Bio-Terrorism - Who and What is the
Threat?
In the early 1940’s it was nuclear fission, today it is
biological technology, an out of control Manhattan Project
hemorrhaging sinuously upon the world scene like a nuclear mushroom,
caught in the winds of scientific whimsy.
Urgent U.S. defense
preparations are underway to cope with this emerging technology, using
strategic war plans computer systems, or
artificial intelligence, to predict what the first fallout will be and
where it will occur.
The discovery of synthetic lab-created retroviruses
designed to attack the very nature of human immunity is in the hands
of every major country in the world. So is the antidote. While the
stalemate continues, people go about their ordinary lives, and
governments ponder who will use it first; will it be used for good or
evil? It can be used to seek out and detect
cancer causing viruses, or as a biological weapon.
The technology is complicated for dissemination to the
general public, civilians are not educated on the subject, thus fear
of the unknown and unseen creates silent terror in a population.
The
New York Times reported on April 24th that Bill Clinton, after reading
The Cobra Event, a fictional book based on
scientific fact about a biological attack on New York City,
immediately convened a panel of experts to brief him on preparations
for biological warfare. A subsequent report suggested stockpiling
vaccines, antibiotics and antidotes, and setting up mechanisms to make
large quantities in a hurry.
A secret drill simulating a germ warfare attack in which
a small pox hybrid virus was dropped along the Mexican-American border
showed the U.S. government is unprepared to deal with such a crisis.
Officials who participated in the drill soon found themselves
overwhelmed by a panicked population, short of antibiotics and
vaccines, hampered by antiquated quarantine laws, and unable to get
trained, immunized medical personnel to the scene, the Times reported.
The technology IS scary, to be sure, and that doesn’t
change the fact of its existence, however people can educate
themselves on the options. Patrick Henry once said, (on the brink of
the American revolution):
Excerpted
"We are apt to shut our eyes against a painful truth,
and listen to the song of that siren till she transforms us into
beasts... For my part, whatever anguish of spirit it may cost, I am
willing to know the whole truth; to know the worst, and to provide for
it."
Biology of a Recombinant Virus
Genetic engineering has brought forth cures for diseases
and synthetic spray vaccines, while it paradoxically spawned deadly
predator viruses that mutate at will and can jump species from a
spider host to a mosquito, lizard, mouse, cat, monkey or human. The
new hypermutant life form can even live
inside a bacteria host and multiply until it explodes out of the cell
and finds its way into the bloodstream.
Weapons-related genetic engineering, in military terms,
is the creation of genetically altered viruses and bacteria in order
to enhance their power as weapons. This can be done by altering an
organism’s DNA, or its genetic code, which is found in every cell and
in every virus particle in existence. In high schools in the United
States today, students are taught how to do genetic engineering. They
learn how to create new variants of (safe) bacteria which are
resistant to antibiotics. One genetic engineering kit for high-school
students costs forty-two dollars and is sold through the mail.
In 1990 and 1991, Russian scientists found a way to
splice Venezuelan equine encephalitis (a brain virus) into the genome,
or DNA, of smallpox. The result was a "recombinant chimera virus"
called Veepox. In ancient Greek mythology, the chimera was a monster
made of parts of different animals.
Recombination means the mixing of genes from different organisms.
Under a microscope, the Veepok looks like smallpox, but it isn’t. It
is a new form of life.
Understanding the biology of a deadly Level-4 (90%
fatality) virus, how it was conceived, and by whom, is the first step
in combatting the effects of biological warfare. The books The Hot
Zone and The Cobra Event by Richard Preston, an MIT and American
Institute of Physics award winning science writer, provide clear
scientific data on Level-4 viral outbreaks in the U.S. and Africa, and
give valuable information on bio-hazard protection against these
microorganisms.
The book, Emerging Viruses, by Dr. Leonard Horowitz, a
Harvard graduate with a master of arts degree in health education and
a master of public health degree in behavioral science, suggests
that the Ebola virus has become a
biological weapon.
Spray Vaccines for Anthrax & Plague
The biotechnology revolution was launched when Dr.
Joshua Lederberg, a professor at Rockefeller University, won the Nobel
Prize in 1946 for discovering that bacteria can swap genes with each
other. By 1970 huge bio programs, administered by the Rockefeller
Foundation in cooperation with the CIA, provided experimental
vaccines to millions of recipients worldwide. Today, Dr. Lederberg
advises the government on biological weapons and the potential for
bio-terrorism.
