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by Harold E Buttram, MD
Introduction
In 1986 the U.S. Congress passed the National
Childhood Vaccine Injury Act, which set up a system whereby
the families of vaccine-injured children could be compensated
for such injuries. Based on personal experience and observation,
there has been much criticism of this system and question
whether not it is serving its intended purpose.
(1) One of the major areas of controversy
surrounding the act involves its limitations in the latent
periods, whereby certain defined reactions following vaccines
must be identified within a certain time period to qualify
for compensation by the childhood vaccine injury act. For
the complication of encephalitis, the time limitation for
the DTP or DTaP vaccine is 3 days; for the measles-mumps-rubella
(MMR) vaccine it is 5 to 15 days.
The limitations in latent periods following
vaccines have been generally accepted by our medical-legal
system as guidelines in other areas as well. Prominent among
these is the "shaken baby syndrome" (SBS) in which
a parent or caretaker is accused of injuring or murdering
an infant by violent shaking and causing a triad of findings
now commonly accepted as diagnostic of SBS: retinal hemorrhages,
subdural hematomas, and diffuse axonal injury. (2-5)
However, it has been observed that many
cases attributed to the SBS have occurred in a time-related
fashion following routine childhood vaccines, especially in
compromised children that had been born from medically complicated
pregnancies. (6) Consequently there are valid reasons for
questioning whether or not some or many cases that have been
accused of SBS were not the result of mistaken diagnoses,
the true causes of death or injury of the child having been
vaccines.
Since questions surrounding the latent
period play a prominent role in many of these cases, it is
timely and appropriate to review the background of this issue.
Are Current
Guidelines in the Latent Period Artifactual?
(A) The DTP
(diphtheria-tetanus-pertussis) Vaccine:
If we think in terms of a vaccine-induced
encephalitis, most of the earlier literature deals with the
pertussis vaccine. Flexner (1930) noted a strong tendency
for the nervous system manifestations to declare themselves
between the 10th and 13th days. (7)
In a review of 108 cases recorded before
1929 by Gorter (1933) , the onset of encephalitis was "strikingly
constant," usually observed between the 10th and 12th
days following vaccination, commonly with a febrile period
on the 7th and 8th days, followed by recovery until onset
of the encephalitis. (8)
In 1929 an editorial in the Journal of
the American Medical Association reported on an increase in
severe neurological complications following infections and
inoculations occurring on about the 11th day after vaccines.
(9) Over 50 years later Munoz, (1984) in a mice study of experimental
encephalomyelitis elicited by injection of pertussigen, found
the same latent period of 11 to 13 days. (10)
In contrast, some of the literature since
the 1970s has reported an entirely different pattern, with
the onset of encephalopathy largely falling within a 3-day
period following vaccines. (11-13) We can only speculate as
to the reasons for this changing pattern.
Perhaps it can be attributed to the fact
that, in those early years, children were given very limited
numbers of vaccines in comparison with more recent years during
which they have routinely received the hepatitis B, H influenza,
and polio vaccines in addition to the DTP, all given at the
same time.
The hepatitis B vaccine has been implicated
in neurological disorders, autoimmune disorders, various forms
of vasculitis and cutaneous reactions, as well as hemorrhagic
complications. (See below, page 6) Both the pertussis and
H influenza vaccines have been shown to have unusually high
hyper-sensitizing properties. (14) In many vaccines thimerosal,
which contains ethyl mercury, has been added as a preservative.
(In some vaccines its use dates back to the 1930s.)
Thimerosal has also been found to have
sensitizing properties. (15) Consequently there are valid
reasons for believing that the pertussis and H influenza vaccines,
some of which contain mercury, may be acting in a three-way
synergy in causing hypersensitivity reactions.
