|
Unlike some doctors and scientists listed and
quoted on this site, Dr. Buttram believes that vaccines are able
to prevent some diseases in some people some of the time. However,
he has serious concerns about saftety, supported by scientific findings.
http://www.mercola.com/2001/jun/9/vaccine_update.htm
Dr. Mercola's Comment:
Dr. Buttram has done an
outstanding job of providing an accurate and current overview of
this complex area. I am constantly amazed at how he consolidates
this information. He is to be hugely congratulated for his hard
work in compiling this information and giving such a balanced and
accurate perspective of the central issues that are involved.
Dr. Buttram is a gentle
humble God loving man and one of the major pioneers in the vaccine
awareness movement. I have known his associate Dr. William Kracht
for many years.
If you are on the east coast
and require physicians who believe and apply most of what I recommend
in this newsletter I could not recommend their clinic more highly.
Woodland Medical Center
5724 Clymer Road
Quakertown, PA 18951
215-536-1890
Vaccine Scene 2001: Update and Overview
Harold E Buttram, MD
April 16, 2001
In our office 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 most important point is parental choice!
Therefore, we ardently believe the best approach to this very controversial
subject is to present both the pros and cons, 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 small incidence of stomach or intestinal bleeding
as a potential long-term side effect.
As you read the following monograph, please keep these key points
in mind in terms of "effectiveness" versus "safety"
of vaccinations:
Scientific evidence does support the effectiveness of immunizations.
They do prevent infectious diseases; some better than others, but
this point is not disputed.
Scientific evidence does not support the safety of immunizations:
Safety studies on vaccinations are limited to short time periods
only: several days to several weeks. There are NO (NONE!) long-term
(months or years) safety studies on any vaccination or immunization.
There is limited but rapidly growing scientific evidence of long-term
adverse side effects of vaccines that need much more study.
In August, 1999 and April, 2000 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 1,000 people were in attendance,
the great majority of whom were parents of autistic children. At
one point in the meeting, when the chairman asked those in the audience
who believed that their child's autism was caused by vaccines to
stand, a largely majority of the audience rose to their feet.
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.
Are the Benefits of Vaccines Exaggerated?
From an historical perspective it is important to keep in mind
that, in the early days of immunizations, there were relatively
few vaccines, and for the most part they were given separately.
Also, it would appear that it was in those early days that vaccines
had their greatest successes, with eradication of smallpox from
the world (although there are disturbing reports of current appearances
in parts of the Far East), and eradication of polio from the Western
Hemisphere, the last case of wild polio having taken place in 1979.
Parenthetically, the average person today believes that mass smallpox
vaccines were responsible for eradicating smallpox from the world.
This is not so, for the simple reason that mass vaccination programs
did not take place in many areas. In some third world countries
10% or less of the populations were immunized against smallpox due
to financial and other limitations, which necessitated a policy
of "quarantine and containment," whereby all contacts
in an infected village and outlying areas were immunized.
If limited vaccines together with quarantine were effective in
the case of smallpox, this raises question about the necessity of
ongoing mass vaccines in other diseases as well, a question which
we believe will assume growing importance as more is learned about
the adverse effects of vaccines.
Among vaccine's other successes, there were less than 100 reported
cases of measles in the U.S.A. in 1998, and most of these were imported.
However, 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 1935 the four leading causes of childhood deaths from
infectious diseases in the U.S.A. were
* diphtheria
* pertussis (whooping cough)
* scarlet fever
* measles
However, by 1945 the combined death rates from these causes had
declined by 95% before the implementation of mass vaccine programs.(l)
Other statistical information provided much the same pattern.(2)
According to a report in Morbidity and Mortality Weekly Report,
July 30, 1999, improvements in
* sanitation
* water quality
* hygiene
and the introduction of antibiotics have been the most important
factors in control of infectious diseases in the past century. Although
vaccines were mentioned, they were not included among the major
factors.(3)
Another factor, which is commonly overlooked, is that the virulence
of micro-organisms tends to be weakened or attenuated with the passage
of time and with the serial passages through human hosts.(4)
Also, populations develop immunity with continued or repeated exposure.
One example of this is whooping cough (pertussis) which is clearly
a milder disease in Western nations than it was 100 or so years
ago.
An example of this process is provided in the text, Vaccination,
100 Years of Orthodox Research Shows that Vaccines Represent a Medical
Assault on the Immune System, by Vera Scheibner, Ph.D.,(5) in which
the author reviews the Swedish experience with whooping cough (pertussis)
and the pertussis vaccine.
In 1979 Sweden banned the pertussis vaccine because of a return
of the disease in fully vaccinated children and also because of
side effects which they considered unacceptable, including brain
damage.
In spite of this ban, which remains in effect today, the infant
mortality in Sweden from pertussis is no greater than in fully vaccinated
populations (3 infant deaths were recorded in Sweden 1987 to 1991,
as compared with 4 infant deaths in New South Wales, Australia,
during a slightly longer time period).
