Tested and Injectable Polio Vaccine on Himself, His Wife, and His Family
Wellness Affect News Editor Comments:
The science and history of the polio vaccine is written by Dr. Viera Scheibner. The entire article, History and Science Prove Vaccines Practice Not Prevent Disease, can be read hither.
This was extracted from her enquiry presented inA critique of the xvi-folio Australian pro-vaccination booklet entitled "The Scientific discipline of Immunisation: Questions and Answers" –You tin can read the entire study hither.
While the polio vaccine is often referred to by those who believe in vaccines as the ultimate instance of a vaccine that eradicated a terrible disease that is no longer with us, the science and history of this vaccine tell a vastly different story.
From Dr. Scheibner's research below, we can clearly see certain facts in the history of polio vaccination:
i. There has been more than than ane blazon of polio vaccine through its history, due to the fact that earlier versions were found to be ineffective and harmful.
2. The occurrence of polio was trending downward prior to the introduction of polio vaccines.
3. The reported effectiveness accredited to polio vaccines tin really be easily accounted for by data manipulation and not actual decreases of occurrence. (Encounter likewise Dr. Suzanne Humphries' first-class handling of this subject hither: Did Vaccines Really Eradicate Polio?)
4. The history of the polio vaccine is a history of contamination of the vaccines responsible for the injury and deaths of countless people.
Update: The New York Times published a story nigh new strains of the polio vaccine being developed. Here is what they wrote concerning the current strain of the polio vaccine:
The Sabin vaccine has drawbacks, all the same: it contains a still-live virus that was mutated long ago so that it is usually also weak to produce affliction. In rare cases, it can mutate back into a dangerous form that paralyzes or kills. And the vaccine is risky in children with allowed-system bug. For those reasons, the Earth Health Organization plans to eventually phase it out.
Source: http://www.nytimes.com/2013/02/19/health/new-polio-strains-that-protect-vaccine-factory-workers.html
The sordid history of Poliomyelitis vaccination
Past Dr. Viera Scheibner (PhD)
International Medical Council on Vaccination
When the Salk injectable "formaldehyde killed" polio vaccine was tested on some 1.8 million American children in 1954‐55, cases of paralysis in the vaccinated and some of their contacts started occurring within days.(43)
The Cutter Laboratories were accused of distributing vaccines containing live polioviruses. Disasters with the Salk vaccines causing vaccine associated paralytic poliomyelitis (VAPP) seem to take been one of the main motivations behind development of an oral "live adulterate" Sabin vaccine, which was believed to simulate the natural infection. All the same, VAPP cases continued occurring with the Sabin vaccine.
I spent many hours locating and reading the older and more than recent articles addressing the effectiveness, or otherwise, of combining IPV and OPV vaccines. I established that the results are not straightforward. Abraham reported that shedding of virulent poliovirus revertants, during immunization with oral poliovirus vaccines, after prior immunization with inactivated polio vaccines, continued.(44)
He also documented that prior immunization with EIPV (enhanced authority IPV) does not prevent faecal shedding of revertant polioviruses after subsequent exposure to OPV. (45)
Mensi and Pregliasco wrote:
In contempo years great alarm has been generated past outbreaks of paralytic poliomyelitis in vaccinated populations…epidemics were observed in Finland in 1984, Senegal and Brazil in 1986, and Israel and Oman in 1988, all countries in which vaccination is widely deployed. 4 epidemics were reported between 1991 and 1992. The first, in 1991, was in Bulgaria, which uses oral vaccination. Forty-iii subjects developed paralytic type 1 polio; 88% of them belonged to a normal community and had not completed or fifty-fifty started a vaccination schedule. The second epidemic occurred in The Netherlands, where inactivated polio vaccine (IPV) is used, and involved 68 patients with blazon iii poliovirus, members of the Amish…(46) [In Holland they are called members of orthodox religion and in fact use the polio vaccination (compliance between forty‐50% and college)].