In the text, Vaccinations and Behavioral
Disorders, by Greg Wilson, the author made the following comment
in regards to the latent period:
"Today the latent period is rarely
mentioned in connection with neurological complications of
immunization ... Contemporary studies on the pertussis vaccine
select an arbitrary time limit in which reactions have to
occur to be considered as vaccine related. This time limit
is usually 3 to 7 days.
"Perhaps the only study which explores
the dynamics of post DPT reactions is an independent Australian
study by Karlsson and Scheibner which, with a monitor which
followed breathing volumes, found particular times of stress-induced
breathing following DPT injections." (16) "Of special
importance (for stress) are days 2,5,6, and 8,11,13-16 and
18-21. (17)
By way of explanation, the above study
involved the use of a Cotwatch breathing monitor controlled
by a micro-processor and designed to provoke alarms with breathing
delays (apnea of hypopnea with 5% or less of normal breathing
patterns) following DTP immunizations. It was found in the
study that these periods of stressed breathing occurred in
clusters of 15 minutes at a time on the post-vaccine days
listed above, varying greatly from child to child.
From our point of view, the important
feature of the study is not so much the specific post-vaccine
days on which the stressed breathing occurred but the fact
that the clusters continued for 21 days following the vaccines,
(18) which would tend to discredit the current medical-legal
limitation for DPT reactions to 3 days.
Dr. Scheibner's findings do have some
support in a study which showed a fairly high incidence of
cardio-respiratory complications in premature infants following
vaccinations. (19) Unfortunately, this study was of limited
duration.
Another study throwing light on the latent
period is one coming from Japan, from which it was found that
increased histamine sensitivity in mice, brought about by
the pertussis vaccine, showed two peaks, one on the 4th day
following vaccination, and a second on the 12th day. (20)
In the same vein, in a letter to the British Medical Journal,
Rosemary Fox, secretary of Parents of Vaccine Damaged Children,
made the following comments:
"Two years ago we started to collect
details from parents of serious reactions suffered by their
children to immunizations of all kinds. In 65% of the cases
referred to us, reactions followed the triple vaccine (diphtheria-pertussis-tetanus).
The children in this group total 182 to date; all are severely
brain damaged, some are also paralyzed, and 5 have died. Approximately
60% of reactions ... occurred within 24 hours of vaccination,
80% within 3 days, and all within 12 days." (21)
It is important to point out in the above-survey
that 20% of reactions occurred beyond the current 3 day medical-legal
limitation for the DPT vaccine.
Another important study throwing light
on the latent period involves an unpublished series of 25
cases with accusations or convictions of parents or caretakers
for the shaken baby syndrome, a series collected by attorney
Toni Blake of San Diego, California (personal communication,
2000) which have the following features: 1) All occurred in
fragile infants born from complicated pregnancies.
Problems included prematurity, low birth
weights, drug/alcohol problems, diabetic mothers, or other
maternal complications. 2) All infants were 6 months age or
less. 3) Onset of signs and symptoms occurred at about 2,4,
or 6 months of age, WITHIN 12 DAYS OF VACCINES, 4) All infants
had subdural hematomas. 5) Some had multiple fractures.
In addition to the work of Dr Viera Scheibner
and attorney Toni Blake, another enlightening area of study
for the latent period is the federal Vaccine Adverse Events
Reporting System (VAERS). In her book, What Your Doctor May
Not Tell You About Children's Vaccinations, (22) Dr. Stephanie
Cave makes the following observations about VAERS:
"It is common knowledge that less
than 10% of all adverse events following vaccinations are
reported to VAERS, which means that instead of the 12,000
to 14,000 reports of hospitalizations, injuries, and deaths
made every year, there may be as many as 120,000 to 140,000."
Even a cursory examination of the VAERS
database for DTP/DTaP vaccines will reveal that the latent
periods for many vaccine reactions extend into the 7 to 13
day periods, some extending beyond 14 days. (23)
No review of the latent period would be
complete without pointing 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 the vaccines 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 US on post-pertussis
vaccine encephalopathy." (25)
As a result of this physician-reluctance
to report vaccine reactions, large numbers of reactions may
be taking place beyond the currently established time limits
of the latent period, unrecognized as to their true nature.