However, it must be recognized that pertussis remains a serious
illness in many third world countries, carrying significant morbidity
and mortality due to factors which often include poor sanitation
and lack of adequate medical facilities. Also many are "virgin
populations" in which whooping cough is a relatively new infection,
and therefore they are lacking in natural immunity which is present
in most Western nations where there is inherited immunity from earlier
epidemics.
Vaccine Safety not Proven:
It should be pointed out that today's children receive from 22
to 35 vaccines before school age, whereas most of today's senior
citizens received only one, the smallpox vaccine. Some of the vaccines
contain mercury, a known neurotoxin under some circumstances.
With the growing public concern 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 1994 special committee of
the National Academy of Sciences (Institute of Medicine) published
a comprehensive review of the safety of the hepatitis B vaccine.
When the committee, which carries 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
safety research had not been done. Furthermore, they found that
serious "gaps and limitations" exist in both the knowledge
and infrastructure needed to study vaccine adverse events.
Among the 76 types of vaccine adverse events reviewed by the IOM,
the basic scientific evidence was inadequate to assess definitive
vaccine causality for 50 (66%). The IOM also noted that "if
research ... (is) not improved, future reviews of vaccine safety
will be similarly handicapped.(6)
The clear implication of this report, which in our experience is
fairly representative of a haphazard pattern towards issues of safety
throughout the vaccine field, is that adverse reactions to the vaccines
may be occurring on a large scale without being recognized as to
their true nature.
In support of this statement, two pioneering studies will be reviewed
below, one from 1955 and the other from 1984, both sounding alarms
on potential side effects from vaccines:
One of the most intriguing studies from older medical literature
dealing with the pertussis vaccine was that of A.L. Low (Chicago,
1955) who performed electroencephalograms (EEGs) on 83 children
before and after pertussis immunization.
In 2 of these children he found that the EEGs turned abnormal following
the immunizations without other signs or symptoms of abnormal reactions.
In his report he commented: "This study shows that mild but
possibly significant (emphasis ours) cerebral reactions may occur
in addition to the reported very severe neurological changes."(7)
Another intriguing study, this one from Germany, was reported in
a little-noted letter-to-the editor in the New England Journal of
Medicine, in 1984.(8) In the study, a significant though temporary
drop of T-helper lymphocytes was found in ll healthy adults following
routine tetanus booster vaccinations. Special concern rests in the
fact that, in 4 of the subjects, the T-helper lymphocytes fell to
levels seen in active AIDS patients.
The implications of these two studies are enormous.
In regards to the latter (German) study, if this was the result
of a single vaccine in healthy adults, it is sobering to think of
the possible consequences of multiple vaccines (19 vaccines within
the first six months of life at latest count) given to infants with
their immature and vulnerable immune systems. Unfortunately, other
than clinical observations, we can only speculate as to these consequences,
as this test has never been repeated.
As for the Low study with EEGs before-and-after pertussis immunization,
at a time when myriads of our children are suffering from various
degrees and phases of brain dysfunction, it is possible that vaccine
reactions may be occurring on a large scale, unrecognized as to
their true nature, and contributing to this pool of unfortunate
children.
It is both sad and shameful that neither of these studies have
had follow-ups in American laboratories and medical centers, as
should have been the case. Had they been done, discovering and documenting
adverse neurological and immunological effects of the vaccines,
they would have led to safer forms and combinations of childhood
vaccines than at present.
From a careful gleaning of medical literature over many years,
we have been able to find only 3 other reports in the literature
of studies done before-and-after immunizations, all from foreign
medical centers:
In a study from Japan, immunizations (DPT, DT, or BCG) were given
to 61 children with a history of febrile seizures or epilepsy, who
had not had a seizure for one year. Following immunizations there
was a significant increase in "epileptic spikes" in post-vaccine
electroencephalograms as compared with those done preceding vaccines.(9)
In January, 1993, a Czechoslovakian medical journal published
the results of a study of 89 children with adverse clinical reactions
following administrations of various combinations of vaccines. 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 clinical reactions.(10)
In 1997 a study from the University of Alberta, Canada, reported
on
findings from before-and-after MMR vaccine in which the effects
on both
the measles specific antibodies and cell mediated immunity, as indicated
by cytokine generation, were tested.(11) The significance of this
report may not rest so much on the specific findings, which will
be reviewed later, as on the fact that it opens up an entirely new
avenue of research, designed to reveal the specific mechanisms of
actions of the vaccines, and also possibly revealing their side
effects.
With these 3 reports from reputable medical centers, published
in peer-review journals, the flood-gates of medical research have
been opened. The truth about vaccine mechanisms, effects, as well
as adverse reactions cannot be long in following. Although late,
we would hope that our own medical and research centers would join
in this search.