Schaap et al. published a graph (effigy 14) correlating the number of reported poliomyelitis cases with the vaccination rates in seven areas in Holland.(47) Interestingly, the areas with the lowest compliance had the everyman number of cases and vice versa. The compliance ranged from 40‐49% to xc‐95%. In the 1992 epidemic, the first two cases occurred in a 14‐twelvemonth old boy and 23‐year old male nurse, both vaccinated members of the orthodox religious group.
Sutter et al described an Oman outbreak equally:
. . . evidence for widespread transmission amidst fully vaccinated children. (48)
Incidence of paralytic disease was highest in children below 2 years:
. . . despite an immunisation programme that recently had raised coverage with three doses of oral poliovirus vaccine (OPV) among 12- months-old children from 67% to 87%… with transmission lasting for more than than 12 months. Amongst the most disturbing features of this outbreak was that it occurred in the face of a model immunisation programme and that widespread manual had occurred in a sparsely populated, predominantly rural setting. ( 49)
Ane of the interesting reasons quoted was:
. . . rapid increases in vaccination coverage before the outbreak may have reduced or interrupted endemic circulation of indigenous strains, diminishing the contribution of natural infection to overall immunity levels in the general population. ( l)
The aforementioned reason was given by Biellik et al. in 1994 when they described the situation in Namibia. They wrote:
Endemic wild poliovirus circulation has continued uninterrupted in Angola and the two northern regions in Namibia across the well-travelled border since 1989, when cases were last reported. Although OPV3 embrace age was fairly depression in northern compared with southern Namibia, a college proportion of northern children might accept been protected, at to the lowest degree to type 1, by natural amnesty, thus suppressing epidemics . . . the apparent interruption of[natural] poliovirus circulation[by vaccination]limited the acquisition of natural immunity. (five) 1
Control of polio in the US shows the same miracle every bit the control of pertussis, namely downwards trend, which stopped when individual states in the Usa mandated DPT and polio.
An interesting example of manipulation of information is polio "eradication" in the Americas. Figure xvi(52) shows the effect of reclassification of poliomyelitis which allowed the ever increasing number of "notified" cases to morph into an ever decreasing number of "confirmed" cases.
Dr HV Wyatt (53) quoted Hanlon et al. as stating:
…injections during an epidemic may provoke poliomyelitis in children already infected with poliovirus, [and] …provocation poliomyelitis occurs with injections of diphtheria/pertussis/tetanus vaccine, which, I am told, gives rise to unease amongst vaccinators. The gamble of provocation poliomyelitis with the killed poliovaccine…occurred in the Cutter incident.
During a poliomyelitis outbreak in Taiwan, Kim et al. reported that 65% of VAPP adult within 28 days of the get-go vaccine dose This written report confirmed observations of others that two thirds of vaccine‐targeted diseases occur afterwards the starting time dose of relevant vaccines, including the polio vaccine,(54) and it also unwittingly confirmed the original and true definition of herd immunity that has nothing to do with vaccines: Epidemics occur during the accumulation of 2 thirds of susceptibles.
Once natural amnesty is 2/3 of susceptibles go the disease, the epidemic stops. Yet, the authors excluded (as unvaccinated) all paralytic cases (65% of all cases) from calculations of efficacy. Ogra evaluated vaccination with alive attenuated and inactivated poliovirus vaccines:
While the combination schedule employing EP-IPV followed past OPV should effect in a decline of vaccine-associated (VAP) death in OPV recipients, such immunization schedule may accept little or no impact on the development of VAP in susceptible contacts. Furthermore, the logistics and the cost of combination schedule must be considered before current recommendations based on the use of OPV or EP-IPV solitary are revised.( 55)
Combined OPV and IPV recommendations
Standing failures of polio eradication past OPV led to the proposals of using a combination of killed followed by oral polio vaccine delivery. Withal, such proposals are flawed and based on the ignorance of the documented by experience.