(B) The Hemophilus influenza
(HiB) vaccine:
In one of the largest, if not the largest
randomized epidemiological trial ever conducted, the effect
of the Hemophilus vaccine on the development of insulin dependent
diabetes mellitus (IDDM) was studied in Finland. (26) All
children born in Finland between October 1st, 1985 and August
31st, 1987, approximately 116,000, were randomized to receive
4 doses of the HiB vaccine (PPR-D, Connaught) starting at
3 months of life or one dose starting at 24 months of life.
An intent to treat method was used to
calculate the incidence of IDDM in both treatment groups until
age 10. The incidence of IDDM was also calculated in a control
group of 128,500 children which did not receive the HiB vaccine.
(27) The results demonstrated a rise in IDDM which was specific
for the vaccinated cohort. (28)
However, the important point for our purposes
was that there was a consistent delay of 3.5 years between
vaccination and onset of IDDM. (It should be pointed out that
IDDM is considered an autoimmune disease.)
At a presentation this past spring in
Nashville, Tennessee sponsored by the American College for
the Advancement of Medicine, (29) Dr. John Classen reviewed
32 publications in the medical literature showing a similar
increases in diabetes mellitus in a number of countries with
the MMR and hepatitis B as well as the HiB vaccine, again
with latent periods up to three years or more, according to
graphs that were provided. (Copies of references will be provided
on request).
Rather than being specific to any one
vaccine, Dr. Classen offered his opinion that the general
immune stimulation from the vaccines was the cause of a rise
in autoimmunity. As an interesting sidelight, Dr. Classen
mentioned that personnel in the US navy are more heavily immunized
than their European counterparts, and that the US navy personnel
have five times more diabetes than their European counterparts.
(C) The MMR
(measles-mumps-rubella) vaccine:
Whereas DTP and Hib vaccine-related encephalopathy
may be the result of
interactions between endotoxin and mercury, (the latter in
the form of the additive, thimerosal), the primary mechanism
of viral vaccines in causing encephalopathy may be related
to the propensity of viruses (and viral vaccines) in bringing
about autoimmune reactions. (30)
In order to provide an overview of the
latent period, there are two basic classes of immune systems,
the humoral or antibody producing system, which tends to produce
immediate-type reactions, and cellular immunity, in which
reactions are delayed. Either class is capable of producing
autoimmunity. (31) Obviously, the usual 15 day limitation
for the MMR vaccine excludes a recognition of the delayed-type
autoimmune reactions and, by inference, even denies their
existence.
In an article by Cohen and Shoenfeld dealing
with questions of vaccine-induced autoimmunity, the authors
pointed out that it is a subject about which relatively little
is known, due to the paucity of clinical and laboratory studies.
(32) In point of fact a more recent review on this subject
cites a temporal relationship of 2 to 3 months between vaccines
and autoimmune reactions. (33)
Recently the subject of the latent periods
for the MMR vaccine came sharply into focus in an article
published in Adverse Drug Reaction & Toxicology Review,
(34) in which researchers Andrew Wakefield and Scott Montgomery,
who have been investigating a possible causal relationship
between the MMR vaccine and the autism-enterocolitis syndrome,
carefully reviewed deficiencies in the early pre-licensing
trials of the MMR vaccine.
In the article they pointed out that
follow up periods following the vaccine were a maximum of
28 days and in some studies even shorter periods. They stressed
that such short periods of observations 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.
The most interesting feature of the Wakefield/Montgomery
article was that it was reviewed by four leading British authorities,
all of whom had previously held positions in the regulation
and licensing of medicines in the United Kingdom. (35) Taken
as a whole, the reviewers were supportive of the article,
three highly so.