What Is Known about Adverse Vaccine Reactions:
(A Cursory Review of the Literature)
Before turning to medical and scientific reports on adverse vaccine
reactions, we must reluctantly point out an almost insuperable difficulty
in getting dependable data on these reactions due to the extreme
reluctance of doctors to report on vaccine reactions, a pattern
which has existed since the earliest days of childhood vaccines.
There are a number of reasons for this. From their earliest years
of training, medical doctors have been taught to look upon vaccines
as one of the greatest achievements in medical science, and any
question about them is often looked upon as disloyalty to the profession.
In addressing this issue in the classic text, Shot in the Dark,
by Coulter and Fisher, the authors quoted an attorney specializing
in vaccine-damaged children.
In commenting on the deficiency in doctors' reporting of vaccine
reactions, the attorney commented, "As is the case with many
pertussis-vaccine-injured children, none of the treating physicians
would commit themselves to a final etiological diagnosis. It is
strange that parents of pertussis-vaccine-damaged children often
can only get an etiological diagnosis by hiring an attorney and
seeing one of the few recognized experts in the U.S. on post-pertussis
vaccine encephalopathy."(12)
In passing, we believe it is appropriate to mention that we have
noticed this same pattern in our office. Having seen quite a few
autistic children in the past several years, more than a few of
which became autistic in a time-related fashion following vaccination,
we have yet to see a single case in which other doctors have implicated
vaccines as a possible cause of the autism.
Recombinant Hepatitis B Vaccine - Anecdotal Reports of Adverse
Reactions:
A scattering of reports suggest that the hepatitis B vaccine may
play a major role, as yet largely unrecognized in hemorrhagic complications
from vaccines. In a collection of abstracts from Medline research
from l990 to October, 1997 on adverse reactions from the recombinant
hepatitis B vaccine, Dr. Andrea Valeri of Italy catalogued a total
of 45 different types of reactions in the world literature.(13)
Among these were necrotizing vasculitis,(14) vaccine-induced autoimmunity,(15)
and segmentary of occlusion of the central retinal vein.(16) In
addition, a report of vasculitis following hepatitis B vaccine is
found in the British Medical Journal.(17)
Thrombocytopenia is listed as a possible complication in the current
Physicians' Desk Reference. In a report of 18 deaths of neonates
following the hepatitis B vaccine by the Vaccine Adverse Event Reporting
System, 1991-1998, hemorrhagic phenomena were common including 2
with cerebral hemorrhages, 4 with pulmonary bleeding, l with bloody
diarrhea, and several with blood in upper airway passages.(18) A
report in Post-Graduate Medicine on acute hemorrhagic encephalitis
sites vaccines as one of the possible causes.(19)
Reports of autoimmune/neurological type reactions from hepatitis
B vaccine include the following:
optic neuritis(28) myasthenia gravis(23) Reiter Syndrome and arthritis(32)
uveitis(21) rheumatoid arthritis(31)
CNS demyelination(25-27)
autism & colitis(33) transverse myelitis(29) Guillain-Barre
Syndrome(22)
visual loss(30) Polyneuropathy(20) erythema nodosum(24)
Tetanus and Hemophilus Influenza (Hib) Vaccines:
The tetanus vaccine does not carry an aura of controversy which
surrounds some of the other vaccines, but in l991 a report by the
National Institute of Medicine did find a causal relation between
the tetanus vaccine and anaphylaxis, a potentially life-threatening
allergic reaction.(34)
The Hib vaccine shares with the pertussis vaccine a notoriety for
its sensitizing potentials,(35) so much so that it has a paradoxical
reaction in causing a temporary reduction in antibody in most adults
and children following immunization, which may increase the risk
of invasive disease should the individual be harboring H influenza
micro-organisms at the time of the Hib immunization.(36)
Pertussis (Whooping Cough) and Vaccine-Induced Encephalitis
The Pertussis vaccine carries the dubious distinction as having
survived the longest period of controversy among any of current
vaccines. This controversy mainly surrounds reports of pertussis-vaccine-induced
encephalitis which have beset the vaccine since its earliest days
in the late l920's and l930's. It is true that public health officialdom
maintains that there is no controversy and that brain damage from
the vaccine is extremely rare.
However, there are many parents as well as a growing number of
physicians and researchers, though still a minority, who consider
the pertussis vaccine potentially dangerous.
For those who are interested in a more in-depth review of this
intriguing subject, we recommend the following 3 books: Shot in
the Dark by Coulter and Harris(12), Vaccination ... , by Vera Scheibner,
Ph.D.,(5) and Vaccination and Behavioral Disorders, by Greg Wilson,(37)
The basic question surrounding the pertussis vaccine is whether
or not, by itself or in combination with other vaccines, it is contributing
to the epidemic of neurobehavioral problems now taking place among
American children as a result of subtle encephalitic-type brain
damage from the vaccine.
At the very least, the studies of Low(7) and Nuono(9) suggest this
as a possibility.