Simian Virus xl contagion of polio vaccines
Perhaps the worst thing about polio vaccines is their continued contamination by monkey viruses of which SV 40 is the best researched one. According to ample medical enquiry evidence, polio vaccines of whatsoever kind cause VAPP.
However, there are other major issues with the polio vaccine that justify scepticism about its benefits, 1 of which is the well‐documented and continuous contamination by monkey viruses SV1‐SV40. Before long later on the poliovirus mass vaccination programmes started in the US, a number of monkey viruses and amoebas were found in the vaccine seed brews.
Hull, Milner et al. (56) and Hull, Johnston et al. (1955) encountered numerous filterable, transferable cytopathogenic agents other than polio virus in "normal" monkey renal prison cell cultures.
Even though these agents completely destroyed civilisation tissues, and even acquired serious diarrhoea in laboratory animals, all of which died, their possible pathogenesis in humans was ignored or glossed over.
The central nervous organization was particularly susceptible to the pathogenic properties of such viruses; the histopathological lesions observed in the intracerebrally inoculated monkeys revealed necrosis and consummate destruction of the choroid plexus.
Findings included generalised aseptic type meningitis. The isolated agent was called simian virus or SV and classified into 4 groups based on the cytopathogenic changes induced in monkey kidney cell cultures infected with these agents.
Hilleman and Sweetness (57) reported on the "Vacuolating virus S.5. forty", which became the all-time researched amidst dozens of known monkey viruses.
Gerber et al. (58) demonstrated that Sweet and Hilleman'due south method of inactivation of SV40 by 10 day treatment using ane: 4000 solution of formaldehyde was inadequate, since information technology took longer than 10 days to establish that the process was a subject area to the asymptotic factor and hence incomplete. Fenner's research (59) has besides established that even the inactivated portion of the viruses reverts back to the original virulence.
Dr Bernice Eddy documented the carcinogenic backdrop of these simian viruses: they caused tumours in hamsters injected with Rhesus monkey kidney cell extracts. (lx) As established past many subsequent researchers, in humans SV40 causes characteristic encephalon tumours, bone sarcomas, mesotheliomas and an specially virulent form of melanoma cancer.
The stage was prepare for a globe‐wide [admitted] contamination of hundreds of millions of children with an oncogenic monkey virus via polio vaccines. SV40 has been directly or indirectly implicated in an epidemic of great number of conditions and brain, lung, bone, renal and other tumours in all ages. (61,62,63,64,65)
Dr Stanley Kops is a modern day advocate for SV40 truth, and he wrote:
To appointment, the scientific literature and research examining SV40 and cancer-related diseases has been based upon an supposition that SV40 was not nowadays in whatever poliovirus vaccines administered in the United States and was removed from the killed polio vaccines by 1963. The presumption has been that the regulation for live oral polio vaccine required that SV40 be removed from the seeds and monovalent pools ultimately produced in the manufacturing procedure…The confirmation of the removal by ane manufacturer, Lederle, has been made public at an international symposium in January 1997, where its representatives stated that all Lederle's seeds had been tested and screened to clinch that it was costless from SV40 virus. However, in litigation involving the Lederle oral polio vaccine, the manufacturer'due south internal documents failed to reveal such removal in all its seeds. The absenteeism of confirmatory testing of the seeds, as well equally testimony for SV40 of a Lederle manager point that this merits cannot be fully substantiated…( 66)
The scientific customs should not be content with assurances to the contrary. The continuing occurrence of the to a higher place characteristic SV40 tumours in younger and peculiarly quite contempo generations of vaccinees should not be ignored or treated with indifference.
Contagion of polio vaccines by chimpanzee coryza virus, or RSV.
Another important consideration in attempts to eradicate poliomyelitis by vaccination is the contagion of polio vaccines by chimpanzee coryza virus, renamed respiratory syncytial virus (RSV).
