The Secret Origin of
AIDS & HIV
by ALAN CANTWELL JR., MD
(Los Alamos is the official home of nuclear
bomb-building, alleged Chinese spies, and the laboratory which directed secret
human radiation experiments on unsuspecting civilians from the 1940s up to the
beginning of the AIDS epidemic.)
At the international AIDS conference held in 2000 in South Africa, one scientist
claimed the chimpanzee virus (SIVcpz) was “ancient” and jumped species as
early as 1675 but didn’t establish itself in the human population until 1930.
This was dutifully reported by science writer Laurie Garrett, who give all the
time-honored reasons for the rapid spread of AIDS in Africa: non-sterile
needles, non-sterile blood products and widespread promiscuous sexual behavior.
The Special Virus Cancer Program (1962-1977)
Conveniently forgotten by scientists and medical journalists was the fact that
surgeons had been transplanting chimpanzee parts into human beings for decades.
When Keith Reemtsma died in June 2000, at age 74, he was hailed as a pioneer in
cross-species organ transplants (now known as xenotransplantation). By 1964 he
had already placed six chimpanzee kidneys into six patients. All his patients
died, but eventually Reemtsma succeeded in many successful human-to-human organ
transplants.
Much more likely to have spread animal viruses to human beings is the largely
forgotten Special Virus Cancer Program (SVCP). This research program was
responsible for the development, the seeding, and the deployment of various
animal viruses, which were capable of producing cancer and immune system damage
when transferred between animal species and into human cells and tissue.
The SVCP began in 1964 as a government-funded program of the National Cancer
Institute (NCI) in Bethesda, Maryland. Originally designed to study leukemia and
lymphoma forms of cancer, the program was soon enlarged to study all forms of
cancer.
The SVCP marshalled many of the nation’s finest virologists, biochemists,
immunologists, molecular biologists, and epidemiologists, at the most
prestigious institutions in a coordinated attempt to assess the role of viruses
in causing human cancer. Many of the top AIDS scientists, including Dr. Robert
Gallo (the co-discoverer of HIV), Myron (Max) Essex (of “cat AIDS” fame),
and Peter Duesberg (who claims HIV is not the cause of AIDS), were connected
with the Program.
The scope of the program was international and included scientists from Japan,
Sweden, Italy, the Netherlands, Israel, and even Uganda, Africa. A main mission
of the SVCP was to collect various human and animal cancers from around the
world and to grow large amounts of cancer-causing viruses. In the process, many
animal viruses were adapted to human cells. These cultured viruses would then be
shipped to researchers throughout the world.
An annual report of the accomplishments of the SVCP was published by the NCI.
The 1971 SVCR report indicates a mouse leukemia virus had been adapted to grow
in human cells. A hybrid virus a mixture of a mouse sarcoma and a cat (feline)
leukemia virus was engineered and grown in cat cells. Chicken and feline
retroviruses produced cancer in monkeys. Mouse-cat virus hybrids and feline
leukemia virus were adapted to human cells in tissue culture. Thus, species
jumping was a common occurrence in these experiments. Biological Warfare,
Primate Research and the SVCP. Also joining forces with the SVCP at the NCI were
the miltary’s biological warfare researchers.
On October 18, 1971, President Richard Nixon announced that the army’s
biowarfare laboratories at nearby Fort Detrick, Maryland, would be converted to
research on the cause, prevention, and treatment of cancer.
As part of Nixon’s so-called War on Cancer, the military biowarfare unit was
retitled the new Frederick Cancer Research Center.
Litton Bionetics was named as the military’s prime contractor for this
project.
The 1971 annual report noted that one of the primary tasks of the now jointly
connected National Cancer Institute-Frederick Cancer Research Center was “the
large scale production of oncogenic (cancer-causing) and suspected oncogenic
viruses to meet research needs on a continuing basis.” Special attention was
given to primate viruses (the alleged African source of HIV) and “the
successful propagation of significant amounts of human candidate viruses.”
Candidate viruses were animal or human viruses that might be capable of
intiating human cancers. And primate cancer-causing viruses were adapted to
‘normal’ human cells.
A steady supply of research animals (monkeys, chimpanzees, mice, and cats) was
necessary, which resulted in the establishment of breeding colonies for the SVCP.