This question, which has never been addressed in a meaningful way,
becomes of over-riding importance in view of the current adverse
health trend among American children, as reflected in an article
in a major news magazine which cited a "dramatic rise in learning
disabilities among American children" with "one of every
six suffering from autism, aggression, dyslexia, or attention deficit
hyperactivity disorder."(38)
Could it be that modern medicine has a huge blind spot to a medical
problem taking place on a large scale? Historically it has happened
before, as in the case of the Austrian obstetrician, Ignaz Semmelweis,
who in the mid l800's was unable to convince his peers to wash their
hands before delivering babies or performing surgery.
Returning now to our review of the literature, medical reports
of pertussis-vaccine-induced encephalitis, rare at any time in the
past, have virtually ceased since the early 1990's when a series
of articles appeared in major medical journals attempting to dismiss
encephalitis-like events following the pertussis vaccine as coincidental.(39-41)
For this reason, aside from earlier literature, one must search
elsewhere to gain some insight into the nature and frequency of
adverse pertussis-vaccine reactions taking place today. Although
research in this area is largely stagnant, there are a few highly
pertinent animal studies which help define the nature of pertussis
endotoxin and its potentially damaging effects on the brain.
Turning to these animal models, attempts to dismiss pertussis-vaccine-encephalitis
as a myth would appear to founder or should have foundered from
the outset based on the simple fact that vaccines like pertussis
are actually used to induce encephalitis (experimental allergic
encephalomyelitis) in laboratory animals.(42)
Among animal models, four will be cited here:
In an experimental encephalomyelitis performed by Munoz and coworkers,
elicited in mice by injecting pertussigen, a derivative of Bordetella
pertussis, along with mice spinal cord extract, there were histological
findings of perivascular infiltrates, consisting largely of lymphocytes
in the brain and spinal cord.(43)
Although Munoz mentioned nothing about the presence or absence
of brain edema, Iwasa stressed the finding of brain edema as a feature
of pertussis-induced encephalopathy.(44) Parenthetically, there
are anecdotal reports of brain edema in infants who showed signs
of increased intracranial pressure, as manifested by bulging fontanelles,
following DPT immunizations.(45-47) Also, in 1972 Galazka reviewed
autopsies of children who died following the pertussis vaccine.
Although limited in number, findings included brain edema, hyperemia,
and soft meninges.(101)
In a study devised to provide an animal model for the systemic
and neurological complications sometimes observed following the
pertussis vaccine in children, Steinman and coworkers discovered
a lethal shock-like syndrome in mice after immunization with B pertussis
vaccine and sensitization to bovine serum albumin. Post-mortem examination
of the brains revealed diffuse vascular congestion and hemorrhages
in both cortex and white matter.(48)(Emphasis ours)
In a review of the effects of bacterial endotoxin in microcirculation
of the body, McCuskey described the effects of endotoxin in causing
vascular inflammation, leading to a pro-coagulation state of the
endothelium.(49)
Other than those articles previously mentioned, and a few to be
reviewed in a subsequent section of this paper dealing with allergies,
there is a virtual vacuum of meaningful information in the current
literature on the pertussis vaccine and vaccine-induced encephalitis.
However, there is one area which promises to be fruitful in clinical
and scientific knowledge about this field, however tragic it may
be from a human standpoint:
There are at present increasing rates of imprisonment of parents
or caretakers on conviction of infant deaths from the "shaken
baby syndrome."(SBS) From first hand knowledge of one case
and familiarity with others, we believe with virtual certainly that
some of these convictions have been the result of misdiagnosis,
the true cause of deaths having been vaccine reactions.(50)
In one case, for instance, 6 vaccines were given at 8 weeks of
age to a severely compromised baby. Following a period of clinical
deterioration, the baby became apneic about 14 days following the
vaccines and, although later resuscitated in a hospital, died shortly
after.
The father was subsequently charged with death of his infant from
SBS. During the subsequent jury trial, vaccines were never mentioned
by any witness or offered as a possible cause of the infant's death.
As a result of this and other factors, the father was convicted
of murdering his infant son and is now serving a life-sentence.
If the truth were known, probably this story could be told many
times over.
The MMR Vaccine (Measles - Mumps - Rubella) and Autism:
Probably the greatest concern with vaccines today rests with their
possible causal relationship with the growing epidemic of neurobehavioral
problems, especially autism, as reviewed in the previous section.
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 these disorders in recent years.
In regards to autism, probably the best statistics come from California,
where a survey mandated by the California state legislature found
a 273% increase incidence during the previous ll years.(51) Reports
from education departments of several states and reports from the
U.S. Congress on the rapidly increasing needs of classrooms for
developmentally delayed children reflect comparable changes throughout
the nation.(52)
As clearly shown in a graph prepared by Bernard Rimland, Ph.D.,
founding director or the Autism Research Institute with headquarters
in San Diego, sharp rises in the incidence of autism in the U.S.A.
took place immediately following the introduction of the MMR vaccine
in l975, and in the United Kingdom following its introduction in
l988.(53)
In our own practice we have carried out a partial sampling of the
charts of autistic children seen here in the year 2000. Among 32
charts that were reviewed, it was found that in 16 cases (50%) the
onset of autistic features in a previously normal child took place
in a time-related fashion following the MMR vaccine.
