Thursday, 11 April 2013

A History of US/North Korean Relations



The use of biologcial warfare, in particular when targetting civilian non-combatants is a War Crime, a Crime Against Humainity,a violation of the Geneva Conventions and the Universal Declaration of Human Rights.

The "forced" confessions of these US captured airmen, supposedly the result of North Korean Communist "brainwashing" led directly to the creation of the 20 year clandestine MK-Ultra mind-control program in 1953, initially with the stated aim of conductive "defensive" research against Manchurian Red indoctrination methods

The Year-One budget approriation for MK-Ultra was $35million in 1953 and ran continuously until it's existance was revealed publically in 1975.

Upon return to the United States, all US airmen made prisoners of war recanted their extensive confessions following extensive debriefing.




In this next Al-Jazeera documentary we hear from Professor Mauri a Japanese scienctist who has been researching this for over 20 years, made 8 visits to North Korea to speak to the survivors and the relatives and has conclused that this ABSOLUTELY happened.




He also speaks (on camera) to the last surviving captured US Airman to have made "false" confessions.

In only mildly evasive language, he admits (on camera) that his confession was genuine, his treatment was fine, he was not tortured, there was no gulag and the "re-education", "indoctrination" and "brainwashing" he recieved in order to make such convincing "flase confessions for the cameras consisted of a single book left in the prisoners' common room.


Again, this incident was the ENTIRE rationale for the whole MK-Ultra iniitiative and massive covert program in US Mind Control - Dulles and the CIA were so freaked out by how complete the "control" over the captured US serviceman was, it scared the living bejesus out of them and motivated the entire McCarthyite Reds Under the Bed paranoia of Communusit subversion.








Nuremberg Principle VI states:


"The crimes hereinafter set out are punishable as crimes under international law:

(a) Crimes against peace:

(i) Planning, preparation, initiation or waging of a war of aggression or a war in violation of international treaties, agreements or assurances;

(ii) Participation in a common plan or conspiracy for the accomplishment of any of the acts mentioned under (i).

(b) War crimes:
Violations of the laws or customs of war which include, but are not limited to, murder, ill-treatment or deportation to slave labor or for any other purpose of civilian population of or in occupied territory; murder or ill-treatment of prisoners of war or persons on the Seas, killing of hostages, plunder of public or private property, wanton destruction of cities, towns, or villages, or devastation not justified by military necessity.

(c) Crimes against humanity:
Murder, extermination, enslavement, deportation and other inhumane acts done against any civilian population, or persecutions on political, racial, or religious grounds, when such acts are done or such persecutions are carried on in execution of or in connection with any crime against peace or any war crime."


Unit 731 was a covert biological and chemical warfare research and development unit of the Imperial Japanese Army that undertook lethal human experimentation during the Second Sino-Japanese War (1937–1945) and World War II. It was responsible for some of the most notorious war crimes carried out by Japanese personnel.

Some of the numerous atrocities committed by the commander Shiro Ishii and others under his command in Unit 731 include: vivisection of living people (including pregnant women who were impregnated by the doctors), prisoners had limbs amputated and reattached to other parts of their body, some prisoners had parts of their bodies frozen and thawed to study the resulting untreated gangrene. Humans were also used as living test cases for grenades and flame throwers. Prisoners were injected with strains of diseases, disguised as vaccinations, to study their effects. To study the effects of untreated venereal diseases, male and female prisoners were deliberately infected with syphilis and gonorrhea via rape, then studied. 

In other tests, subjects were deprived of food and water to determine the length of time until death; placed into high-pressure chambers until death; experimented upon to determine the relationship between temperature, burns, and human survival; placed into centrifuges and spun until death; injected with animal blood; exposed to lethal doses of x-rays; subjected to various chemical weapons inside gas chambers; injected with sea water to determine if it could be a substitute for saline; and burned or buried alive.

Japanese scientists performed tests on prisoners with plague, cholera, smallpox, botulism, and other diseases. This research led to the development of the defoliation bacilli bomb and the flea bomb used to spread the bubonic plague. Some of these bombs were designed with ceramic (porcelain) shells, an idea proposed by Ishii in 1938.

These bombs enabled Japanese soldiers to launch biological attacks, infecting agriculture, reservoirs, wells, and other areas with anthrax, plague-carrier fleas, typhoid, dysentery, cholera, and other deadly pathogens. During biological bomb experiments, scientists dressed in protective suits would examine the dying victims. Infected food supplies and clothing were dropped by airplane into areas of China not occupied by Japanese forces. In addition, poisoned food and candies were given out to unsuspecting victims and children, and the results examined.

In 2002, Changde, China, site of the flea spraying attack, held an "International Symposium on the Crimes of Bacteriological Warfare" which estimated that at least 580,000 people died as a result of the attack. The historian Sheldon Harris claims that 200,000 died. In addition to Chinese casualties, 1,700 Japanese in Chekiang were killed by their own biological weapons while attempting to unleash the biological agent, which evidences serious issues with distribution

According to Maj. Robert Peaty, of the Royal Army Ordnance Corps, who was the senior British officer at Mukden, a prisoner-of-war camp 350 miles from Pingfan, doctors from Unit 731 administered the regular injections of infectious diseases, disguised as harmless vaccinations, which eventually killed 186 Americans.



The Unit 731 complex covered six square kilometers and consisted of more than 150 buildings. The design of the facilities made them hard to destroy by bombing. The complex contained various factories. It had around 4,500 containers to be used to raise fleas, six cauldrons to produce various chemicals, and around 1,800 containers to produce biological agents. Approximately 30 kg of bubonic plague bacteria could be produced in several days.

The related Unit 8604 was operated by the Japanese Southern China Area Army and stationed at Guangzhou, known historically as Canton or Kwangchow. This installation conducted human experimentation in food and water deprivation as well as water-borne typhus. According to postwar testimony, this facility served as the main rat breeding farm for the medical units to provide them with bubonic plague vectors for experiments.

After Imperial Japan surrendered to the Allies in 1945, Douglas MacArthur became the Supreme Commander of the Allied Powers, rebuilding Japan during the Allied occupation. MacArthur secretly granted immunity to the physicians of Unit 731, including their leader, in exchange for providing America, but not the other wartime allies, with their research on biological warfare.

American occupation authorities monitored the activities of former unit members, including reading and censoring their mail. The U.S. believed that the research data was valuable. The U.S. did not want other nations, particularly the Soviet Union, to acquire data on biological weapons.

The Tokyo War Crimes Tribunal heard only one reference to Japanese experiments with "poisonous serums" on Chinese civilians. This took place in August 1946 and was instigated by David Sutton, assistant to the Chinese prosecutor. The Japanese defense counselor argued that the claim was vague and uncorroborated and it was dismissed by the tribunal president, Sir William Webb, for lack of evidence. The subject was not pursued further by Sutton, who was likely aware of Unit 731's activities. His reference to it at the trial is believed to have been accidental.

Although publicly silent on the issue at the Tokyo Trials, the Soviet Union pursued the case and prosecuted twelve top military leaders and scientists from Unit 731 and its affiliated biological-war prisons Unit 1644 in Nanjing, and Unit 100 in Changchun, in the Khabarovsk War Crime Trials. Included among those prosecuted for war crimes including germ warfare was General Otozō Yamada, the commander-in-chief of the million-man Kwantung Army occupying Manchuria.

The trial of those captured Japanese perpetrators was held in Khabarovsk in December 1949. A lengthy partial transcript of the trial proceedings was published in different languages the following year by a Moscow foreign languages press, including an English language edition.

The lead prosecuting attorney at the Khabarovsk trial was Lev Smirnov, who had been one of the top Soviet prosecutors at the Nuremberg Trials. The Japanese doctors and army commanders who had perpetrated the Unit 731 experiments received sentences from the Khabarovsk court ranging from two to 25 years in a Siberian labor camp. 

The Americans refused to acknowledge the trials, branding them communist propaganda.

Having been granted immunity by the American Occupation Authorities at the end of the war, Ishii never spent any time in jail for his crimes and died at the age of 67 of throat cancer.

Under the American occupation the members of Unit 731 and other experimental units were allowed to go free. One graduate of Unit 1644, Masami Kitaoka, continued to do experiments on unwilling Japanese subjects from 1947 to 1956 while working for the National Institute of Health Sciences. He infected prisoners with rickettsia and mental health patients with typhus.


“. . . As long ago as 1962, forty sci­en­tists were employed at the U.S. Army bio­log­i­cal war­fare lab­o­ra­to­ries on full-time genet­ics research. ‘Many oth­ers,’ it was said, ‘appre­ci­ate the impli­ca­tions of genet­ics for their own work.’ The impli­ca­tions were made more spe­cific that genetic engi­neer­ing could solve one of the major dis­ad­van­tages of bio­log­i­cal war­fare, that it is lim­ited to dis­eases which occur nat­u­rally some­where in the world.

‘Within the next 5 to 10 years, it would prob­a­bly be pos­si­ble to make a new infec­tive micro-organism which could dif­fer in cer­tain impor­tant respects from any known disease-causing organ­isms. Most impor­tant of these is that it might be refrac­tory to the immuno­log­i­cal and ther­a­peu­tic processes upon which we depend to main­tain our rel­a­tive free­dom from infec­tious dis­ease.’

The pos­si­bil­ity that such a ‘super germ’ may have been suc­cess­fully pro­duced in a lab­o­ra­tory some­where in the world in the years since that assess­ment was made is one which should not be too read­ily cast aside. . .”

(A Higher Form of Killing; Robert Har­ris and Jeremy Pax­man; Hill and Wang [SC]; ISBN 0–8090-5471-X; p. 241.)


Fort Detrick, Md., was created in the middle of World War II and became the center for America's biological warfare efforts. But that role shifted in 1969, the government says, to focus solely on defense against the threat of biological weapons.

Then called Detrick Air Field, the science and research facility housed four biological agent production plants.

Anthrax was considered the most important agent. Simulants were tested, and one bomb was readied for production in 1944. One million bombs were ordered, though the order was canceled when the war ended in 1945.

During the 1950s, the biological weapons program was among the most classified within the Pentagon. There was an emphasis on biological agents for use against enemy forces as well as plants and animals.