Healthy animals were shipped in from various parts of the world for breeding
purposes and experimentation; and virus-infected animals were shipped out again
to various labs.
By 1971, a total of 2,274 primates had been inoculated at Bionetics Research
Laboratories, under contract to Fort Detrick. Over 1000 of these monkeys had
already died or had been transferred to other primate centers. (Some animals
were eventually released back into the wild). By this time, experimenters had
spread lymphoma-producing viruses into several species of monkeys, and had also
isolated a monkey virus (Herpesvirus saimiri) that would have a close genetic
relationship to a new Kaposi’s sarcoma virus that produced the “gay
cancer” of AIDS a few years later.
In order to prime primates and other research animals to acquire cancer, their
immune system was deliberately suppressed by drugs, radiation, or cancer-causing
chemicals or substances. The thymus gland and/or the spleen was removed, and
viruses were injected into newborn animals or into the womb of pregnant animals.
Some animals were also injected with malaria to keep them chronically sick and
immunodepressed.
Primates (especially newborn and baby chimpanzees) were the most favored lab
animals because they were most similar biochemically and immunologically to
human beings, and because there would be no official testing of these lab
viruses on humans. An irradiated rhesus monkey colony supplied animals for
transplantation experiments.
Robert Gallo was a project officer of a primate study contracted by Bionetics
that pumped cancerous human tissue, as well as a variety of chicken and monkeys
viruses into newborn macaques (a small species of monkey). This 1971 SVCP report
(NIH-71-2025) declared: “Inasmuch as tests for the biological activity of
candidate human viruses will not be tested in the human species, it is
imperative that another system be developed for these determinations and,
subsequently for the evaluation of vaccines or other measure of control. The
close phylogenetic relationship of the lower primates of man justifies
utilization of these animals for these purposes.”
Researchers at Bionetics evaluated the long-term cancer effects of injecting
human and animal cancer material into various species of monkeys. Newborn
monkeys, irradiated monkeys, and monkeys primed with cancer-causing chemicals,
were injected with blood (“using multiple sites and volumes as large as
possible”) taken from various forms of human leukemia. In other studies,
tissue cultures infected with various animal viruses were inoculated into
primates. Many kinds of human cancer tissue were injected into the animals. How
many “new” and “emerging” viruses were created and adapted by the SVCP
is not known. And it is unlikely that complete records of this animal cancer
virus experimentation will ever be examined.
Cats were also bred for leukemia and sarcoma cancer studies. An inbred germfree
colony of mice was established. Mouse cancer viruses were manipulated to produce
resistant and non-resistant strains. These adapted viruses would be employed in
the 1980s in human gene replacement experiments. Such experiments utilized a
weakened strain of the mouse leukemia virus to infect and “taxi-in” the
missing genes to genetically-defective human cells.
The End of the SVCP and the Birth of AIDS
By 1977 the SVCP came to a inglorious end. According to Gallo,
“Scientifically, the problem was that no one could supply clear evidence of
any kind of human tumor virus, not even a DNA virus, and most researchers
refused to concede that viruses played any role in human cancers.
Politically, the Virus Cancer Program was vulnerable because it attracted a
great deal of money and attention and had failed to produce dramatic, visible
results.”
Despite all this, the SCVP was the birthplace of genetic engineering, molecular
biology, and the human genome project. More than any other program it built up
the field of animal retrovirology, which led to the vital understanding of
cancer and immunosuppressive retroviruses in humans. Like manna from heaven,
AIDS in gays put the virologists back in business. And HIV, a cancer-causing and
immunosuppressive retrovirus, would make Robert Gallo the most famous scientist
in the world.
Few people understand clearly that AIDS is a new form of cancer, and this aspect
of AIDS has not been publicized for obvious reasons. Physicians have always told
their patients that cancer is not contagious or sexually transmitted.
Virologists wanted AIDS and “gay cancer” to be a new disease because HIV was
supposedly brand new. It was easier to blame gays for initiating this new
disease with their sexual lifestyle than it was to point the finger at
scientists. And if AIDS was connected to animal cancer research, some people
might wonder if the new disease had anything to do with all those species
jumping experiments in the 1970s. Making people understand that AIDS is cancer
would only confuse them.
And so, instead of looking for the source of HIV in the thousands of animal
cancer experiments performed througout the world, the virologists insisted on
looking for the source of the virus in primates in the African rainforest.