It is important to point out that an uncombined measles vaccine
had been in use in the U.S.A. since 1961, with only a slight rise
in autism from 1961 to 1975 when the combined MMR vaccine came into
use, bringing with it the sharp increases in autism. As a result
of this, some are coming to believe that the 3 vaccines should be
given separately, about which more will be said later.
In our opinion, one of the prime researchers in the field of autism
is Vijendra Singh, Ph.D., Department of Biology, Utah State University,
who 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).(54)
If the MMR vaccine is causing autoimmune reactions, what would
be the mechanism?
Although research in this area is in its infancy, we do know this:
Both 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 incorporate genetic material from the tissues in which
they are cultured.(55)
Furthermore, protein sequences in the measles virus have been found
to have similarities to those found in brain tissues, (56) so that
by the process of "mimicry," the formation of antibodies
against one may cross react with the other, which the work of Dr.
Singh tends to confirm.
As another factor, it is possible that the reaction rates in the
second-generation vaccine recipients of today may be happening on
a much larger scale due to previous sensitization of mothers from
their vaccines, this sensitization being transmitted in turn to
the fetus.(57)
A second prime researcher in the field of autism, in our view,
is Dr. Andrew Wakefield, Reader in experimental gastroenterology,
Royal Free Hospital and University College Medical School, London.
This researcher and coworkers were the first to suggest a possible
link between the triple MMR vaccine and clinical combination of
autism with bowel disorder, now referred to as the autistic enterocolitis
syndrome.
As a result Dr. Wakefield has become the center of a storm of controversy
in the United Kingdom, as well as a highly sought speaker at conferences
in the U.S.A. Although coauthor of many peer-reviewed clinical and
scientific papers, the course of Dr. Wakefield's pioneering work
in this field can be found in a series of three articles,(58-60)
as well as his presentation to the United States House of Representatives
Committee on Government Reform, April 6, 2000.(61)
In summary, Dr. Wakefield and coworkers have studied over l50 developmentally
delayed children with colitis, in which enlarged and inflamed intestinal
nodes are a prime feature. Wakefield stressed that patterns in these
children appear to be distinct from other forms of inflammatory
bowel disease, such as Crohn's disease and ulcerative colitis.
Working in collaboration with a state-of-the-art laboratory in
Ireland, subsequent molecular studies from intestinal biopsies performed
on these children detected measles virus genetic material in 24
out of 25 specimens (96%), in contrast with only 5% of detected
measles virus in control specimens sent in a "blinded"
fashion.
In explaining the ability of the MMR-derived measles virus to establish
itself in the intestinal mucosa of affected children, Wakefield
cited earlier reports warning of the potential of viral interference
in the triple MMR vaccine, whereby one virus could interfere with
another.(62,63)
Commenting on these early articles, Wakefield stated,
"The ability of mumps virus to interfere with the cellular
immune response to certain strains of measles virus and thereby,
in particular combinations potentially to reduce viral clearance
and increase the risk of persistent (intestinal) infection, is an
intriguing hypothesis to some of those involved in the current debate."(61)
Parenthetically, Dr. Wakefield is not opposed to the measles, mumps,
and rubella vaccines, but he does believe that their administration
should be widely separated.
In an article just released at time of this writing in the Adverse
Drug Reaction & Toxicology Review,(64) Andrew Wakefield and
coauthor Scott Montgomery carefully reviewed the inadequacies of
the early pre-licensing trials of the MMR vaccine with a maximum
follow up of 28 days and even shorter periods in some of the studies.
They stressed that such short periods of observation following
the vaccine were totally inadequate to detect delayed reactions,
including pervasive developmental delay (autism), immune deficiencies,
and inflammatory bowel disease, which are known from earlier published
reports to occur following both the natural measles infection and
the measles vaccine.
Again the authors reviewed earlier evidence of viral interference
in which the near proximity in time of the natural infections of
mumps, measles, chicken pox, and other viral infections in the pre-vaccine
days resulted in increased incidence of autism and enterocolitis.
This is particularly true because the measles virus is an enteropathic
virus capable of causing acute gastroenteritis, mesenteric adenitis,
and ileocolitis.
Perhaps the most interesting feature of the article is that it
was reviewed by four leading British authorities, all of whom had
previously held positions in the regulation and licensing of medicines.(65)
Taken as a body, the reviewers were supportive of the Wakefield/Montgomery
paper, three highly so. Two of these will be quoted here:
Professor Duncan Vere, former member of the Committee on the Safety
of Medicines, agreed that the periods for the tests were too short.