In 1956, Morris et al. described monkey cytopathogenic amanuensis that produced acute respiratory illness in chimpanzees at the Walter Reed Ground forces Found of Enquiry and named it chimpanzee coryza virus (CCA). (67)
In 1957, Chanock et al. wrote on the association of a new type of cytopathogic myxovirus with infantile croup. (68)
Chanock and Finberg reported on two isolations of like agents from infants with severe lower respiratory illness (bronchopneumonia, bronchiolitis and laryngotracheobronchitis). The two viruses were indistinguishable from an agent associated with the outbreak of coryza in chimpanzees (CCA virus) studied past Morris in 1956.
A person working with the infected chimpanzees after experienced respiratory infection with a rise in CCA antibodies during convalescence. They proposed a new name for this amanuensis "respiratory syncytial virus" (RSV). RSV has spread via contaminated polio vaccines like wildfire all over the globe and continues causing serious lower respiratory tract infections in infants.
Beem et al. isolated the virus from inpatients and outpatients in the Bob Robert Memorial Hospital for Children (University of Chicago) during the winter of 1958‐1959, in association with man acute respiratory affliction. (69)
The virus (named Randall) had an unusual cytopathic effect characterised by extensive syncytial areas and giant cells. Soon, 48 similar agents were isolated from 41 patients.
There were antigenic similarities between RV and Long and Sue strains of CCA; it produced illness in humans (the age range three weeks to 35 years): astute respiratory diseases, croup, bronchiolitis, pneumonia and asthma ranging from mild coryza to fatal bronchiolitis.
The isolation rate (46%) was particularly high amid infants below six months.
In Commonwealth of australia, Lewis et al. isolated further viral specimens identical with CCA. (70)
Prior to July 1960, the influenza and parainfluenza viruses predominated in baby epidemic respiratory infections; in July 1961 the pattern changed abruptly with sudden increases in bronchiolitis and bronchitis, that were previously exceptional. 58% were under 12 months, and patients nether 4 years predominated. Infants with bronchiolitis and severe bronchitis yielded RCA, non previously isolated. Deaths have occurred.
Rogers' 1959 observations on antibiotic ineffectiveness, and new serious additional problems fell on deaf ears. He wrote that life‐threatening microbial infections continued to occur despite antibiotics, and that the previous microbial landscape likewise shifted by 1957‐1958. There was streptococcal predominance from 1938‐1940, and then an "impressive" increase in the number of life‐threatening enterobacterial infections post antibiotic.
During the preantimicrobial era most infections were acquired before admission to hospital, while in the postantimicrobial era the vast majority of infections arose in hospital . . . Mycotic infections, specially with Candida albicans, became a major problem. Unusual serious generalised clostridial infections arose and antibiotics have not dramatically altered the risk of, or mortality resulting from, endogenous infections in ill, hospitalised patients. ( 71)
Levy et al. wrote:
Respiratory syncytial virus (RSV) is the well-nigh prevalent cause of lower respiratory tract infections (LRTI) in infants and young children. Infections with RSV is a major wellness trouble during early childhood and primary RSV infections occurs about oft between the ages of vi weeks and 2 years. Approximately one half of all infants become infected with RSV during the first yr of life and nearly all infants by the end of their 2nd twelvemonth of life…in the US each yr, approximately 100,000 children are hospitalised at an estimated price of $300 1000000. More than half of those admitted for RSV bronchiolitis are between 1 and 3 months of age. (72) [Clearly implicating vaccination.]
RSV vaccine developed in the late 1960s failed miserably. It is no mystery why there is no RSV vaccine recommended today. Fulginiti and others showed the vaccine was ineffective, and induced an exaggerated, altered clinical response… causing RSV illness requiring hospitalisations among vaccinees, and led to delayed dermal hypersensitivity. (73)
Simoes wrote:
Since it was identified as the agent that causes chimpanzee coryza in 1956, and afterwards its subsequent isolation from children with pulmonary affliction in Baltimore, The states, respiratory syncytial virus (RSV) had been described as the single most important virus causing acute respiratory-tract infections in children. The WHO estimates that of the 12.2. million annual deaths in children under 5 years, a 3rd are due to acute infections of the lower respiratory tract. Streptococcus pneumoniae, Haemophilus influenzae, and RSV are the predominant pathogens… vaccinated children were not protected from subsequent RSV infection. Furthermore, RSV-naïve infants who received formalin-inactivated RSV vaccine, and who were naturally infected with RSV later, developed more severe disease in the lower respiratory tract than a control group immunized with a trivalent parainfluenza vaccine. ( 74)
Information technology should surprise nobody that data from ten developing countries –with intense polio vaccination, revealed that RSV was the most frequent crusade of LRT infections (70% of all cases).