The Army says no biological weapons were used during the Korean War, though such allegations were made by the Chinese and the Koreans.

Growing Protests

One plan at Fort Detrick in the late 1950s was to use the yellow fever virus against an enemy by releasing infected mosquitoes by airplane or helicopter. Detrick's labs were capable of producing a half-million mosquitoes per month, with plans for up to 130 million per month.

The military also tested bombs in Utah with brucella suis, a bacterium that can lead to fever and influenzalike sickness. And scientists at Fort Detrick also worked on a number of possible pathogens that could destroy crops or trees.

By the 1960s, the U.S. biological warfare program had begun to decline, with funding gradually decreasing. There were growing protests in the United States over the use of defoliants in Vietnam and anger about a sheep-kill incident in Utah. That incident occurred in 1968, when 3,000 sheep were found dead in the Skull Valley area, adjacent to the Army's Dugway Proving Ground. Although the findings were not conclusive, it was believed that nerve agents had somehow drifted out of Dugway during a test of aerial spraying.

In 1969, the Army announced that 23 U.S. soldiers and one U.S. civilian had been exposed to a sarin nerve agent on the Japanese island of Okinawa, while cleaning sarin-filled bombs. The incident created international concerns and revealed that the Army had secretly positioned chemical munitions in Southeast Asia.

That same year, President Nixon took action against biological and chemical weapons. He reaffirmed a no-first-use policy for chemical weapons, renounced the use of biological weapons and limited research to defensive measures only.

Leading Researcher

The Army fort that had its beginnings during World War II is now a sprawling campus of brick government buildings outside Frederick, Md., located an hour's drive north of Washington, D.C.

Government scientist Bruce E. Ivins worked at the heart of Fort Detrick, inside the main building of the U.S. Army Medical Research Institute for Infectious Diseases. It was there that he was one of the leading researchers on anthrax vaccines. The building houses a number of highly secure labs where anthrax spores would be used.

Ivins, who died on July 29, helped investigate the deadly anthrax attacks in 2001. He apparently had been notified that he was to be prosecuted for the five deaths connected to the anthrax attacks.



Blaming Gays, Blacks, and Chimps for AIDS 
Are species-jumping animal virus experiments responsible for the HIV Holocaust? 

Paranoia magazine                                               
by Alan Cantwell, M.D.  
  


In the fall of 1986 the Soviets shocked the world by claiming that HIV was secretly developed at Fort Detrick, the U.S. Army's biological warfare unit. Although the claim was dismissed as "infectious propaganda", Russian scientists had worked hand in hand with biological warfare scientists in the transfer of viruses and virus-infected tissue into various non-human primates (monkeys, apes, chimps) during the 1970s before AIDS appeared. With improved international relationships, the Russian accusation vanished.

Although evidence supporting the man-made theory has never been mentioned in the major U.S. media, the theory continues to be ridiculed. For example, in the San Francisco Chronicle,( "Quest for the Origin of AIDS", January 14, 2001), William Carlsen writes: "In the early years of the AIDS epidemic, theories attempting to explain the origin of the disease ranged from the comic to the bizarre: a deadly germ escaped from a secret CIA laboratory; God sent the plague down to punish homosexuals and drug addicts; it came from outer space, riding on the tail of a comet."

AIDS certainly did not come from the hand of God or outer space. However, there is ample evidence to suspect the hand of man in the outbreak of AIDS that first began in the late 1970s in New York City.

Creating AIDS in animals before the epidemic

In 1974 veterinarians actually created an AIDS-like disease when newborn chimps were removed from their mothers and weaned exclusively on virus-infected milk from cows infected with "bovine C-type virus." Within a year the chimps died of leukemia and pneumocystis pneumonia (the "gay pneumonia" of AIDS). Both diseases had never been observed in chimps before this virus-transfer experiment.

Also downplayed is the laboratory creation of feline leukemia and "cat AIDS" by the transfer of HIV-like cat retroviruses in the mid-1970s. These experiments were conducted at Harvard by Myron (Max) Essex, later to become a famous AIDS researcher. All this man-made creation of AIDS in laboratory animals directly preceded the "mysterious" 1979 introduction of HIV into gay men, the most hated minority in America.

Nowadays, scientists hunt for "ancestor" viruses of HIV in chimps in the African wild and ignore all the immunosuppressive viruses that were created in virus laboratories shortly before AIDS. No consideration is given to any of these lab viruses as possible man-made ancestors of the many "strains" of HIV (and HIV-2) that jumped species to produce AIDS in humans.

The gay experiments that preceded AIDS (1978-1981)

Scientists also discount any connection between the official outbreak of AIDS in 1981 and the experimental hepatitis B vaccine program (1978-1981) at the New York Blood Center in Manhattan that used gays as guinea pigs shortly before the epidemic. Curiously, the exact origin of AIDS in the United States remains unstudied. Health authorities simply blame promiscuous gay men, but never adequately explain how a black heterosexual African disease could have transformed itself exclusively into a white young gay male disease in Manhattan.

Researchers claim HIV incubated in Africa for more that a half century until AIDS broke out there in 1982. However, in the U.S. there was no incubation period for gay men. As soon as homosexuals signed up as guinea pigs for government-sponsored hepatitis B vaccine experiments, they began to die with a strange virus of unknown origin. The hepatitis B experiments began in Manhattan in the fall of 1978; the first few cases of AIDS (all young gays from Manhattan) were reported to the CDC in 1979.

Scientists have also failed to explain how a brand new herpes virus was also introduced exclusively into gays, along with HIV, in the late 1970s. This herpes virus is now believed to be the cause of Kaposi's sarcoma, the so-called "gay cancer" of AIDS. Before AIDS, Kaposi's sarcoma was never seen in healthy young men. Identified a decade after HIV, in 1994, this KS virus is closely related to a primate cancer-causing herpes virus extensively studied and transferred in animal laboratories in the decade before AIDS.

Also downplayed to the public is a new microbe (Mycoplasma penetrans), also of unknown origin, that was introduced into homosexuals, along with HIV and the new herpes virus. Thus, not one but three new infectious agents were inexplicably transferred into the gay population at the start of the epidemic (HIV, the herpes KS virus, and M.penetrans).

In his book, Virus [2000], Luc Montagnier (the French virologist who co-discovered HIV) blames promiscuous American gay tourists for bringing this new mycoplasma to Africa, and for bringing back HIV. He provides no evidence for this homophobic theory. Nor does he mention the various mycoplasmas that were passed around in the 1970s in scientific labs, and the fact that these microbes were frequent contaminants in virus cultures and vaccines.

Why are all these simultaneous introductions of new infectious agents into gay men ignored by scientists? Surely a credible explanation would be important in determining the origin of HIV and AIDS.

Why are scientists so opposed to the man-made theory? And why do they believe so passionately in the chimp theory? One explanation might be that scientists don't want the public to know what happened to the tens of thousands of imported primates who were held captive in laboratories throughout the world in the decade before AIDS.

The forgotten Special Virus Cancer Program (1964-1977)

Rarely mentioned by AIDS scientists and media reporters is the fact that surgeons have been transplanting chimpanzee parts (and chimp viruses) into people 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 primate (chimp and monkey) viruses to human beings is the largely forgotten Special Virus Cancer Program (SVCP). This research program was responsible for the development, the production, the seeding, and the deployment of various animal cancer and immunosuppressive AIDS-like viruses and retroviruses. These laboratory created viruses were capable of inducing disease when transferred between animal species and also when transplanted 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, the program was soon enlarged to study all forms of cancer. The scope of the program was international and included scientists from Japan, Sweden, Italy, the Netherlands, Israel, and Africa. The 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. As a result, thousands of liters of dangerous man-made viruses were adapted to human cells and shipped around the world to various laboratories. The annual reports of the SVCP contain proof that species jumping of animal viruses was a common occurrence in labs a decade before AIDS.

The SVCP gathered together the nation's top virologists, biochemists, immunologists, molecular biologists, and epidemiologists, to determine the role of viruses and retroviruses in the production of human cancer. Many of the most prestigious medical institutions were involved in this program.

Connected with the SVCP were the most famous future American AIDS scientists, such as Robert Gallo (the co-discoverer of HIV), Max Essex of "cat AIDS" fame, and Peter Duesberg, who claims HIV does not cause AIDS. Gallo and Essex were also the first to promote the widely accepted African green monkey theory of AIDS. This theory was proven erroneous as far back as 1988, but was heavily circulated among AIDS educators and the media until the theory was superceded by the chimp theory in the late 1990s.

Biowarfare research, primate research and the SVCP

Also joining forces with the SVCP at the NCI were the military'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 cancer research. As part of Nixon's so-called War on Cancer, the military biowarfare unit was retitled the new Frederick Cancer Research Center, and Litton Bionetics was named as the military's prime contractor for this project.

According to the 1971 SVPC annual report, the primary task 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 cause human cancers.

For these experiments a steady supply of research animals (monkeys, chimpanzees, mice, and cats) was necessary; and multiple breeding colonies were established for the SVCP. Primates were shipped in from West Africa and Asia for experimentation; and virus-infected animals were shipped out to various labs worldwide.

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 the early 1970s, experimenters had transferred cancer-causing viruses into several species of monkeys, and had also isolated a monkey virus (Herpesvirus saimiri) that would have a close genetic relationship to the new Kaposi's sarcoma herpes virus that produced the "gay cancer" of AIDS in 1979.

In order to induce 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 were removed, and viruses were injected into newborn animals or into the womb of pregnant animals. Some animals were injected with malaria to keep them chronically sick and immunodepressed.

The U.S. is the world's leading consumer of primates, and 55,000 are used yearly in medical research. Primates (especially newborn and baby chimpanzees) are the most favored lab animals because they are similar biochemically and immunologically to human beings. Humans share 98.4% of their DNA with chimpanzees. Chimps were extensively used by SVCP because there would be no official testing of "candidate" lab viruses on humans.

In the decade before AIDS, 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 monkey viruses, into newborn macaques (a small species of monkey that carries a close relative of the KS virus).