Peter Fletcher, formerly a senior professional
medical officer for the Department of Health wrote, "being
extremely generous, evidence of safety (of the MMR vaccine)
was very thin." Noting that single vaccines for measles,
mumps, and rubella already existed, he argued, "caution
should have ruled the day ... granting of a product license
was definitely premature."
Professor Duncan Vere, former member of
the Committee on the Safety of Medicines, agreed that the
periods for tests were too short. "In almost every case,"
he wrote, "observation periods were too short to include
the onset of delayed neurological or other adverse events."
(D) The Hepatitis
B vaccine:
Other than the references provided by
John Classen, M.D. on the findings of increased diabetes from
the hepatitis B vaccine with a latent period of 3 years, I
am not aware of additional information bearing on the latent
periods between hepatitis B vaccine and other forms of reactions,
which reflects the sheer lack of data on the subject.
However, many reactions to hepatitis B
vaccine may be taking place unrecognized, for two reasons:
Reason one, I have in my possession a list of 109 references
of published articles reporting on complications from the
hepatitis B vaccine including autoimmune disorders, neurological
disorders, vasculitis and cutaneous reactions. This list will
be provided on request.
For reason two, in 1994 a 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. (36)
For this reason, the published reports
of hepatitis B vaccine reactions may only be a small portion
of those actually taking place, with large numbers of delayed
reactions taking place unrecognized.
Conclusion
Based on published evidence that many
vaccine reactions take place beyond current medical-legal
time limits that have been established for vaccines, and on
overwhelming evidence that large numbers of delayed vaccine
reactions may be taking place unrecognized, there are grounds
for believing that these time limitations may be unrealistic
and artifactual.
References:
(1) Buttram HE, The National
Vaccine Childhood Injury Act - a Critique, Townsend Letter
for Doctors & Patients, October, 1998:66-68.
(2) David TJ, Shaken baby
(shaken impact) syndrome; non-accidental head injury in infancy,
Royal Soc Med, Nov., 1999; 99:556-561.
(3) Weston IT, The pathology
of child abuse, in: Heifer RE, Kempe CH, editors, The Battered
Child, University of Chicago Press, 1968:77-100.
(4) Caffey J, On the theory
and practice of shaking infants; its potential residual effects
of permanent brain damage and mental retardation, Am J Dis
Child, 1972; 124:161-169.
(5) Guthkelch AN, Infantile
subdural hematoma and its relationship to whiplash injury,
Brit Med J, 1971; 11:430-431.
(6) Buttram HE, Shaken baby
syndrome or vaccine-induced encephalitis?, Medical Sentinel,
Fall, 2001; 6(3):83-89.
(7) Flexner S, Postvaccinal
encephalitis and allied conditions, JAMA, 1930; 94(5):305-311.
(8) Gorter E, Postvaccinal
encephalitis, JAMA, 1933; 101(24):1871-1874.
(9) JAMA (editorial), Postinfectious
encephalitis, a problem of increasing importance, May, 1929;
92(18):1523-1524.
(10) Munoz JJ et al, Elicitation
of experimental encephalomyelitis in mice with the aid of
pertussigen, Cellular Immunology, 1984; 83(1):92-100.
(11) Menkes JH & Kinsbourne
M, Workshop on neurologic complications of pertussis and pertussis
vaccination, Neuropediatrics, 1990; 21:171-176.
(12) Menkes JH, Neurologic
complications of pertussis vaccination, Ann Neurology, 1990;
28:428.
(13) Cody CL et al, Nature
and rates of adverse reactions associated with DTP and DT
immunization in infants and children, Pediatrics, Nov., 1981;
68(5):650-660.
(14) Terpstra OK et al, Comparison
of vaccination of mice and rats with Hemophilus influenza
and Bordetella pertussis as models, Clin Exp Pharmacol Physiol,
March-April, 1979; 6(2):139-149.