Currently, Rockefeller University in cooperation with
SIGA Pharmaceuticals has developed a revolutionary nasal spray
antidote for military defense applications. The Defense Advanced
Research Projects Agency (DARPA) is funding the research under the
umbrella of the Department of Defense.
The nasal spray, called a "mucosal vaccine," is the
latest breakthrough in vaccine technology. It is a rapidly deployable
defense against biological warfare agents such as anthrax and plague,
and can be administered by a soldier,
civilian, or even a child. No needles or shots are necessary. This
genetically engineered commensal delivers an antigen (stimulates the
production of antibodies) from a variety of pathogens (cause of
disease), viral or bacterial, to surfaces in the mouth, nasal
passages, gastrointestinal and genital tracts.
By combining a
specific antigen with specific commensals (harmless bacteria that
naturally inhabit the body’s
mucosal surfaces), vaccines or other neutralizing agents are rapidly
produced.
It is not known, when, if ever, this spray vaccine will be
marketed to the general population, but someone stands to make
$billions, akin to a biological Bill Gates, if a bio-war outbreak
occurs in the United States.
Long Term Effects of Experimental Vaccines
Other commensal vectors may soon be used to vaccinate
children against influenza in 1999. Doctors tested the vaccine,
called FluMist, on 1,602 children ages 15 months to 6 years in 1996.
One percent of the children receiving the vaccine spray developed
influenza, compared to 18 percent in the untreated group. The
long-term "fall out" effects of these
experimental vaccines are still unknown.
The effects of older vaccines may only just now be
surfacing in baby-boomers today as their immune systems weaken and
dormant viruses emerge. According to The Health Century by Edward
Shorter, Ph.D., Americans are paying a heavy price, particularly those
inoculated with Sabin oral polio vaccines prior to 1964, as
recipients of 40 different simian (monkey) virus contaminants, called
SV40, produced by Merck Laboratories in the 1950’s.
During interviews for his book, Dr. Shorter audiotaped
Dr. Maurice Hilleman, director at Merck vaccine division. Hilleman
said he notified Albert Sabin of his concerns that the SV40 virus
might have long-term effects such as cancerous tumors. In 1961, the
SV40 contaminated polio vaccines
were pulled off the shelves at Merck after studies showed it might in
fact be carcinogenic to humans. No mention of the cancer connection
was made in the press until 1962. By then millions of children had
received both the Salk inactivated polio vaccine and Sabin’s live
virus vaccine, produced in contaminated
Rhesus monkey kidney cells.
Years later, in December 1986, when asked why the press
was silent on this issue, an elderly Albert Sabin replied, "...There’s too much scaring the public unnecessarily. Oh, your children
were injected with cancer virus and all that. That’s not very good."
In March 1996, new evidence was presented by Dr. W. John
Martin, professor of pathology at the University of Southern
California, at the Twentieth Century Plagues symposium in Los Angeles
and San Francisco, that SV40 gene sequences had been found in
childhood choroid plexus brain tumors.
Martin noted that chronic
fatigue syndrome, attention deficit hyperactivity
disorder, autism, and other behavior-linked illnesses "may be an
inadvertent consequence of stealth virus vaccine contaminants" derived
from simian viruses. Stealth viruses are unique cell-destroying
viruses that are not recognized by the human immune system. These
viruses cause persistent infections because
they are missing specific genes which ordinarily evoke an immune
response.
In his 1997 book, Emerging Viruses: AIDS and Ebola,
Nature, Accident or Intentional?, Dr. Leonard Horowitz notes, " ---
Anyone who received polio vaccines prior to 1964 is at risk of
carrying SV40 and spreading it to others at home or in the community.
The virus is apparently circulating now throughout the human race."
NOTE: ABC News on February 19, 1999 noted that the
current issue of the Journal of the National Cancer Institute reported
that simian SV-40 virus has been found in 10% of the baby-boomer
population who received live polio vaccine prior to 1963.
Origins of AIDS & Ebola
Dr. Horowitz’s book mainly explores evidence that AIDS
and Ebola viruses were byproducts of a genetic engineering program,
conducted by Merck and other government funded labs to develop and
test effects of bio-war viruses.
One source from which his theory was
derived was a five volume text entitled
Virology which noted that during the late 1960’s researchers advanced
a new theory of evolution - that through future research of viral
evolution (retroviruses) a "genetically superior race of humans could
be synthetically evolved."