Recorded in the 1971 SVCP report (NIH-71-2025), Gallo's project notes state:

"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 measures of control. The close phylogenetic relationship of the lower primates to man justifies utilization of these animals for these purposes."

Researchers at Bionetics injected human and animal cancer material into various species of monkeys to determine the cancer effect. Newborn and irradiated monkeys 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. How many "new" and "emerging" viruses were created and adapted to human tissue and to various primates is not known. Some primates were released back into the wild carrying lab viruses with them. The possible spread of these lab viruses to other animals in the wild has been ignored by scientists searching for the origin of HIV and its close relatives in African animals.

Cats were also bred for leukemia and sarcoma cancer studies. Germ free colonies of inbred mice were 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 beings.

The end of the SVCP and the birth of AIDS

By 1977 the SVCP came to an 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 SVCP 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. As the SVCP was winding down, thousands of gay men were signing up as guinea pigs in government-sponsored hepatitis B vaccine experiments in New York, Los Angeles, and San Francisco. These same cities would soon become the three primary epicenters for the new "gay-related immune deficiency syndrome," later known as AIDS.

Two years after the termination of the SCVP, the introduction of HIV into gay men (along with a herpes virus and a mycoplasma) miraculously revived retroviral research and made Gallo the most famous scientist in the world. Could virus-contaminated hepatitis vaccines lie at the root of AIDS? In the early 1970s the hepatitis B vaccine was developed in chimpanzees. To this day, some people are fearful about taking the hepatitis B vaccine because of its original connection to gay men and AIDS.

Was HIV (and the KS herpes virus and a new mycoplasma) introduced into gays during these vaccine trials when thousands of homosexuals were injected in Manhattan beginning in 1978, and in the West Coast cities in 1980-1981?

As mentioned, the first gay AIDS cases erupted in Manhattan a few months after the gay experiment began at the NY Blood Center. When a blood test for HIV became available in the mid-1980s, the Center's stored gay blood specimens were reexamined. Most astonishing is the statistically significant fact 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 the AIDS epidemic became "official" in 1981). This signifies that Manhattan gays in 1980 had the highest incidence of HIV anywhere in the world, including Africa, the supposed birthplace of HIV and AIDS. And epidemic cases in Africa did not appear until 1982.

Although denied by the AIDS establishment, a few researchers are convinced that these vaccine experiments served as the vehicle through which HIV was introduced into the gay population. 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 [1988], and in Queer Blood: The Secret AIDS Genocide Plot [1993].

These books also debunk the preposterous "Patient Zero" story of 1987, which claimed a promiscuous gay Canadian airline steward brought AIDS to America. The highly implausible story was sensationalized in the media and served to further obscure the origin of AIDS in America and blame gay promiscuity. Even Montagnier is doubtful that the U.S. epidemic could have developed from a single patient.

Never mentioned by proponents of the chimp theory is the fact that the New York Blood Center established a chimp virus laboratory in West Africa in 1974. One of the purposes of VILAB II, at the Liberian Institute for Biomedical Research in Robertsfield, Liberia, was to develop the hepatitis B vaccine in chimps. A few years later this vaccine was inoculated into gays at the Center.

Chimps were captured from various parts of West Africa and brought to VILAB. Alfred Prince, Head of virology at the NY Blood Center, has been the director of Vilab for the past 25 years. The lab prides itself by releasing "reha bilitated" chimps back into the wild.

Also closely allied with "pre-AIDS" development of a hepatitis B vaccine is the little publicized primate colony outside New York City called LEMSIP (the Laboratory for Experimental Medicine and Surgery). Until disbanded in 1997, LEMSIP supplied New York area scientists with primates and primate parts for transplantation and virus research.

Founded in 1965, LEMSIP was affiliated with the New York University Medical Center, where the first cases of AIDS-associated Kaposi's sarcoma were discovered in 1979. Researchers at NYU Medical Center were also heavily involved in the development of the experimental hepatitis B vaccine used in gays; and the Medical Center received government grants and contracts connected with biological warfare research beginning in 1969, according to Leonard Horowitz, author of Emerging Viruses: AIDS and Ebola [1996].

Scientific disinformation and the 1959 HIV-positive blood test from Africa

By predating HIV back to the 1930s, the chimp theory effectively discredits the man-made theory of AIDS, which dates the introduction of HIV to the late 1970s. Only time will tell whether the chimp theory will hold up to further scientific scrutiny.

Conspiracy theorists believe some wildly popular AIDS origin stories in the press reek of scientific disinformation. One example is the Patient Zero story. Another is the media blitz surrounding the English sailor who supposedly contracted AIDS in 1959. This now-disproven story made worldwide headlines in 1990 and obviously served to contradict the underground conspiracy theory (particularly among African-Americans) that AIDS was man-made.

The New York Times (July 24, 1990) declared:

"The case also refutes the widely publicized charges made by Soviet officials several years ago that AIDS arose from a virus that had escaped from a laboratory experiment that went awry or was a biological warfare agent. The human retrovirus group to which the AIDS virus belongs was unknown at the time. Nor did scientists then have the genetic engineering techniques needed to create a virus."

Several years later, the case was discovered to be not a case of AIDS because the sailor's tissue remains were accidentally (or deliberately) contaminated with HIV.

In 1998 the media alerted the public to further evidence that AIDS started in Africa. The proof consisted of an old 1959 stored frozen blood specimen discovered to be HIV-positive. Researchers claimed the tiny amount of serum contained fragments of HIV "closely related" to a virus found in 3 chimpanzees in the African wild and in the frozen remains of a chimp named Marilyn, discovered in a freezer at Fort Detrick.

The 1959 specimen was obtained from a Bantu man living in Kinshasa, the Congo. His name and health status were not recorded. Details of the history and testing of this specimen (later heralded as the "world's oldest HIV-positive blood sample") are recorded in The River: A Journey to the Source of HIV and AIDS [1999], by journalist Edward Hooper who theorizes that HIV was introduced into Africans via the polio vaccine programs in the late 1950s. Hooper claims the polio vaccine was prepared using chimp kidney cells contaminated with the ancestor virus of HIV.

When tested for HIV in the mid-1980s, the 1959 blood sample was the only specimen out of 700 stored frozen Congo bloods that tested positive for HIV. Originally collected by Arno Motulsky on a Rockefeller grant, the African sample was one of many sent to the University of Washington in Seattle and used for genetic testing and included in a report, "Population Genetic Studies," published in 1966. Around 1970, the remaining 672 frozen bloods were flown to Emory University in Atlanta for further genetic tests.

In 1985 the specimens again changed hands, this time for HIV testing by Andre Nahmias, a virologist and animal researcher associated with the Yerkes Primate Center at Emory. The Congo specimens were tested along with 500 other blood specimens taken from blacks living in sub-Saharan Africa between the years 1959 and 1982. Initially over 90% of specimens taken in 1959 tested positive for HIV by the ELISA test. However, these HIV-positive tests were later determined to be false-positive. After the examinations at Emory, the specimens were shipped to Harvard University in Cambridge, Massachusetts, for HIV testing in Max Essex' lab.

Three specimens initially tested HIV-positive, but finally only the 1959 specimen from the unidentified Bantu man was confirmed HIV- positive. Around the time of these examinations, Essex's lab was unknowingly contaminated with primate viruses.

In 1986, Essex discovered a new "human" AIDS virus that later proved to be a contaminating monkey virus. The source of the primate virus traced back to a captive monkey at a primate center in nearby Southborough, Massachusetts. This primate contamination at his lab resulted in the erroneous green monkey theory, heavily popularized by Gallo and the media.

Also unpublicized is the little known fact that Gallo's lab at the National Cancer Institute was plagued with contamination by primate viruses. In 1975 he reported a new human "HL-23" virus that eventually proved to be three contaminating ape primate viruses (gibbon-ape virus, simian sarcoma virus, and baboon endogenous virus). Gallo claims he has no idea how these viruses contaminated his research.

In 1996 Hooper convinced Nahmias to turn over the remaining 1959 specimen to David Ho of Rockefeller University in Manhattan for PCR testing. In 1996 Ho was named Time magazine's "Man of the Year", at a time when few people had ever heard of him. Ho is also the director of the Aaron Diamond AIDS Research Center, affiliated with Rockefeller University since 1996. The Diamond Center is also now connected with the New York Blood Center, home of the gay vaccine experiments that gave birth to AIDS.

Ho determined the tiny amount of the remaining specimen did not contain live virus, nor was the complete virion of the virus present. Instead, some fragments of the virus (about 15% of the total genome) were tested and presented to the scientific world as the oldest specimen of HIV in the world. Ho's PCR results cannot be confirmed by independent investigators because the 1959 specimen is now totally used up.

When published in the journal Nature on February 5, 1998 ("An African HIV-1 sequence from 1959 and implications for the origin of the epidemic"), Hooper's name appeared on the report, along with Ho, Bette Korber, Nahmias, and others, The report was heavily publicized as proof that HIV existed in the African population in 1959.

Although there are no HIV-positive tissue specimens from Africa from the 1960s and 1970s, and no proven cases of AIDS either, Hooper relies heavily on this 1959 test to support his theory that HIV entered the African population via the polio vaccines programs in the late 1950s.

In The River Hooper quickly dismisses the claims of physician Robert Strecker, the first whistle-blower of man-made AIDS, as well as the research in Horowitz's Emerging Viruses, and in my own books, AIDS & The Doctors of Death, and Queer Blood.

In condemning AIDS biowarfare research, Hooper declares, "Sadly, supporters of the Streckers have continued to peddle their ill-informed and outdated versions of the myth, blaming variously the Soviets, the CIA, the Germans, and the World Health Organization (WHO) well into the nineties." He dismisses the hepatitis B vaccine connection to AIDS by noting that only two of the 826 gay vaccinees had developed AIDS by 1983.

Hooper ignores the fact that by 1981 over 20% of the men in the trials were HIV-positive and that by 1982, over 30% of the men were HIV-positive. He dismisses the World Health Organization's African smallpox vaccine connection by saying, "there is no reason for either HIV or SIV [simian immunodeficiency virus] to be accidentally present in the vaccine." Hooper fails to consider the possibility that the vaccines could have been deliberately contaminated with HIV. Hooper has been a United Nations official, but no details of this are included in his book .