The Pre-AIDS Gay Hepatitis B Experiments (1978-1981)
As the SVCP was winding down, thousands of gay men were signing up as guinea
pigs for government-sponsored hepatitis B vaccine experiments in New York, Los
Angeles, and San Francisco. In a few years these cities would become the
epicenters for “gay-related immune deficiency syndrome, ” later known as
AIDS.
Could virus-contaminated vaccines lie at the root of AIDS?
In the early 1970s the hepatitis B vaccine was developed in chimpanzees, now
widely accepted as the animal from which HIV supposedly evolved. To this day,
some people are fearful about taking the hepatitis B vaccine because of its
original connection to gay men and AIDS; and older physicians remember the
original experimental hepatitis vaccine was made from the pooled blood serum of
hepatitis-infected homosexuals.
Was HIV "introduced" into gays during these vaccine trials when
thousands of homosexuals were injected in New York beginning in 1978, and in the
West Coast cities in 1980-1981?
AIDS first erupted in gays living in New York City in 1979 a few months after
the experiment began in Manhattan. The astounding and statistically significant
fact is that 20% of the gay men who volunteered for the hepatitis B experiment
in New York were discovered to be HIV-positive in 1980 (a year before AIDS
became “official” in 1981). This would mean that Manhattan men had the
highest incidence of HIV anywhere in the world, including Africa, the supposed
birthplace of HIV and AIDS. The fact is that definite, proven cases of AIDS in
Africa would not appear until 1982.
Some researchers are convinced that these vaccine experiments served as the
vehicle through which HIV was “introduced” into the gay population in
America. Nevertheless, AIDS scientists have downplayed any connection of AIDS
with the vaccine.
My own extensive research into the hepatitis B experiments is presented in AIDS
and the Doctors of Death: An Inquiry into the Origin of the AIDS Epidemic,
published in 1988. Also included in this book is evidence suggesting patient
Zero” story of 1987, which claimed a promiscuous gay Canadian airline steward
brought AIDS to America. Montagnier “is doubtful that the American epidemic
could have developed from a single patient.”
Montagnier admits that he stands apart from Robert Gallo on many matters. In a
mind-blowing statement he declares “Gallo was not a medical doctor, but rather
a biochemist by training. His limited experience with viruses at the time
perhaps explains his misinterpretations and the contaminations that occurred in
his laboratory.” ( Gallo has always declared himself as a physician. If he is
not, then we certainly do have a conspiracy problem on our hands.)
What is obvious from their authored books is that while the continent of Africa
dies, these two top scientists in AIDS research continue their vendetta in
print, and continue to promote their own pet theories on the origin of HIV and
AIDS to an adoring scientific community.
“Gay and Straight” Strains of HIV and Sexual Preference
It is common knowledge that AIDS is a heterosexual disease in Africa,and that
AIDS started exclusively as a gay disease in the United States.
Although the public was told early on that “no one is immune from AIDS”, the
fact remains that even now (20 years after the first AIDS cases) 80% of the new
AIDS cases in America are gay men, IV drug addicts, and their sexual partners.
Why is this? Certainly HIV does not discriminate between sexual preference and
race! Or does it?
In the mid-1990s molecular biologists identified at least 8 different subtypes
(or “clades” or “strains”) of HIV that were infecting various people
around the world. Remarkably, it turns out that the “B” strain is the
predominant strain infecting gays in the U.S. Even more remarkable is that this
strain of HIV has an “affinity” to infect rectal tissue, thus explaining why
gays are more likely to get AIDS than straights. In contrast, the HIV strains
common in Africa have an affinity for vaginal and cervical cells, as well as for
cells of the foreskin of the penis. Thus, HIV is more likely to infect
heterosexuals in Africa.
How do we know this? Max Essex (a Harvard veterinarian who performed pre-AIDS
experiments transferring feline leukemia virus between cat populations) tested
subtype E strains of HIV from Thailand. He discovered that this Asian strain
readily infected women’s genital cells of the vagina and cervix. But the
“gay” B strain of HIV did not infect them as easily.
AIDS experts tell us American AIDS came from Africa, but the strain of HIV
prevalent in gay men is almost never seen in Africa! How is this possible?
Were strains of HIV engineered to adapt easily to cells likely to be infected in
gay sex? Or adapted to genital cells involved in vaginal sex?