AIDS For Profit
The irony of this scheme, according to Horowitz, was
that the lab (Merck Department of Virus Cell Biology) allegedly
responsible for the AIDS contaminated Hepatitus B vaccine injected
into 1,083 New York homosexuals, may also reap billions of dollars in
future revenues from developing and
marketing AIDS-related drugs for T-cell disorders.
Aids-like Viruses used for pre-cancer diagnosis?
Horowitz found buried in the basement of the Davis
Library at the University of North Carolina a book entitled Special
Virus-Cancer Program, published by the National Institute of Health in
Bethesda, Md. which detailed a $35 million collaborative program
structured for the purpose of proving that viruses are the causative
(etiological) agents of cancer - and certain AIDS-like retroviruses
can be used for pre-cancer diagnosis by seeking out and detecting
inactive human cancer viruses.
The text covered the period from 1970 to 1971, the
critical period during which Bionetics Research Labs, a Division of
Litton Industries, had created numerous AIDS-like retroviruses.
Observed Horowitz:
"Litton Bionetics had not only been involved in the
development of AIDS-like, Marburg-like, and Ebola-like viruses, but
had been innoculating simian monkeys with these mutant horrors as
early as 1962, and had shipped the infected monkeys to labs around the
world, including the ones in which the Marburg and Reston [Ebola]
outbreaks occurred."
(There had been an Ebola outbreak at a vaccine
factory in Marburg, Germany and another at a primate quarantine unit
in Reston, Virginia, owned by Hazelton Research).
A few of the collaborative labs involved in the Special
Virus-Cancer Program were listed as Hazelton Research Labs; Merck
Institute (pharmaceuticals); Bionetics Research Labs; and Anderson
Hospital & Tumor Institute.
The 1971 text of Special Virus-Cancer Program also noted
that,
"there are now over 100 viruses which are known to cause
virtually all kinds of cancer in every major group of animal including
non-human primates."
Through this research it was discovered that
AIDS-like viruses could be used for
pre-cancer diagnosis. A mouse Leukemia type-C virus which was adapted
to grow in human cells, if innoculated into a human, could seek out
and detect inactive human Sarcoma viruses. The down side to this
procedure was that humans then became the mixers for "mutant" Leukemia
and Sarcoma viruses, or retroviruses.
Horowitz suggested that the AIDS epidemic’s simultaneous
emergence in Central Africa and New York during the late 1970’s (and
later Ebola) was the result of a mass innoculation program originating
from experimental monkey-virus-contaminated vaccines supplied by the
Litton and Merck network of researchers.
World Health Organization: Vaccine Tests in Africa
The World Health Organization (WHO) is often at the
center of these controversies. WHO helps developing countries
establish national biological control laboratories and sets standards
for development, manufacture, distribution and administration of
essentially all pharmaceuticals used throughout the world.
In 1969 the U.S. Department of Defense requested $10
million from Congress to perform studies on immune-system-destroying
agents for germ warfare defense. According to WHO records, in 1970
studies were conducted on viruses that were capable of altering the
immunologic response capacity of T-Lymphocytes (immunity T-cells).
Prior to that, WHO had issued a 5-year research report on advances in
virology experimentation relating primarily to the causal relationship
between viruses and human cancer. The report stated that Russian and
American researchers had learned how the human immune system
can be "bolstered or destroyed by old and newly developed germs."
The WHO also applied administrative leadership and
funding for several programs designed to evaluate specific disease
vulnerabilities of minority groups - from American Indians to African
natives - through collection and analysis of
gene pools and blood supplies.
In 1970 the WHO and the Vaccine Development Committee
endorsed an African smallpox immunization program with a budget of $14
million for use in Zaire and neighboring countries. By today’s
standards, that would amount to about $70 million, a huge budget for
innoculations on a faraway undeveloped
continent. It is noteworthy that AIDS was non-existent in Africa
prior to 1975 - and Ebola was not recorded until 1976.
Both originate
from the same area in Zaire.
Moreover, noted Horowitz, Merck
Laboratories, the U.S. Army, USAID, the National Cancer Institute and
Litton Bionetics were all focused on,
"vaccines and studies in which
cancer-causing [retro] viruses were isolated
and transported from Africa to the U.S. and visa versa."