Despite his massive research, Hooper seems naïve about the continuing transfer of viruses between various primate species at primate centers. For example, in 1995 he interviewed Preston Marx at LEMSIP. At that time Marx was a representative of David Ho's organization, the Aaron Diamond Research Center.

Hooper writes:

"I was shocked by the cavalier way in which tissues and sera from one species had been introduced into other species, long after the risks of cross-species transfer had been highlighted by the SV40 [polio vaccine] debacle, and I was astonished that survivors from troops that had been stricken by mystery illnesses could have been casually sold to other centers, for use in experiments there. Furthermore, this apparent lack of monitoring and central control seemed to be echoed in other fields, like xenotransplantation (the transplanting of organ or cells from one species to another) - and here, of course, the implications were even more frightening."

By predating his polio vaccine theory back to the late 1950s, Hooper greatly simplified his theory of AIDS origin. He ignored all those animal viruses that were placed into human tissue in the 60s and 70s, and all those dangerous viral creations that were genetically altered for cancer research, vaccine research, and secret biological warfare.

The chimp in the freezer at Fort Detrick

On February 1, 1999 Lawrence K Altman, longtime physician-writer for The New York Times, dutifully reported "the riddle of the origin of the AIDS virus has apparently been solved." A team of researchers, headed by Beatrice Hahn at the University of Alabama, performed viral studies on three chimps in the African wild and had also studied the frozen remains of a chimp, discovered by accident in a freezer at Fort Detrick. The chimp had tested positive for HIV in 1985. On the basis of all this research, Hahn declared that a common subspecies of chimp (Pan troglodytes troglodytes) was the animal source of the virus "most closely " related to HIV.

In a media blitz U.S. government scientists presented a phylogenetic ancestral "family tree" of primate viruses (which few people could understand) to prove that HIV was genetically descended from a chimp virus in the African bush. Molecular analysis of virus genetic data, performed by Bette Korber and the supercomputer Nirvana at the Los Alamos National Labor atory in New Mexico, indicated that HIV had jumped species from a chimp to a human in Africa around the year 1930. (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.)

Beatrice Hahn theorized that the epidemic started when a hunter cut himself while butchering chimp meat and subsequently became infected. Scientists readily accepted Hahn's notion that the AIDS virus and its closest relatives jumped species from chimps to humans on multiple occasions, thereby explaining the origin of the three separate subtypes of HIV-1 (M, N, and O), as well as HIV-2.

Chimps in West Africa are hunted for food, as well as for medical experimentation. Young chimps are especially prized for scientific research and are usually caught by shooting their mothers. Many die from stress and inhumane conditions during capture and transport to laboratories and zoos in Western nations.

Due to all this killing, chimps are now an endangered species. During the past century the African chimp population has dropped from two million to less than 150,000. Despite the mass killing of chimps, they are still blamed for causing the worldwide epidemic of AIDS.

Beatrice Hahn is no stranger to primate theories, having worked in Gallo's lab when he was heavily promoting the green monkey theory in the mid-1980s and the "close relationship" of the monkey virus to HIV. Now Hahn's virus was claimed to be a closer relative than the contaminating monkey virus in Essex' lab that formed the basis of the false green monkey theory.

Media journalists paid no attention to these discrepancies. Hahn's new chimp findings, along with the old 1959 blood specimen, fully convinced the AIDS establishment, and an adoring media, that Africa was indeed the source of HIV and the AIDS epidemic.

The 2000 London Origin of AIDS Conference

When Hooper's book appeared in the fall of 1998, molecular scientists quickly used the new chimp virus data to completely discredit Hooper's polio vaccine theory. AIDS in Africa could not be caused by a virus jumping species in the 50s if it had already jumped species back in the 1930s. Researchers refused to believe scientists could have played any role in the origin of HIV and AIDS.

Hooper bypassed the biowarfare theory by predating HIV back to the 50s. Now scientists bypassed Hooper by dating HIV back several decades earlier. The fact that there was no African epidemic until the early 1980s did not seem pertinent. To make their view official, a small group of scientists proposed an "invitation only" meeting to settle the origin matter once and for all.

In October 2000 the Royal Society of London held a two-day conference on the origins of HIV. Obviously, the biowarfare theory of AIDS was not discussed. On the contrary, one professor emphatically declared "all human infectious diseases have an animal origin." Although there never was a disease like AIDS (until scientists started to flagrantly pass viruses around to repeatedly break the species barrier ), the same professor declared that "natural transfer of these infections is a common event in animal populations."

Using the viral fragments from the 1959 specimen and comparing them with the select viruses contained in the data bank at Los Alamos , Betty Korber refined her computer calculations to establish a likely date of 1940, "with confidence levels extending from 1871 to 1955." The Rega Institute in Antwerp estimated the transfer could have occurred between 1590 and 1760, with 1675 the most likely date.

Hooper spoke but his views were largely ignored by the molecular biologists. Preston Marx warned about more human diseases caused by viruses emerging from primates, None of the speakers mentioned what happened to the thousands of liters of animal viruses that were passed around the world by the Special Virus Cancer Program in the decade before AIDS.

Instead, the London conferees alerted the public to a new view of medical science, championed by the virologists. The "Last Word" at the conference was that "all human viral infections were initially zoonotic (animal) in origin. Animals will always provide a reservoir for viruses that could threaten human populations in the future." And the scientists predicted: "There is still a myriad of current unknown viruses in animal populations on land, sea, and air with the potential to cause human disease." Apparently, none of these viruses were in animal laboratories.

AIDS, cancer, genetic science and covert human medical experimentation

Although rejected completely by most scientists, the man-made theory of AIDS is a rational explanation for the origin of HIV. This theory is partly based on an awareness of the gene-polluting activities and species jumping virus experiments of irresponsible scientists during the two decades before the epidemic.

In addition, the record clearly shows that scientists and biowarfare scientists experiment secretly on unsuspecting people. Horrific aspects of the Cold War Human Radiation Experiments attest to the fact that covert medical experimentation is not an "X-Files" fantasy or a totally paranoid belief.

It is easy to understand why researchers might want to obscure the man-made origin for AIDS and blame primates. It is now apparent that most of the major researchers promoting the African primate origin of AIDS were connected with the largely secret Special Virus Cancer Program, or are scientists involved in the transfer of viruses in animal research, particularly primate research.

From the very beginning of the epidemic, researchers disclaimed any connection between AIDS and cancer, as well as any connection between HIV and animal retrovirus cancer research. In 1984, Gallo originally named HIV a cancer-causing "leukemia/lymphoma" virus. To obscure the cancer connection, the name was immediately changed to "lymphotropic" virus.

My own Kaposi's sarcoma research, first published in medical journals in 1981, showed "cancer-associated bacteria" as possible infectious agents in "classic" KS tumors. Before HIV was discovered in 1984, additional papers in 1982 and 1983 showed similar cancer bacteria in the enlarged lymph nodes and KS tumors of gay men with "gay cancer" and AIDS. Since the 1950s, cancer-associated bacteria have been linked to viruses, as well as to mycoplasmas. This aspect of cancer research has been suppressed for decades by the cancer establishment. A history of this research and its relevancy to AIDS is the subject of my books, AIDS: The Mystery and the Solution [1984] and The Cancer Microbe: The Hidden Killer in Cancer, AIDS and Other Immune Diseases [1990].

Gallo, in his 1991 book, falsely claims that no infectious agent had ever been found in KS. The refusal of AIDS scientists to recognize cancer microbe research, published in peer reviewed scientific journals, is a further indication that the AIDS establishment seeks to control all aspects of HIV research in such a way as to never connect the origin of AIDS with previous cancer research and covert biological warfare research. This cover-up conceals the possibility that AIDS, in reality, is a new man-made form of infectious and contagious cancer.

Could a small coterie of government scientists concoct a bogus (but scientifically plausible) primate theory of AIDS origin and bamboozle the public to believe it in order to cover-up the truth?

In the 1930s the highly respected German scientific community was entirely transformed by fascist beliefs proclaiming the genetic inferiority of the Jews and the genetic superiority of the German Master Race. This Nazi takeover of science and the media eventually led to the murder of millions in the Holocaust. Could the genetic science surrounding the origin of AIDS obscure a genocidal and world depopulation program of man-made origin? It is time for the man-made theory of HIV to be examined fairly.

Proponents of this theory should not be dismissed as paranoid conspiracy theorists; and AIDS educators should educate themselves about this hidden history of AIDS and its implications for the origin of HIV.

How many more species jumping viruses will we have to endure before we question the integrity and the agenda of scientists who still blissfully jump viruses between species in animal laboratories?

Lawrence K. Altman, the Times reporter who in 1999 wrote that the origin of the AIDS virus was solved, recently asked "Where did AIDS come from?" Now seemingly undecided, Altman answers, "We can only guess. Determining the answer would be important because discovering how AIDS came to be an epidemic might prevent a similar catastrophe in the future." ("The AIDS questions that linger," January 30, 2001).

It doesn't take a rocket scientist to figure out how researchers could have created HIV and how they could have transferred the virus to gay and blacks in a covert medical experimentation for genocidal or population control purposes.

The secrecy and scientific disinformation surrounding the Human Radiation Experiments of the Cold War era has taught us how easily government scientists can fool the public on scientific matters. And when it comes to scientific monkey business, researchers know that most people are chumps.