"In almost every case," he wrote, "observations periods
were too short to include the time of onset of delayed neurological
or other adverse events."
He also added, "one not insignificant detail is whether compensation
for vaccine damage is available to an injured child and family,
or is denied by the authorities who advocate the vaccine whilst
denying the risks on the inadequate (if extensive) evidence available."
Peter Fletcher, formerly a senior professional medical officer
for the Department of Health wrote, "being extremely generous,
evidence on safety (of the MMR) was very thin." Noting that
single vaccines for measles, mumps, and rubella already existed,
he argued, "caution should have ruled the day ... The granting
of a product license was definitely premature."
Childhood Immunizations and the Increasing Incidence of Atopy (Allergies):
The increasing incidence of allergic disorders in Western nations
is now universally recognized, with every third child in industrialized
societies having an allergic disorder.(66) In some areas the incidence
of asthma has increased 200% in the past 20 years.(67) Another survey
showed a 46% increase in death rate nationwide from asthma between
1977 and 1991.(68)
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 membranes.(69)
In contrast, 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, eczema, nasal allergies, food
allergies, and a general pattern of sickness in today's children.
It has not gone unnoticed that the increasing incidence of atopic
disorders has coincided in a time-related fashion with the childhood
vaccine programs, and reports are now appearing from widely separated
geographic areas in which vaccinated children were found to have
significantly more allergic disorders than children with limited
or no vaccines.(70-73)
The suspected role of the pertussis vaccine in potentiating allergic
disorders tends to be confirmed in animal studies(74-76) as well
as a human study.(77) Thimerosol, an organic mercurial compound
widely used as a preservative in vaccines, also has been studied
for its sensitizing properties.(78)
Among these, the study by Kosecka and coworkers(74) deserves special
emphasis: In the study rats were sensitized to ovalbumin (OA) by
injection of OA alone or together with a very small dose of pertussis
toxin. In each group secretory responses to nerve stimulation, serum
IgE levels, and intestinal mast cell counts were determined.
It was found that sensitization was very transient (14 days) when
OA was given alone but when the OA was combined with pertussis toxin,
the intestinal mast cell count, serum IgE levels, etc, remained
elevated for 8 months. The authors concluded that their findings
indicated that when tiny amounts of pertussis toxin were administered
with a food protein, it would result in long-term sensitization
to the antigen and altered intestinal neuroimmune function.
Are Vaccines Skewing the Human Immune System?
In brief summary, the immune system is divided into two major classes:
Cellular immunity, in which the mucous membranes of the body play
a prominent role, and humoral immunity, with the production of antigen-specific
antibodies by plasma cells in the bone marrow.
Cellular immunity, which involves macrophage activation and the
cytotoxic T lymphocyte as its major agents, is responsible for control
of viruses, fungi, as well as bacteria. Humoral immunity, on the
other hand, is predominantly involved in control of bacteria.
Both of these classes are governed by TH lymphocytes, the "T"
referring to the thymus gland, from which they are derived, and
the "H" referring to a helper or activating activity.
Early in life these "naïve" or uncommitted TH lymphocytes
are differentiated into either armed TH1 cells, which governs in
cellular immunity or armed TH2 cells, which governs in humoral immunity.
This initial differentiation , at which naïve TH cells become
either armed TH1 cells or armed TH2 cells has a critical impact
on the outcome of adaptive immune response, depending on whether
it is dominated by macrophage activation of the former or antibody
production of the latter.(79)
It has been found that this differentiation is profoundly affected
by cytokines, which are produced by lymphocytes and serve as chemical
messengers. The two cytokines, Interleukin 12 and Interferon gamma,
in vitro, tend to promote the development of TH1 cells. Interleukin
4, 5, 6, and 10, on the other hand, tend to promote the differentiation
of TH2 cells.(80)
Once one subset becomes dominant, it is difficult to shift the
response to the other subset, as the cytokines from one subset tend
to dominate the other. The overall effect is that certain reponses
are dominated either by humoral (TH2) or cell-mediated (TH1) responses.(81)
Among the different cytokines, some have been shown to have damaging
effects: Interleukin I may cause increased blood brain barrier permeability
and meningeal inflammation(82) and brain damage in experimental
animals.(83) Interferon-gamma has been found to reduced the intestinal
barrier and increase permeability,(84,85) and to bring about profound
morphological, functional, and permeability changes in human brain
blood-vessel endothelial cells.(86)
The study by Pabst and coworkers, previously mentioned as the first
of its kind, with the testing of cytokines before-and-after the
MMR vaccine, found that the predominant response was an increase
in interferon-gamma.(11) As has just been shown (references 84 and
85), interferon gamma increases intestinal permeability. Does this
tie in with the findings of increased intestinal permeability that
has been found in children with autism(87) and consequently with
the MMR vaccine?