Quarantine Trials
A telling article by WHO consultants in March 1970
presciently warned of grave psychological consequences if a biological
attack occurred in the U.S.:
"The response to a chemical or biological
attack may require precautionary or other measures on such a scale
that extraordinary means of social
control will have to be introduced, and these may remain in force long
after the need for them has passed. Thus an attack may lead to social
changes out of all proportion to the actual damage done."
The 1993 book, The Hot Zone by Richard Preston
unwittingly corroborates the WHO consultants’ prediction of
"extraordinary means of social control."
During the 1976 Ebola outbreak in Kinshasa, the World
Health Organization and public officials sent the Army in to enforce
quarantines; roadblocks were set up, hospital staff were quarantined
inside the hospital, planes and boats were
not allowed in or out, communications were cut off, and anyone trying
to leave the city was shot.
"Virus hunter" Dr. Karl M. Johnson,
former head of Special Pathogens Branch of Center for Disease Control
(CDC) in Atlanta, Georgia, had been Chief of the WHO team in Kinshasa
during the outbreak.
At his home in Big
Sky, Montana, where he now does consulting work on "hot zones,"
Johnson rhetorically observed,
"A virus can be useful to a species by
thinning it out...."
Ebola Outbreak in Reston, Virginia
The notion that AIDS and Ebola are synthetic by-products
of genetic engineering, or "black biology," is not dissuaded in The
Hot Zone. During the 1989 Ebola outbreak at the primate quarantine
building in Reston, Virginia, four monkey caretakers became infected
with Ebola virus, yet none of those American workers became sick.
Author Preston inadvertently
revealed his inner suspicions, or offered a subliminal hint, when he
wrote:
" ...However, something eerie and perhaps sinister occurred.
All four men eventually tested positive for Ebola Reston virus. They
had all been infected with the agent. The virus had entered their
bloodstreams and multiplied in their cells. Ebola proliferated in
their bodies. It cycled in them. It carried on its life inside the
monkey workers. But it did NOT make them sick, even while it
multiplied inside them. If they had headaches or felt ill, none of
them could recall it. Eventually the virus cleared from their systems
naturally, disappeared from their blood, and as of this writing, none
of the men was affected by it."
Why would Preston consider the immunity of the four
Americans to Ebola virus "eerie" or "sinister"?
Perhaps because
thousands of black Africans contracted the hemorragic virus in Africa,
and died slowly while their organs liquified and blood poured from
every orifice of their body. Yet the American monkey handlers,
working for Hazelton Research, who received
treatment at Fairfax Hospital by Fort Detrick scientists, remained
healthy.
Wrote Preston:
"The workers at Reston had symptomless Ebola
virus. Why didn’t it kill them? To this day, no one knows the answer
to that question."
Ebola Not Found in Nature
Another corroborative chapter in The Hot Zone recounts a
Spring 1988 joint U.S. Kenya expedition comprised of Fort Detrick and
Kenyan scientists to the Rift Valley where the Kinshasa Highway, or
AIDS Highway as it is called in Africa, passes by Mount Elgin, the
origin of both the Ebola and AIDS virus outbreaks.
They found no
trace of the Ebola virus in any part of the natural environment.
"Exactly where the virus came from is one of the great mysteries..."
noted Preston.
Ebola: A Russian Bio-Weapon
Simultaneously, on yet another continent, in April 1988,
Dr. Nikolai Ustinov, a forty-four year old scientist at a
virology-research facility in Western Siberia pricked his finger with
a needle and contracted the Ebola virus.
He had been studying its
potential as a bio-weapon that could be loaded into special biological
warheads on the MIRV missiles that were aimed
at the United States. At the time, the Soviet missile warheads were
designed for strategic genetically engineered strains of smallpox
virus, anthrax, and Black death which was resistant to antibiotics.
The deputy chief at the Biopreparat facility, Dr.
Kanatjan Alibekov, known today in America as Ken Alibek, attempted to
obtain the special immune serum from the Ministry of Defense, but
bureaucratic delays prevented its arrival in Siberia until it was too
late. After moving to the United States in 1992, Alibek told
American officials the Ebola strain had been obtained by Soviet
intelligence, but he didn’t know where it came from, maybe Marburg,
Germany, he said.
The Soviets froze Ustinov’s blood and body parts and
kept the Ustinov Ebola strain alive and replicating in the Biopreparat
lab called Vector. They named the strain Variant U, after Ustinov, and
mass produced it in simple bio-reactors. They dried Variant U,
processed it into an inhalable dust, resembling pink talcum powder,
then tested the airborne weapon on animals in special explosion-test
chambers. Just one to five microscopic
particles of Variant U lodged in the lungs of a monkey was equal in
lethality to eight thousand spores of weapons-grade anthrax.