Dr. Alan Cantwell is a retired dermatologist and AIDS and cancer researcher, who has written extensively on the man-made origin of AIDS. E-mail address: alanrcan@aol.com  Dr, Cantwell's books are available toll-free in the USA from Book Clearing House @ 1-800-431-1579, and on the internet at Amazon.com

REFERENCES:

Cantwell AR Jr: Bacteriologic investigation and histologic observations of variably acid-fact bacteria in three cases of Kaposi's sarcoma. Growth 45: 79-89, 1981. 
Cantwell AR Jr: Necroscopic findings of pleomorphic, variably acid-fast bacteria in a fatal case of Kaposi's sarcoma. Journal of Dermatologic Surgery and Oncology 7: 923-930, 1981. 
Cantwell AR Jr: Variably acid-fast bacteria in vivo in a case of reactive lymph node hyperplasia occurring in a young male homosexual. Growth 46: 331-336, 1982. 
Cantwell AR Jr: Kaposi's sarcoma and variably acid-fast bacteria in vivo in two homosexual men. Cutis 32: 58-74, 1983. 
Cantwell AR Jr: Necroscopic findings of variably acid-fast bacteria in a fatal case of acquired immunodeficiency syndrome and Kaposi's sarcoma. Growth 47: 129-134, 1983. 
Cantwell Jr, A: AIDS:The Mystery & the Solution. Los Angeles: Aries Rising Press, 1984. 
Cantwell Jr, A: AIDS & The Doctors of Death: An Inquiry into the Origin of the AIDS Epidemic. Los Angeles: Aries Rising Press, 1988. 
Cantwell Jr, A: The Cancer Microbe. Los Angeles: Aries Rising Press, 1990. 
Cantwell Jr, A: Queer Blood: The Secret AIDS Genocide Plot. Los Angeles: Aries Rising Press, 1993. 
Cantwell AR Jr: "Gay cancer, emerging viruses, and AIDS." New Dawn (Melbourne), Sept 1998. 
Faden RR (Chair): The Human Radiation Experiments: Final Report of the President's Advisory Committee. New York: Oxford University Press, 1996. 
Gallo R: Virus Hunting: AIDS, Cancer and the Human Retrovirus. New York: Basic Books, 1991. 
Hooper E: The River: A Journey to the Source of HIV and AIDS. Boston, MA: Little, Brown and Company, 1999 
Horowitz LG: Emerging Viruses: AIDS & Ebola. Rockport, MA: Tetrahedron Publishing Group, 1996. 
Lee RE: AIDS: An Explosion of the Biological Time-Bomb? Biographical Publishing Company, Prospect, CT, 2000. 
Montagnier L: Virus. New York: WW Norton Co, Inc, 2000. Special Virus Cancer Program (Progress Report #8). Bethesda, MD: National Institutes of Health, August 1971.

Johnathan J Pollard



Pollard is the direct forerunner of the 5 Dancing Israelis.

He's the only Israeli spy ever to be caught and convicted and is currently serving a life sentence.

In Israel, they have town squares named after him.

The US Ambassador to Israel was recently asked (there is a non-stop lobbying campaign) if the US had any intention of pardoning him or extending executive clemency to allow him to "return" (he's Jewish, but not an Israeli) to Israel, and the Ambassador correclty stated "We extended him leniancy by not having him executed".

Pollard took money and sold US National Secruity secrets to Israel, who GAVE them to the Soviet Union in a swap for Soviet Jews.

Netanyahu apparently nearly succeeded in persuading Bill Clinton to release Pollard in the late 90s, but he vetoed the idea when George Tenet and a number of senior Generals, including several of the Joint Chiefs stated they wiould resign if Pollard was ever released on their watch.

Wednesday, 10 April 2013

Perrin 9-1-1: "Eleven minutes late, seasonal manpower shortages,BostonLogan Airport"






As of March, 2013, there is no official, recognised list of casulties or confirmed fatalities due to the four acknowledged 9/11 terminal events.


Nor are there any confirmed officical passenger rolls or even headcount talllies derrived from any of the 9/11 flight manifests.

These are statutarily required-to-be-filed documents - chiefly to prevent exactly this kind of ambiguity from ever occurring.

There is no getting around this.

By law, every plane flight must hand off to the land-side airport authority staff at the gate, an envelope containing a full flight manifest with the names of every person aboard, passenger, crew member or dead-heading airline employee hitching a ride home.

Every single one. Before sealing the door and pushing back from the gate, without exception.

Aviation fuel explosions can happen anywhere and terrorist hijacking can occur just as easily and frequently during taxiing or on anywhere on the tarmac whether the plane is in motion or not, and knowing precisely who is aboard that plane when the aluminum people-tube hermetically seals itself could be a matter of life or death.

Not a single one of the four flight-manifest envelopes has ever been produced for Flights 11, 175, 77 or U-93, nor has any record ever been disclosed that they were ever filed by airline ground staff that day with the Tower before departutre.

This has led to some considerable confusion - upwards of a dozen variations on each passenger/"victim" list (and I use those quotes advisedly, as the next paragraph will make clear) have been produced, with serveral on seperate occasions being proclaimed definitive inspite of obvious defficiencies and inconsistencies.

They are, however, almost without exception, wholly and completely conistent in one reagard, at least: none of the "hijackers" appear anywhere on them, either under their 
own names (which we are told they used to make reservations) or identifiable alliases, Arabic or otherwise.

All four lists have been thoroughly Northwoods'ed up.




This document, titled “Justification for U.S. Military Intervention in Cuba” was provided by the Joint Chiefs of Staff to Secretary of Defense Robert McNamara on March 13, 1962, as the key component of Operation Northwoods.

Written in response to a request from the Chief of the Cuba Project, Col. Edward Lansdale, the Top Secret memorandum describes U.S. plans to covertly engineer various pretexts that would justify a U.S. invasion of Cuba.

These proposals - part of a secret anti-Castro program known as Operation Mongoose - included staging the assassinations of Cubans living in the United States, developing a fake “Communist Cuban terror campaign in the Miami area, in other Florida cities and even in Washington,” including “sink[ing] a boatload of Cuban refugees (real or simulated),” faking a Cuban airforce attack on a civilian jetliner, and concocting a “Remember the Maine” incident by blowing up a U.S. ship in Cuban waters and then blaming the incident on Cuban sabotage.

Author James Bamford writes that Operation Northwoods “may be the most corrupt plan ever created by the U.S. government.”

http://www.gwu.edu/~nsarchiv/news/20010430/
http://www.gwu.edu/~nsarchiv/news/20010430/northwoods.pdf









Most troubling is the fact that of just over 200 dead, the list includes over 40 named and identifiable millionaires; for example, not just people like Barabara Olsen but Frasier Producer David Angell and at least one Democratic fundraiser prominent enough in Boston politics to prompt both Bill Clinton and John Kerry to show up and speak at her memorial.


And a LOT of Corporate CEOs..... people with potentially RATHER a lot of reason to disappear.... much like the records in Building 7 or the Murraugh Building....


In Britain, we call that "Doing a Reggie Perrin"....








So, of the 200 or so passengers on the planes, over 40 of them were named and identifiable multimillionaires.

All of whom were either under indictment, investigation or had good reason to want to disappear.

The other names appear to have been totally made up.

Millionaires make up 1-2% of the general population, but 20% of the population of these flights.

A 767 has around 8 seats in Premiere / business class - that would mean at least 2-3 millionaires would have to have been downgraded to Coach, EVEN IF the hijacking teams of 5 each were not already sitting there (which we are told that they were).








"3. A "Remember the Maine" incident could be arranged in several forms:

b. We could blow up a drone (unmannded) vessel anywhere in the Cuban waters. We could arrange to cause such incident in the vicinity of Havana or Santiago as a spectacular result of Cuban attack from the air or sea, or both. The presense of Cuban planes or ships merely investigating the intent of the vessel could be fairly compelling evidence that the ship was taken under attack. The nearness to Havana or Santiago would add credibility especially to those people that might have heard the blast or have seen the fire. The US could follow with an air/sea rescue operation covered by US fighters to "evacuate" remaining members of the non-existant crew. Casualty lists in US newspapers would cause a helpful wave of national indignation. "


8. It is possible to create an incident which will demonstrate convincingly that a Cuban aircraft has attacked and shot down a chartered civil airliner enroute from the United States to Jamaica, Guatemala, Panama or Venezuela. The destination would be chosen only to cause the flight plan route to cross Cuba. The passengers could be a group of college students off on a holiday or any grouping of persons with a common interest to support chartering a non-scheduled flight.

a. An aircraft at Eglin AFB would be painted and numbered as an exact duplicate for a civil registered aircraft belonging to a CIA proprietary organization in the Miami area. At a designated time the duplicate would be subsituted for the actual civil aircraft and would be loaded with the selected passengers, all boarded under carefully prepared aliases. The actual registered aircraft would be converted to a drone.

b. Take off times of the drone aircraft and the actual aircraft will be scheduled to allow a rendezvous south of Florida. From the rendezvous point the passenger-carrying aircraft will descend to minimum altitude and go directly into an auxiliary field at Eglin AFB where arrangements will have been made to evacuate the passengers and return the aircraft to its original status. The drone aircraft meanwhile will continue to fly the filed flight plan. When over Cuba the drone will being transmitting on the inter- national distress frequency a "MAY DAY" message stating he is under attack by Cuban MIG aircraft. The transmission will be interrupted by the destruction of aircraft which will be triggered by radio signal. This will allow IACO radio stations in the Western Hemisphere to tell the US what has happened to the aircraft instead of the US trying to "sell" the incident. "

9. It is possible to create an incident which will make it appear that Communist Cuban MIGs have destroyed a USAF aircraft over international waters in an unprovoked attack.

a. Approximately 4 of 5 F-101 aircraft will be dispatched in trail from Homestead AFB, Florida, to the vicinity of Cuba. Their mission will be to reverse course and simulate fakir aircraft for an air defense exercise in southern Florida. These aircraft would conduct variations of these flights at frequent intervals. Crews would be briefed to remain at least 12 miles off the Cuban coast; however, they would be required to carry live ammunition in the event that hostile actions were taken by the Cuban MIGs.

b. On one such flight, a pre-briefed pilot would fly tail-end Charley at considerable interval between aircraft. While near the Cuban Island this pilot would broadcast that he had been jumped by MIGs and was going down. No other calls would be made. The pilot would then fly directly west at extremely low altitude and land at a secure base, an Eglin auxiliary. The aircraft would be met by the proper people, quickly stored and given a new tail number. The pilot who had performed the mission under an alias, would resume his proper identity and return to his normal place of business. The pilot and aircraft would then have disappeared.

c. At precisely the same time that the aircraft was presumably shot down a submarine or small surface craft would disburse F-101 parts, parachute, etc., at approximately 15 to 20 miles off the Cuban coast and depart. The pilots retuning to Homestead would have a true story as far as they knew. Search ships and aircraft could be dispatched and parts of aircraft found.


