells..
We are not sure whether measles and mumps vaccines are available throughout the USA although one contact in Kentucky has obtained these from Merck. I have written to Merck to confirm whether they will still supply these vaccines . Both are from chick cell lines. Please E mail me if you have any information on the the availability of these vaccines . Please say if you are writing from the USA and if you wish which state you are from.
State law regarding vaccination for school entry
Most US states require children to be vaccinated for kindergarten, school and college entry. However exemptions may exist for parents who have a conciencious objection. I will try to add details of the laws in states as I find out about them.
Minnesota
Informed
Consent /German Measles Vaccine
(
submitted by Christina Abel RN (Ret.)
In the state of Minnesota, children can go to school without being vaccinated. A notarized signature is all that is required to be in compliance with the 1980 Minnesota immunization law, M.S. 123.70 Subd. 3(d) and in 1989, for post-secondary students, M.S. 135A.14 Subd. 3(b).
Information on Rubella vaccine submitted by Christina Abel RN (Ret.)
Alternatives
to vaccines made from aborted babies (Introduction,
British and International information)
News
Back to Index
Some to other vaccine sites (we take no responsibility for the content of these sites)
More information on state exemptions http://hometown.aol.com/Tauwillow/exemptio.htm
Homeophathic alternatives to vaccines http://www.lyghtforce.com/HomeopathyOnLine/text/gold
Join The Campaign for Ethical Vaccines US. Please
go to www.cogforlife.org
(Please
note cogforlife will shortly be taking over running this page.)
Shows the Center of Disease Control, US Gov., does not approve of blanket vaccination of the population: http://www.cogforlife.org/smallpoxforum.htm
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