Variant U was on the verge of becoming a strategic
bio-weapon, ready to be loaded into MIRV warheads, when the Soviet
Union fell apart and Russian scientists left to work in other
countries. The Biopreparat facility had employed 25,000 people and
consisted of forty sprawling research and production facilities. It
worked both sides of the street: curing diseases
and inventing new ones. When government funding decreased
dramatically and scientists lost their jobs, Ken Alibek came to the
United States.
He said other biologists may have gone to China,
Israel, Iraq, Iran, Syria, and Libya, some carrying freeze-dried
Variant U Ebola with them. No one kept track of
them.
Hantavirus in Russia?
In a March 9, 1998 New Yorker magazine article entitled,
Annals of War - Bioweaponeers, by Richard Preston, Alibek discussed
accidental contamination of the soil outside a bio-factory at
Omutninsk.
Wild rodents living in the woods outside the factory had
become chronically infected with the Schu-4 military strain of
tularemia, a bacterium that causes a type of pneumonia, which was
being developed in the plant. It was a hot, lethal strain that came
from the United States: an American biological weapon that the Soviets
had managed to obtain.
The mutant bacteria had "jumped species," from
its natural host to rodents. People catch tularemia easily from
rodents, noted Preston.
Just recently, in April 1998, health officials have
begun monitoring mice populations near Colorado Springs in the United
States. The Associated Press reported a 17-year-old boy who lived on
a ranch west of Colorado Springs, died on April 18th of Hantavirus.
The press described Hantavirus as,
"a rare pneumonia-like disease
[which] is contracted by ingesting airborne dust particles of the
feces, urine or saliva of tiny deer mice."
Aged: Targets of Bio-War
The world’s most serious known bio-weapon outbreak
occurred in the Ural Mountains east of Moscow at Yekaterinburg.
In
April 1979, the military microbiology lab there known as Compound 19,
emitted a cloud of human inhalation anthrax spores that spread
downwind killing 68 people and contaminating livestock and food
sources. A subsequent study from Harvard
University, based on research at the scene, noted the absence of any
victims under the age of 24.
In February 1998, the Washington Post
reported that a news conference in Moscow revealed the 1979 leak did
not release anthrax, but some kind of "new biological weapon" that was
designed to target middle-aged men.
Bio-Terrorism Comes in Many Forms
Establishing the truth about U.S., Iraqi, or Russian
biological weapons programs is ambiguous because research on defensive
means, such as vaccines, and on offensive weapons involves identical
equipment.
If a scientist is developing a defensive vaccine, he must
test it against a virulent agent. And even small quantities of these
virulent organisms can be grown to significant quantities in a few
weeks and moved around the country in portable bio-reactors.
Bio-terrorism comes in many forms:
a hantavirus leak
into the general population from a secret bio-research facility
a
super-mutant antibiotic-resistant staphylococcus found in hospitals
contaminated experimental vaccines injected into Gulf War soldiers
genocide in Africa
pharmaceutical profiteers creating retroviruses,
then making millions on "miracle" cures and vaccines
a terrorist
suitcase left in a New York subway
military bio-quarantine
containments and social controls
last but not least, the threat
of biological warfare.
Remedies
Education is the only defense against new emerging
viruses.
Even the most sophisticated predator virus is still subject
to natural law. It degenerates and falls apart when exposed to
sunlight (ultra-violet rays). Simple household bleach can eradicate
any virus from a contaminated area. (Bleach was used by the Fort Detrick Army team to decontaminate the Reston
monkey house and the bio-suits afterwards).
Human skin is
virus-proof; the vulnerable areas of the body are eyelids, lips,
mucous membranes and open cuts, all of which can be covered or
protected with readily available bio-hazard equipment, most of which
is commonly used in hospitals.
Perhaps a quote published in Richard Preston’s March 9,
1998 New Yorker article entitled Annals of War - Bioweaponeers, by Dr.
Peter Jahrling, chief scientist at USAMRIID (Ft. Detrick), offers some
hope --- "I don’t think anyone could knock out New York City with a
genetically engineered bug, but someone might be able to knock out a
few people and thereby make an incredible panic."
Contact: Stormbird8@aol.com
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by Stormbird8@aol.com
Note: See related story: Bio-Hazard Protections