"Boarded under carefully prepared aliases".

There is NO formal/official victims list of the dead for 9/11.

Normal legal process for identification of the dead and finding of the termination of life was ever followed - the entire function of the coroner and State and County Medical Examiner was ignored and not done.

They just issued 3000-odd death certificates.

I can can believe it is possible to hijack and fly two jet airliners into tall buildings. Just.

I cannot believe that 10-20 high-net worth US Citizens would accept a down-grade on their flights to allow a group of poorly-dressed shabby-looking Ay-rabs to sit together at the front of the plane without insisting the American honour their First Class or Business class reservations, which they had clearly paid for, by placing them on an alternative flight.

That's impossible.

19 hijackers.

40+ millionaires (at least)

Divided between 4 planes.

It just doesn't work.


Peter O'Hanraha-hanrahan - Live report from 9/11



It's only funny because it's true.

The Battle of Trafalgar Square - The 1990 Poll Tax Riots



The Tea Party are f**king pussies,

This is what democracy looks like. This is how we won.

Yes Real Prime Minister AKA The Thatcher Sketch (1984)



This is actually not all that bad!

Well, at least we now know for sure she was a better actor than Reagan...

(I suspect Bernard Ingham may have had a hand in this...)

Tuesday, 9 April 2013

Jimmy and Maggie




Note what day his fun-run challenge climaxed (so to speak).

Irrespective of whether you believe in the reality of Satanic cults, Satanic Ritual Abuse and ritualised child murder, (and the evidence is overwhelming) the Satanic Cults believe in them.

And they honour and venerate Satanic holidays like Beltane and Hallowe'en.


With blood.


This is Not News (Apparently)



Sir Jim spent 11 consecutive New Years Eves at Chequers with Thatcher, by invitation.





























Friday, 5 April 2013

Deadly Immunity




" We are extemely concerned that A, B and C might lead to D, we can prove that The Government and Corporate America are lying to The People and not telling us the whole truth and we demand a complete investigation to get better Science and ensure that everything possible is done to ensure future vaccine safety."

Goldacre - Setting up and Knocking Down the MMR Vaccination Science Straw Man

"Study after study has found no evidence whatsoever between J and D, you people are hysterical peasant cattle who are endangering Public Health to exploit the irrationality of other cattle in order push your own hidden agenda of wiping Israel off the map and killing all The Jews, because you are a Nazi."


Published on Thursday, June 16, 2005 by Salon.com
Deadly Immunity
When a study revealed that mercury in childhood vaccines may have caused autism in thousands of kids, the government rushed to conceal the data -- and to prevent parents from suing drug companies for their role in the epidemic.

by Robert F. Kennedy Jr.

In June 2000, a group of top government scientists and health officials gathered for a meeting at the isolated Simpsonwood conference center in Norcross, Ga. Convened by the Centers for Disease Control and Prevention, the meeting was held at this Methodist retreat center, nestled in wooded farmland next to the Chattahoochee River, to ensure complete secrecy. The agency had issued no public announcement of the session -- only private invitations to 52 attendees. There were high-level officials from the CDC and the Food and Drug Administration, the top vaccine specialist from the World Health Organization in Geneva, and representatives of every major vaccine manufacturer, including GlaxoSmithKline, Merck, Wyeth and Aventis Pasteur. All of the scientific data under discussion, CDC officials repeatedly reminded the participants, was strictly "embargoed." There would be no making photocopies of documents, no taking papers with them when they left.

The federal officials and industry representatives had assembled to discuss a disturbing new study that raised alarming questions about the safety of a host of common childhood vaccines administered to infants and young children. According to a CDC epidemiologist named Tom Verstraeten, who had analyzed the agency's massive database containing the medical records of 100,000 children, a mercury-based preservative in the vaccines -- thimerosal -- appeared to be responsible for a dramatic increase in autism and a host of other neurological disorders among children. "I was actually stunned by what I saw," Verstraeten told those assembled at Simpsonwood, citing the staggering number of earlier studies that indicate a link between thimerosal and speech delays, attention-deficit disorder, hyperactivity and autism. Since 1991, when the CDC and the FDA had recommended that three additional vaccines laced with the preservative be given to extremely young infants -- in one case, within hours of birth -- the estimated number of cases of autism had increased fifteenfold, from one in every 2,500 children to one in 166 children.

Even for scientists and doctors accustomed to confronting issues of life and death, the findings were frightening. "You can play with this all you want," Dr. Bill Weil, a consultant for the American Academy of Pediatrics, told the group. The results "are statistically significant." Dr. Richard Johnston, an immunologist and pediatrician from the University of Colorado whose grandson had been born early on the morning of the meeting's first day, was even more alarmed. "My gut feeling?" he said. "Forgive this personal comment -- I do not want my grandson to get a thimerosal-containing vaccine until we know better what is going on."

But instead of taking immediate steps to alert the public and rid the vaccine supply of thimerosal, the officials and executives at Simpsonwood spent most of the next two days discussing how to cover up the damaging data. According to transcripts obtained under the Freedom of Information Act, many at the meeting were concerned about how the damaging revelations about thimerosal would affect the vaccine industry's bottom line.

"We are in a bad position from the standpoint of defending any lawsuits," said Dr. Robert Brent, a pediatrician at the Alfred I. duPont Hospital for Children in Delaware. "This will be a resource to our very busy plaintiff attorneys in this country." Dr. Bob Chen, head of vaccine safety for the CDC, expressed relief that "given the sensitivity of the information, we have been able to keep it out of the hands of, let's say, less responsible hands." Dr. John Clements, vaccines advisor at the World Health Organization, declared flatly that the study "should not have been done at all" and warned that the results "will be taken by others and will be used in ways beyond the control of this group. The research results have to be handled."

In fact, the government has proved to be far more adept at handling the damage than at protecting children's health. The CDC paid the Institute of Medicine to conduct a new study to whitewash the risks of thimerosal, ordering researchers to "rule out" the chemical's link to autism. It withheld Verstraeten's findings, even though they had been slated for immediate publication, and told other scientists that his original data had been "lost" and could not be replicated. And to thwart the Freedom of Information Act, it handed its giant database of vaccine records over to a private company, declaring it off-limits to researchers. By the time Verstraeten finally published his study in 2003, he had gone to work for GlaxoSmithKline and reworked his data to bury the link between thimerosal and autism.

Vaccine manufacturers had already begun to phase thimerosal out of injections given to American infants -- but they continued to sell off their mercury-based supplies of vaccines until last year. The CDC and FDA gave them a hand, buying up the tainted vaccines for export to developing countries and allowing drug companies to continue using the preservative in some American vaccines -- including several pediatric flu shots as well as tetanus boosters routinely given to 11-year-olds.

The drug companies are also getting help from powerful lawmakers in Washington. Senate Majority Leader Bill Frist, who has received $873,000 in contributions from the pharmaceutical industry, has been working to immunize vaccine makers from liability in 4,200 lawsuits that have been filed by the parents of injured children. On five separate occasions, Frist has tried to seal all of the government's vaccine-related documents -- including the Simpsonwood transcripts -- and shield Eli Lilly, the developer of thimerosal, from subpoenas. In 2002, the day after Frist quietly slipped a rider known as the "Eli Lilly Protection Act" into a homeland security bill, the company contributed $10,000 to his campaign and bought 5,000 copies of his book on bioterrorism. Congress repealed the measure in 2003 -- but earlier this year, Frist slipped another provision into an anti-terrorism bill that would deny compensation to children suffering from vaccine-related brain disorders. "The lawsuits are of such magnitude that they could put vaccine producers out of business and limit our capacity to deal with a biological attack by terrorists," says Andy Olsen, a legislative assistant to Frist.

Even many conservatives are shocked by the government's effort to cover up the dangers of thimerosal. Rep. Dan Burton, a Republican from Indiana, oversaw a three-year investigation of thimerosal after his grandson was diagnosed with autism. "Thimerosal used as a preservative in vaccines is directly related to the autism epidemic," his House Government Reform Committee concluded in its final report. "This epidemic in all probability may have been prevented or curtailed had the FDA not been asleep at the switch regarding a lack of safety data regarding injected thimerosal, a known neurotoxin." The FDA and other public-health agencies failed to act, the committee added, out of "institutional malfeasance for self protection" and "misplaced protectionism of the pharmaceutical industry."

The story of how government health agencies colluded with Big Pharma to hide the risks of thimerosal from the public is a chilling case study of institutional arrogance, power and greed. I was drawn into the controversy only reluctantly. As an attorney and environmentalist who has spent years working on issues of mercury toxicity, I frequently met mothers of autistic children who were absolutely convinced that their kids had been injured by vaccines. Privately, I was skeptical. I doubted that autism could be blamed on a single source, and I certainly understood the government's need to reassure parents that vaccinations are safe; the eradication of deadly childhood diseases depends on it. I tended to agree with skeptics like Rep. Henry Waxman, a Democrat from California, who criticized his colleagues on the House Government Reform Committee for leaping to conclusions about autism and vaccinations. "Why should we scare people about immunization," Waxman pointed out at one hearing, "until we know the facts?"

It was only after reading the Simpsonwood transcripts, studying the leading scientific research and talking with many of the nation's preeminent authorities on mercury that I became convinced that the link between thimerosal and the epidemic of childhood neurological disorders is real. Five of my own children are members of the Thimerosal Generation -- those born between 1989 and 2003 -- who received heavy doses of mercury from vaccines. "The elementary grades are overwhelmed with children who have symptoms of neurological or immune-system damage," Patti White, a school nurse, told the House Government Reform Committee in 1999. "Vaccines are supposed to be making us healthier; however, in 25 years of nursing I have never seen so many damaged, sick kids. Something very, very wrong is happening to our children." More than 500,000 kids currently suffer from autism, and pediatricians diagnose more than 40,000 new cases every year. The disease was unknown until 1943, when it was identified and diagnosed among 11 children born in the months after thimerosal was first added to baby vaccines in 1931.