We know scientists in the SVCP were able to adapt certain retroviruses to infect
specific kinds of cells. As early as 1970 biowarfare scientists were learning to
design certain infectious agents (particularly viruses) that would attack the
cells of certain racial groups.
More recently, in 1997, Stephen O’Brien and Michael Dean of the Laboratory of
Genomic Diversity at the National Cancer Institute have shown that one out of
ten white people have AIDS-resistant genes, whereas blacks in Africa have none.
Is this simply another peculiarity of a virus that jumped species in the African
bush? Or is HIV a designer virus, specifically adapted in its subtypes to infect
certain racial groups and gay people?
When AIDS appeared in 1981, health officials assured the “general public”
that there was nothing to fear. “AIDS is a gay disease” was the phrase
repeated over and over again in a media blitz. As late as 1987, Robert Gallo
told Playboy reporter David Black, “I personally don’t know of a single case
(in America) of a man getting the (AIDS) virus from a woman through heterosexual
intercourse.”
In Africa, where AIDS affects men and women in equal numbers, Gallo’s
explanation to Black was: “It happens, but that may be due to differences in
sexual practices, more promiscuity or to a greater incidence of venereal
disease.” Gallo give Playboy his reassurance of the future of heterosexual
AIDS in America: “AIDS will never become an overwhelming danger to the general
public.”
Solving the Mystery of the Origin of AIDS
The pre-AIDS species jumping experiments of the Special Virus Cancer Program (SVCP)
have been largely expunged from the history of HIV and AIDS. The viral
contamination problems inherent in viral research have also been downplayed. As
a result, the origin of HIV and AIDS has been distorted and obscured.
A serious examination of the SVCP provides “missing links” to the possible
laboratory origin of HIV. The ability of SVCP scientists to produce “new”
diseases with cancer-causing animal viruses is a matter of record. The ability
of animal viruses to easily contaminate laboratory experiments and vaccine
manufacture is also well known. All these factors make the man-made theory of
AIDS rational and compelling.
Some areas of HIV/AIDS history that require further analysis are:
The connection between AIDS and cancer
The connection of HIV to known (pre-AIDS) animal cancer lab viruses
The connection of the SVCP to the outbreak of AIDS
The connection of vaccine programs to the outbreak of AIDS
The connection of biological warfare research to the outbreak of AIDS
The disinformation surrounding the origin of AIDS
The disinformation blaming the “victims” of AIDS for the disease
The total secrecy of biological warfare and its implications for science
The wedding of cancer and AIDS scientists to biological warfare scientists
The “sworn to secrecy” problem of the government/military scientists
The wedding of government to medical science for military b/w purposes
The long history of secret medical experiments on unsuspecting citizens
All these factors need to be explored more fully and impartially in order to
more fully elucidate the man-made, laboratory origin of HIV and AIDS.
To continue to ignore these issues is to ignore the fate of countless millions
who will die from AIDS and other “emerging viruses” in the future.
The Special Virus Cancer Program (and biowarfare experimentation worldwide) has
forever changed the course of history of medical science, resulting in the
current dangers of biological terrorism and the fear of newly emerging man-made
viruses and other infectious agents.
To study the theories of origin of HIV/AIDS and to ignore the SVCP with its
biowarfare implications is like studying the Holocaust and failing to mention
the Nazis. Some readers may find this analogy offensive, but in light of the
close connection of the SVCP with the outbreak of HIV and AIDS, it is suggested
that final judgement be reserved until all the pertinent facts are ascertained.
The SVCP and “the hand of man” lie at the root of HIV. The flowering of the
worldwide epidemic of AIDS is proof that the seeds were well planted.
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Related Websites:
http://www.bhc.edu/EastCampus/leeb/aids/index.html
http://aidsbiowar.com
Acknowledgement: I am grateful to Robert E Lee, Vincent Gammill, Billi Goldberg,
and Boyd “Ed” Graves, for their contributions of research material for this
study.
[Dr. Cantwell is a medical researcher and author of AIDS & The Doctors of
Death, and Queer Blood, both published by Aries Rising Press, PO Box 29532,Los
Angeles, CA 90029, USA. These books are available on the Internet at Amazon.com,
Barnes & Noble, or through mail order at Book Clearing House @
1-800-431-1579. ]