In both the New England Journal of Medicine(88) and the journal,
Thorax,(89) articles have appeared stating that a healthy immune
system has a "bias" towards the TH1 immune system, while
people with allergies, asthma, and diseases of an autoimmune origin
have what is known as the TH2-skewed immune response. However, either
antibodies or T cells of the cellular immune system can cause tissue
damage in autoimmune diseases.(90)
A study of cytokine levels in 20 autistic children by S Gupta and
coworkers found that TH1 cytokines were consistently lowered and
TH2 cytokines were consistently elevated as compared with controls.(91)
Once again, does this tie in with immunizations? Are immunizations
tilting the immune systems into TH2-skewed immune response? Considering
that vaccines are administered by parenteral injection, designed
primarily to stimulate antibody response, this would appear to be
the case.
However, we cannot know the answers to this and other similar questions
until definitive studies are done, testing both the immediate and
long-term effects of vaccines on the human system. Among these,
the testing of cytokines and related lymphocyte subpopulations before-and-after
immunizations appear to be the most promising.
Gulf War Syndrome, Chronic Fatigue Syndrome, and Fibromyalgia
In a study of 33 veterans suffering with symptoms of Gulf War Syndrome,
there were marked increases in markers indicating increased coagulability
of the blood of the subjects as compared with healthy controls.(92)
The authors hypothesized that exposures to chemical, biological,
warfare pathogens, and/or vaccine adjuvants (including the controversial
anthrax vaccine) during the Persian Gulf War had brought about immune
reactions which had activated the coagulation system by the cross
reaction of antibodies with antithrombotic (anticlotting) proteins
lining the endothelial surfaces of blood vessels, the end result
being a deposition of fibrin within blood vessels and a reduction
of blood flow. Similar hypercoagulability states have been found
in patients with the chronic fatigue syndrome.(93)
At this point no one knows to what extent each of the various exposures
(chemicals, biological warfare, and/or vaccines) played in the pathogenesis
in the Gulf War Illness, but serious investigators have little doubt
it was a combination of these exposures that caused the illness.
Considering that the GWS and CFS have much in common clinically
as well as in laboratory findings, should we not be investigating
the possibility that two conditions have similar causes?
Are Vaccines Bringing about Genetic Change?
In a Letter-to-the-Editor of Science Magazine in October 1967,
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."(94)
In a larger sense, the question about the possible effects of vaccines
in causing adverse genetic changes might be considered as the black
hole of scientific knowledge. Even if it is taking place, do we
have the technology to identify it?
For the present, however, genetic abnormalities have been found
only in persons with major vaccine-related 0health disorders, as
reviewed below:
To date, a careful review of the world's literature has disclosed
only two publications reporting on adverse genetic changes known
or suspected to be related to vaccines: In a study from Italy, 30
patients with post-vaccine diseases of the central nervous system
were tested for Herpes virus and tissue typing (HLA A,B,C, HLA DR-DQ).
The comparison of the patients with controls showed an increased
presence of HLA A3 and DR-7, reflecting genetic change in 73.3%
of patients.(95) In the second report, a three-year study was done
in collaboration with the University of Michigan School of Medicine
involving 24 gulf war veterans with a pattern of symptomatic health
disorders that have been referred to as the Persian Gulf War-Related
Illness.
Among these, 50% were found to have abnormal RNA, indicating chromosomal
damage after "toxic events."(96) Although the report from
the University of Michigan Medical School comments only on toxic
chemical exposures in the Gulf War, vaccines may also have played
a role, especially the controversial anthrax vaccine.(97) Perhaps
the greatest significance of these reports, aside from the findings,
is simply in the fact that scientific investigations have begun
in this very important area.
Thimerosal (Mercury) in Some US Licensed Vaccines:
According to recent revelations based on tables provided by the
U.S. Center for Disease Control,(98) among the six vaccines required
during 2, 4, and 6 months ages, which include DTaP, Hepatitis B,
Hib, and IPV, if one includes the 25 micrograms of mercury in most
DTaP vaccines, 12.5 micrograms in some Hepatitis B vaccines, and
25 micrograms in some Hib vaccines, theoretically it is possible
that some infants are receiving over 100 times the amount of mercury
that the US Environmental Protection Agency says is the maximum
allowable daily exposure.(99)
(Current EPA standards allow a maximum of 0.1 micrograms per kilogram
of body weight as the maximum safe dose of mercury per day.)
For centuries mercury has been known to be a potent neurotoxin
and one of the most toxic of the heavy metals. A possible mechanism
for this toxicity was recently disclosed in an animal study in which
mercury vapor exposures resulted in retrograde degeneration of neuronal
(brain) membranesm producing molecular lesions similar to those
seen in the brains of patients with Alzheimer's disease.(100)
Recently it has also been shown to be sensitizing,(78) so that
along with pertussis and the Hib vaccine,(35,74) we have 3 potentially
sensitizing agents in this group of vaccines.
Conclusions:
Having in mind the foregoing material and today's vaccine scene,
one is reminded of Hamlet's words when he said, "The times
are out of joint."