Some skeptics dispute that the rise in autism is caused by thimerosal-tainted vaccinations. They argue that the increase is a result of better diagnosis -- a theory that seems questionable at best, given that most of the new cases of autism are clustered within a single generation of children. "If the epidemic is truly an artifact of poor diagnosis," scoffs Dr. Boyd Haley, one of the world's authorities on mercury toxicity, "then where are all the 20-year-old autistics?" Other researchers point out that Americans are exposed to a greater cumulative "load" of mercury than ever before, from contaminated fish to dental fillings, and suggest that thimerosal in vaccines may be only part of a much larger problem. It's a concern that certainly deserves far more attention than it has received -- but it overlooks the fact that the mercury concentrations in vaccines dwarf other sources of exposure to our children.

What is most striking is the lengths to which many of the leading detectives have gone to ignore -- and cover up -- the evidence against thimerosal. From the very beginning, the scientific case against the mercury additive has been overwhelming. The preservative, which is used to stem fungi and bacterial growth in vaccines, contains ethylmercury, a potent neurotoxin. Truckloads of studies have shown that mercury tends to accumulate in the brains of primates and other animals after they are injected with vaccines -- and that the developing brains of infants are particularly susceptible. In 1977, a Russian study found that adults exposed to much lower concentrations of ethylmercury than those given to American children still suffered brain damage years later. Russia banned thimerosal from children's vaccines 20 years ago, and Denmark, Austria, Japan, Great Britain and all the Scandinavian countries have since followed suit.

"You couldn't even construct a study that shows thimerosal is safe," says Haley, who heads the chemistry department at the University of Kentucky. "It's just too darn toxic. If you inject thimerosal into an animal, its brain will sicken. If you apply it to living tissue, the cells die. If you put it in a petri dish, the culture dies. Knowing these things, it would be shocking if one could inject it into an infant without causing damage."

Internal documents reveal that Eli Lilly, which first developed thimerosal, knew from the start that its product could cause damage -- and even death -- in both animals and humans. In 1930, the company tested thimerosal by administering it to 22 patients with terminal meningitis, all of whom died within weeks of being injected -- a fact Lilly didn't bother to report in its study declaring thimerosal safe. In 1935, researchers at another vaccine manufacturer, Pittman-Moore, warned Lilly that its claims about thimerosal's safety "did not check with ours." Half the dogs Pittman injected with thimerosal-based vaccines became sick, leading researchers there to declare the preservative "unsatisfactory as a serum intended for use on dogs."

In the decades that followed, the evidence against thimerosal continued to mount. During the Second World War, when the Department of Defense used the preservative in vaccines on soldiers, it required Lilly to label it "poison." In 1967, a study in Applied Microbiology found that thimerosal killed mice when added to injected vaccines. Four years later, Lilly's own studies discerned that thimerosal was "toxic to tissue cells" in concentrations as low as one part per million -- 100 times weaker than the concentration in a typical vaccine. Even so, the company continued to promote thimerosal as "nontoxic" and also incorporated it into topical disinfectants. In 1977, 10 babies at a Toronto hospital died when an antiseptic preserved with thimerosal was dabbed onto their umbilical cords.

In 1982, the FDA proposed a ban on over-the-counter products that contained thimerosal, and in 1991 the agency considered banning it from animal vaccines. But tragically, that same year, the CDC recommended that infants be injected with a series of mercury-laced vaccines. Newborns would be vaccinated for hepatitis B within 24 hours of birth, and 2-month-old infants would be immunized for haemophilus influenzae B and diphtheria-tetanus-pertussis.

The drug industry knew the additional vaccines posed a danger. The same year that the CDC approved the new vaccines, Dr. Maurice Hilleman, one of the fathers of Merck's vaccine programs, warned the company that 6-month-olds who were administered the shots would suffer dangerous exposure to mercury. He recommended that thimerosal be discontinued, "especially when used on infants and children," noting that the industry knew of nontoxic alternatives. "The best way to go," he added, "is to switch to dispensing the actual vaccines without adding preservatives."

For Merck and other drug companies, however, the obstacle was money. Thimerosal enables the pharmaceutical industry to package vaccines in vials that contain multiple doses, which require additional protection because they are more easily contaminated by multiple needle entries. The larger vials cost half as much to produce as smaller, single-dose vials, making it cheaper for international agencies to distribute them to impoverished regions at risk of epidemics. Faced with this "cost consideration," Merck ignored Hilleman's warnings, and government officials continued to push more and more thimerosal-based vaccines for children. Before 1989, American preschoolers received only three vaccinations -- for polio, diphtheria-tetanus-pertussis and measles-mumps-rubella. A decade later, thanks to federal recommendations, children were receiving a total of 22 immunizations by the time they reached first grade.

As the number of vaccines increased, the rate of autism among children exploded. During the 1990s, 40 million children were injected with thimerosal-based vaccines, receiving unprecedented levels of mercury during a period critical for brain development. Despite the well-documented dangers of thimerosal, it appears that no one bothered to add up the cumulative dose of mercury that children would receive from the mandated vaccines. "What took the FDA so long to do the calculations?" Peter Patriarca, director of viral products for the agency, asked in an e-mail to the CDC in 1999. "Why didn't CDC and the advisory bodies do these calculations when they rapidly expanded the childhood immunization schedule?"

But by that time, the damage was done. Infants who received all their vaccines, plus boosters, by the age of 6 months were being injected with levels of ethylmercury 187 times greater than the EPA's limit for daily exposure to methylmercury, a related neurotoxin. Although the vaccine industry insists that ethylmercury poses little danger because it breaks down rapidly and is removed by the body, several studies -- including one published in April by the National Institutes of Health -- suggest that ethylmercury is actually more toxic to developing brains and stays in the brain longer than methylmercury.

Officials responsible for childhood immunizations insist that the additional vaccines were necessary to protect infants from disease and that thimerosal is still essential in developing nations, which, they often claim, cannot afford the single-dose vials that don't require a preservative. Dr. Paul Offit, one of CDC's top vaccine advisors, told me, "I think if we really have an influenza pandemic -- and certainly we will in the next 20 years, because we always do -- there's no way on God's earth that we immunize 280 million people with single-dose vials. There has to be multidose vials."

But while public-health officials may have been well-intentioned, many of those on the CDC advisory committee who backed the additional vaccines had close ties to the industry. Dr. Sam Katz, the committee's chair, was a paid consultant for most of the major vaccine makers and shares a patent on a measles vaccine with Merck, which also manufactures the hepatitis B vaccine. Dr. Neal Halsey, another committee member, worked as a researcher for the vaccine companies and received honoraria from Abbott Labs for his research on the hepatitis B vaccine.

Indeed, in the tight circle of scientists who work on vaccines, such conflicts of interest are common. Rep. Burton says that the CDC "routinely allows scientists with blatant conflicts of interest to serve on intellectual advisory committees that make recommendations on new vaccines," even though they have "interests in the products and companies for which they are supposed to be providing unbiased oversight." The House Government Reform Committee discovered that four of the eight CDC advisors who approved guidelines for a rotavirus vaccine laced with thimerosal "had financial ties to the pharmaceutical companies that were developing different versions of the vaccine."

Offit, who shares a patent on the vaccine, acknowledged to me that he "would make money" if his vote to approve it eventually leads to a marketable product. But he dismissed my suggestion that a scientist's direct financial stake in CDC approval might bias his judgment. "It provides no conflict for me," he insists. "I have simply been informed by the process, not corrupted by it. When I sat around that table, my sole intent was trying to make recommendations that best benefited the children in this country. It's offensive to say that physicians and public-health people are in the pocket of industry and thus are making decisions that they know are unsafe for children. It's just not the way it works."

Other vaccine scientists and regulators gave me similar assurances. Like Offit, they view themselves as enlightened guardians of children's health, proud of their "partnerships" with pharmaceutical companies, immune to the seductions of personal profit, besieged by irrational activists whose anti-vaccine campaigns are endangering children's health. They are often resentful of questioning. "Science," says Offit, "is best left to scientists."

Still, some government officials were alarmed by the apparent conflicts of interest. In his e-mail to CDC administrators in 1999, Paul Patriarca of the FDA blasted federal regulators for failing to adequately scrutinize the danger posed by the added baby vaccines. "I'm not sure there will be an easy way out of the potential perception that the FDA, CDC and immunization-policy bodies may have been asleep at the switch re: thimerosal until now," Patriarca wrote. The close ties between regulatory officials and the pharmaceutical industry, he added, "will also raise questions about various advisory bodies regarding aggressive recommendations for use" of thimerosal in child vaccines.

If federal regulators and government scientists failed to grasp the potential risks of thimerosal over the years, no one could claim ignorance after the secret meeting at Simpsonwood. But rather than conduct more studies to test the link to autism and other forms of brain damage, the CDC placed politics over science. The agency turned its database on childhood vaccines -- which had been developed largely at taxpayer expense -- over to a private agency, America's Health Insurance Plans, ensuring that it could not be used for additional research. It also instructed the Institute of Medicine, an advisory organization that is part of the National Academy of Sciences, to produce a study debunking the link between thimerosal and brain disorders. The CDC "wants us to declare, well, that these things are pretty safe," Dr. Marie McCormick, who chaired the IOM's Immunization Safety Review Committee, told her fellow researchers when they first met in January 2001. "We are not ever going to come down that [autism] is a true side effect" of thimerosal exposure. According to transcripts of the meeting, the committee's chief staffer, Kathleen Stratton, predicted that the IOM would conclude that the evidence was "inadequate to accept or reject a causal relation" between thimerosal and autism. That, she added, was the result "Walt wants" -- a reference to Dr. Walter Orenstein, director of the National Immunization Program for the CDC.

For those who had devoted their lives to promoting vaccination, the revelations about thimerosal threatened to undermine everything they had worked for. "We've got a dragon by the tail here," said Dr. Michael Kaback, another committee member. "The more negative that [our] presentation is, the less likely people are to use vaccination, immunization -- and we know what the results of that will be. We are kind of caught in a trap. How we work our way out of the trap, I think is the charge."