(15) Patrizi A et al, Sensitization
to thimerosal in atopic children, Contact Dermatitis, Feb.,
1999; 40(2):94-97.
(16) Vaccination and Behavioral
Disorders, a Review of the Controversy, Greg Wilson, Tuntable
Creek Publishing, PO Box 1448, Lismore NSW 2480, Australia,
2000, pages 48-49.
(17) Karlsson L & Scheibner
V, Association between non-specific stress syndrome, DPT injections
and cot death, paper presented to the 2nd immunization conference,
Canberra, May 27-29, 1991.
(18) Vaccination: 100 Years
of Orthodox Research Shows that Vaccines Represent a Medical
Assault on the Immune System, Viera Scheibner, Ph.D., Australian
Print Group, Maryborough, Victoria, Australia, 1993, pages
230-235.
(19) Pourcyrous M et al, Interleukin-6,
C-reactive protein, and abnormal cardiorespiratory responses
to immunization in premature infants, Pediatrics, March, 1998;
101(3):461.
(20) Horiuchi S et al, Two
different histamine-sensitizing activities of pertussis vaccine
observed in mice on the 4th and 12th days of sensitization,
Japan J Med Sci Biol, 1993; 46:17-27.
(21) Fox R, letter, British
Med J, Feb. 21, 1976.
(22) What Your Doctor May
Not Tell You About Children's Vaccinations, Stephanie Cave,
M.D., F.A.A.F.P., Warner Books, An AOL Time Warner Company,
2001, page xvi.
(23) VAERS Databases: www.vaers.org,
www.fda.gov/cber, orwww.fedbuzz.com/vaccine/vacmain.htm
(24) Reisinger RC, A final mechanism of cardiac and respiratory
failure, SIDS, 1974, Proc of Camps Intern Symp on SID in Infancy;
also Congressional Record S. 1745, September 20, 1973.
(25) A Shot in the Dark, Harris
L Coulter & Barbara Loe Fisher, Avery Publishing Group,
Inc., Garden City Park, New York, 1991, Page 47.
(26) Classen JB, Classen DC,
Association between type I diabetes and Hib vaccine, causal
relation likely, British Med J, 1999; 319:1133.
(27) Tuomilehto J, Virtala
E, Karvonen M et al, Increase in incidence of
insulin-dependent diabetes mellitus among children in Finland,
Intern J Epidemiology, 1995; 24:984-992.
(28) Tuomilehto J, Karonen
M, Pitkaniemi J et al, Record high incidence of type 1 (insulin
dependent) diabetes mellitus in Finnish children, Diabetologia,
1999; 42:655-660.
(29) American College for
the Advancement of Medicine, 23121 Verdugo Dr., Ste. 204,
Laguna Hills, CA 92653, phone 949-583-7666, fax 949-455-0679.
(30) Singh V & V Yang,
Serological association of measles virus and human herpes
virus-6 with brain autoantibodies in autism, Clin Immunol
and Immunopath, 1998; 88(1):105-108.
(31) Immunobiology, Charles
A Janeway et al, fourth Edition, Current Biology Publications,
New York, 1999, page 495.
(32) Cohen DC & Shoenfeld
Y, Vaccine-induced autoimmunity, J Autoimmunity, 1996; 9:699-703.
(33) Shoenfeld Y & A Aron-Maor,
Vaccination and autoimmunity-'vaccinosis:' a dangerous laison?,
J Autoimmunity, Feb., 2000; 14(1):1-10.
(34) Wakefield AJ & S
Montgomery, Measles, mumps, rubella vaccine: through a glass
darkly, Adv Drug React Toxicol Rev, Jan., 2001; 19(3):1-19.
(35) Hurley DR, DW Vere, AP
Fletcher, Referee 1, 2, 3, & 4, Adverse Drug React Toxicol
Rev, 2001; 19(4): 1-2.
(36) Stratton 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 D.C., 1994,
pp 211-236.
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