By federal, state, and school policies, parents are being compelled
to keep up-to-date on their children's vaccines whether they wish
it or not, and then when serious health problems ensue, as appears
to be increasingly the case, parents are told that the vaccines
had nothing to do with it.
In more than a few instances, parents are threatened with having
their children placed in a foster home if they refuse to complete
the recommended course of vaccines, and in some cases this has actually
been carried out.
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 pharmaceuticals, with no recourse open to parents, we have all
the potential ingredients for a tragedy of historical proportions.
Nothing written in this paper is intended to imply that immunizations,
when used in judicious moderation, do not at times serve a necessary
purpose. However, simple observation throws strong suspicion on
childhood vaccines, in their present numbers and forms, as posing
one of the major causes of the increasing pattern of sickness, allergies,
autism, and other neurobehavioral problems now being seen in our
youngsters.
For sake of argument, let us assume that scientific proof eventually
implicates the vaccines as one of the prime sources of these problems
and that, in addition, it becomes known that safer methods could
have been found to accomplish the same ends if they had been sought.
If we continue to enforce the vaccine programs as at present, one
shudders to think what future generations will think and write about
us. Mistakes might be forgiven, but not the enforcement of those
mistakes. If such does prove to be the case, we can rest assured
that they will be neither kind nor charitable in their judgments
of us.
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with 66 cents in stamps.
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Dr. Mercola's favorite vaccine websites:
Provided are a listing of Medical hyperlinks:
The best web site I know for vaccine related information is the
National Vaccine Information Center (NVIC)
http://www.909shot.com
Dr. Classen's excellent vaccine site
http://www.vaccines.net/
The best site for Anthrax Vaccine Information
http://www.anthraxvaccine.org
Vaccinations May Increase Death Toll
By Helen Pearson
Inadequate vaccines can encourage the emergence of nastier bugs,
placing the unprotected at risk, a new mathematical model shows.
The effect could undermine future vaccination programs.
Many vaccines save people from dying of a disease, but do not stop
them carrying and transmitting it. Over a few decades this may cause
more virulent strains to evolve, predict Andrew Read and his colleagues
of the University of Edinburgh, UK(1).
In some situations, such as in areas endemic for malaria, deadlier
disease strains could kill more people than vaccination saves. Most
of the time the benefits of vaccination will be eroded.
Vaccines for HIV, and hepatitis B and C "give most cause for
concern", says immunologist Charles Bangham, of Imperial College
in London. These viruses are difficult for the body's immune system
to eradicate, leaving them time to reproduce and evolve. Tearaway
strains of flu also emerge regularly and evade existing vaccines.
Infections that linger in the body are more likely to meet a second
bug, explains evolutionary biologist Dieter Ebert from the University
of Fribourg in Switzerland. The competition drives pathogens to
evolve faster, nastier killing tactics to get the most from their
host.
Don't Encourage Them
Vaccines that encourage evolution include those that slow a disease-causing
organism's growth or target its harmful toxin. These types are being
pursued to fight diseases such as anthrax and malaria. The possibility
that these might save individuals but harm populations "has
not been considered before", says Ebert, and should be a factor
in public-health policy.
Most existing vaccines, such as those for smallpox, polio and measles,
are very effective as they use a different strategy. They stimulate
a natural immune reaction which either kills off subsequent infections
or blocks pathogen reproduction and transmission altogether.
Read does not advocate halting such programs. New vaccines should
similarly aim to prevent pathogens getting a toehold, says Bangham;
many in the pipeline do not.
Several different vaccines are being developed to fight malaria:
results of clinical trials for one that interrupts the life cycle
of microorganism Plasmodium falciparum were announced last week(2).
'Multivalent vaccines' that target several different parts of a
pathogen or life cycle at once are the better choice, Read suggests.
Nature December 13, 2001
Dr. Mercola's Comment:
Many people will not realize that Nature is one
of the most prestigious scientific journals in the world. I point
that out to highlight the fact that the concern with vaccines is
actually starting to be voiced by some well respected scientists.
Additional Comment from Dawn Richardson of PROVE:
Being healthy becomes an even more elusive goal
if you primarily rely on vaccines to get there. When you read this
article, keep in mind that children now receive as many as 39 doses
of vaccines for 12 different viral and bacterial illnesses and there
are literally hundreds of new vaccines in development.
It is also interesting to keep in mind that the
bacteria strains chosen for inclusion in the pnuemococcal vaccine
for children were specifically chosen because they are the strains
that have evolved to be the most antibiotic resistant. It is very
difficult to do fair and comprehensive risk/benefit analysis when
there is so much about the unintended consequences of vaccines that
have yet to even be studied.
More is not better - educated parents everywhere
will continue to demand having options for their individual children
and the legal right to exercise those options.
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The Vaccination Debate Goes Mainstream
A Summary of the Proofs That Vaccination Does Not Prevent Smallpox
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