Even in public, federal officials made it clear that their primary goal in studying thimerosal was to dispel doubts about vaccines. "Four current studies are taking place to rule out the proposed link between autism and thimerosal," Dr. Gordon Douglas, then-director of strategic planning for vaccine research at the National Institutes of Health, assured a Princeton University gathering in May 2001. "In order to undo the harmful effects of research claiming to link the [measles] vaccine to an elevated risk of autism, we need to conduct and publicize additional studies to assure parents of safety." Douglas formerly served as president of vaccinations for Merck, where he ignored warnings about thimerosal's risks.

In May of last year, the Institute of Medicine issued its final report. Its conclusion: There is no proven link between autism and thimerosal in vaccines. Rather than reviewing the large body of literature describing the toxicity of thimerosal, the report relied on four disastrously flawed epidemiological studies examining European countries, where children received much smaller doses of thimerosal than American kids. It also cited a new version of the Verstraeten study, published in the journal Pediatrics, that had been reworked to reduce the link between thimerosal and autism. The new study included children too young to have been diagnosed with autism and overlooked others who showed signs of the disease. The IOM declared the case closed and -- in a startling position for a scientific body -- recommended that no further research be conducted.

The report may have satisfied the CDC, but it convinced no one. Rep. David Weldon, a Republican physician from Florida who serves on the House Government Reform Committee, attacked the Institute of Medicine, saying it relied on a handful of studies that were "fatally flawed" by "poor design" and failed to represent "all the available scientific and medical research." CDC officials are not interested in an honest search for the truth, Weldon told me, because "an association between vaccines and autism would force them to admit that their policies irreparably damaged thousands of children. Who would want to make that conclusion about themselves?"

Under pressure from Congress, parents and a few of its own panel members, the Institute of Medicine reluctantly convened a second panel to review the findings of the first. In February, the new panel, composed of different scientists, criticized the earlier panel for its lack of transparency and urged the CDC to make its vaccine database available to the public.

So far, though, only two scientists have managed to gain access. Dr. Mark Geier, president of the Genetics Center of America, and his son, David, spent a year battling to obtain the medical records from the CDC. Since August 2002, when members of Congress pressured the agency to turn over the data, the Geiers have completed six studies that demonstrate a powerful correlation between thimerosal and neurological damage in children. One study, which compares the cumulative dose of mercury received by children born between 1981 and 1985 with those born between 1990 and 1996, found a "very significant relationship" between autism and vaccines. Another study of educational performance found that kids who received higher doses of thimerosal in vaccines were nearly three times as likely to be diagnosed with autism and more than three times as likely to suffer from speech disorders and mental retardation. Another soon-to-be-published study shows that autism rates are in decline following the recent elimination of thimerosal from most vaccines.

As the federal government worked to prevent scientists from studying vaccines, others have stepped in to study the link to autism. In April, reporter Dan Olmsted of UPI undertook one of the more interesting studies himself. Searching for children who had not been exposed to mercury in vaccines -- the kind of population that scientists typically use as a "control" in experiments -- Olmsted scoured the Amish of Lancaster County, Penn., who refuse to immunize their infants. Given the national rate of autism, Olmsted calculated that there should be 130 autistics among the Amish. He found only four. One had been exposed to high levels of mercury from a power plant. The other three -- including one child adopted from outside the Amish community -- had received their vaccines.

At the state level, many officials have also conducted in-depth reviews of thimerosal. While the Institute of Medicine was busy whitewashing the risks, the Iowa Legislature was carefully combing through all of the available scientific and biological data. "After three years of review, I became convinced there was sufficient credible research to show a link between mercury and the increased incidences in autism," says state Sen. Ken Veenstra, a Republican who oversaw the investigation. "The fact that Iowa's 700 percent increase in autism began in the 1990s, right after more and more vaccines were added to the children's vaccine schedules, is solid evidence alone." Last year, Iowa became the first state to ban mercury in vaccines, followed by California. Similar bans are now under consideration in 32 other states.

But instead of following suit, the FDA continues to allow manufacturers to include thimerosal in scores of over-the-counter medications as well as steroids and injected collagen. Even more alarming, the government continues to ship vaccines preserved with thimerosal to developing countries -- some of which are now experiencing a sudden explosion in autism rates. In China, where the disease was virtually unknown prior to the introduction of thimerosal by U.S. drug manufacturers in 1999, news reports indicate that there are now more than 1.8 million autistics. Although reliable numbers are hard to come by, autistic disorders also appear to be soaring in India, Argentina, Nicaragua and other developing countries that are now using thimerosal-laced vaccines. The World Health Organization continues to insist thimerosal is safe, but it promises to keep the possibility that it is linked to neurological disorders "under review."

I devoted time to study this issue because I believe that this is a moral crisis that must be addressed. If, as the evidence suggests, our public-health authorities knowingly allowed the pharmaceutical industry to poison an entire generation of American children, their actions arguably constitute one of the biggest scandals in the annals of American medicine. "The CDC is guilty of incompetence and gross negligence," says Mark Blaxill, vice president of Safe Minds, a nonprofit organization concerned about the role of mercury in medicines. "The damage caused by vaccine exposure is massive. It's bigger than asbestos, bigger than tobacco, bigger than anything you've ever seen." It's hard to calculate the damage to our country -- and to the international efforts to eradicate epidemic diseases -- if Third World nations come to believe that America's most heralded foreign-aid initiative is poisoning their children. It's not difficult to predict how this scenario will be interpreted by America's enemies abroad. The scientists and researchers -- many of them sincere, even idealistic -- who are participating in efforts to hide the science on thimerosal claim that they are trying to advance the lofty goal of protecting children in developing nations from disease pandemics. They are badly misguided. Their failure to come clean on thimerosal will come back horribly to haunt our country and the world's poorest populations.


Robert F. Kennedy Jr. is senior attorney for the Natural Resources Defense Council, chief prosecuting attorney for Riverkeeper and president of Waterkeeper Alliance. He is the co-author of "The Riverkeepers."

© 2005 Salon.com


Thursday, 4 April 2013

Paul made this Freedom of Information request to Transport for London

From: Paul

2 April 2013

Dear Transport for London,

It was stated for the public record at the July 7th Inquest that on
July 7th, 2005, Tfl control declared a system-wide "Code Amber"
across the London Underground, signalling a complete evacuation of
the network at 9.13 am.

Please could you confirm the running times and provide please the
service logs relating to all Southbound Northern Line services
confirmed as departing Kings Cross St Panceas after 8.30am which
were confirmed as arriving at Bank Station, prior to the Code Amber
condition going into effect?

Could you please also confirm the exact time at which Southbound
Northern line services calling at Bank were in fact suspended and
the evacuation procedure went into effect both at Bank Station
specifically and on the Southbound Northern line City branch
generally.

It is stated that Code Amber triggers the evacuation proceedure for
the Underground network -please could you confirm how Code Amber
typically impacts provision of service on the DLR, if at all, from
a policy point of view? How would a decision to extend the
suspension to the DLR be made and who would typically be
responsible for making it?

Are you also confirm, if possible, if the relevant officer or
post-holder did indeed make that executive decision, and at what
time?

A Tfl Travel Update issued at 12:35 pm states:

"12:35 Docklands Light Railway services are currently suspended.
This is precautionary measure"

Please could you provide a detailed breakdown and timeline of when
in fact this suspension went into effect and the circumstances
informing the executive decision to suspend DLR services across the
board , with reference to the key decision makers.

Please could you also supply copies of the service log, confirming
scheduled and actual arrival times for all Eastbound DLR services
normally scheduled to depart from Bank between 8.45 am and
confirmed as having arrived at Canary Wharf prior to the decision
to suspend the DLR.

If such are available, please could you also supply copies of any
incident reports relating to specific services or rolling stock,
station premesise, track or other TFL or DLR property, premesise
or assets on this stretch of line (Bank to Canary Wharf) within the
given timeframe (8.30 am to the time of network-wide suspension)
that potentially could have contributed to the decision to suspend
DLR services.

Additionally, a later Tfl Service Update published at 16:45 stated
:

"DLR
Full services have resumed following a Police sweep of the network.
But Bank, Stratford and Canning Town - where the DLR interchanges
with the Tube - will be closed."
Please could you confirm the nature, character and cause that
prompted this "sweep" and confirm in as much detail as is available
within the record from which specific Police Force (Metropolitan,
City or British Transport), which specific policing unit
(counterterrorism, community support, Commissioner's Office) and,
to the extent that the record indicates, who specifically was the
point of contact liasing with Tfl during this timeframe, either
advising or instructing the imposition and lifting of the
system-wide service suspension on the DLR, along with any and all
additional germaine facts or advice shared by these key decision
makers mitigating the respective decisions to first suspend, then
fully resume a substantially normal service at the relevant
junctures during the day's events.

I would also be grateful if you could clarify the basis for the
stark contrast apparently manifest in the evaluating the current
threat level estimate present across the Underground network and
the DLR network, namely any pertinent or germain information then
available supportive of the view that any security threat to the
DLR network was either negligible or non-existant and required no
further precautionary action, while the security and safety doubts
relative to the Underground remained both formidable and credible,
engendering the sense that some additional degree of caution be
exercised, something not considered to be a factor on the DLR when
lifting the suspension of service more promptly and decisively by
mid-afternoon.

Finally, I would be grateful if you could provide copies of all
daily maintainence logs submitted by the subcontractor relating to
both station platforms and in-service rolling stock units on the
Northern Line, City Branch, Kings Cross to Bank inclusive, and all
DLR premesises, property and Rolling stock units in-service and
operating between the Bank interchange and Canary Wharf incluisive,
relating to the whole 24 period of July 7th 2005

Yours faithfully,

(And with apologies and thanks in advance, yours very gratefully)

Mr. Paul Coker



From: FOI
Transport for London

3 April 2013





Dear Mr Coker



TfL Ref: FOI-0019-1213



Thank you for your email received by Transport for London (TfL) on 2 April
2013 asking for information about the events of 7 July 2005.



Your request will be processed in accordance with the requirements of the
Freedom of Information Act and TfL’s information access policy.



A response will be provided to you by 30 April.



In the meantime, if you would like to discuss this matter further, please
do not hesitate to contact me.



Yours sincerely



Lee Hill

FOI Case Officer



FOI Case Management Team

General Counsel

Transport for London







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