Polio vaccines are not only ineffective in preventing paralysis, they carry the run a risk of contamination with many harmful adventitious microorganisms, of which merely some monkey viruses have been researched in more than detail. Many other potentially dangerous microorganisms remain unaddressed.
Polio vaccination and brain-eating amoebas.
Contamination of monkey kidney tissue cultures (used in the production of polio vaccines) past live amoebas.
In 1996, while watching a Telly news written report on the death of two 5‐twelvemonth olds in Australia from brain‐eating amoebae, I remembered a note in Hull et al.'s newspaper
Recently, an amoeba was isolated from monkey kidney tissue cultures and was identified as belonging to the genus Acanthamoeba. It grew readily in tissue cultures… It appeared to have the power to infect and kill monkeys and mice following intracerebral and intraspinal inoculation.(75)
Amoebas are unicellular protozoan microorganisms. According to Ma et al.(76), they are classified in the phyllum Sarcomastigophora and belong to Rhizopoda, equipped past propulsive pseudopodia and/or protoplasmic catamenia without product of pseudopodia. Acanthopodina, a suborder of Amoebida, grade two families, Vahlkampfiidae and Acanthoamoebididae, with two genera Naegleria and Acanthamoeba respectively, with a number of species. Naegleria species form three life‐stages, trophozoites, flagellates and cysts and Acanthamoeba species only ii, trophozoites and cysts.
Jahnes et al.(77) isolated 2 strains of obviously the aforementioned amoeba which looked like round bodies, similar in appearance to cells manifesting changes induced by certain simian (monkey) viruses. On closer test, they proved to be amoebic cysts. They varied in size, from 10 to 21 microns in diameter. In one experiment, the cysts were treated with ten% formalin, done and inoculated into monkey kidney tissue culture tubes. The monkey kidney cells phagocytised the cysts. The trophozooites turned into cysts under refrigeration down to four degrees C. These were resistant even under –50 degrees C for months and survived in the pH range 5.0‐9.0. Their tissue cultures were non afflicted by streptomycin and penicillin.
Culbertson (78,79) confirmed that amoebas acquired brain disease and death within days, in monkeys and mice. The reports showed, that following inoculations, "extensive chorio‐meningitis and subversive encephalomyelitis occurred" and killed monkeys in 4 to 7 days and mice in three to four days. Intravenous injections of the amoebas resulted in perivascular granulomatous lesions. Intranasal inoculation in mice resulted in fatal infections in about four days. These mice exhibited ulceration of the frontal lobes of the encephalon. There were amoebas in the lungs, and they caused astringent pneumonic amoeba reaction. Haemorrhage was a common feature. Sections of the kidney showed amoebas present in the glomerular capillaries.
Amoebas showed the power to migrate through the tissues. The size of the inoculum did not affair: both small and large inoculums produced amoebic invasions. Intragastric inoculations were unsuccessful most probably because amoebic cysts were dissolved by bile.
Researchers, every bit a rule failed to accost the seriousness of the introduction into children of Acanthamoeba via the polio vaccines, even though they were aware of their origin from monkey kidney tissue cultures used in the production of polio vaccines. Even so they noted that the most contaminated age grouping was babies below the age of crawling – between two and ten months.
Live amoebas were isolated from the air (80) in the Britain, together with respiratory syncytial virus, and from the surfaces in infirmary cubicles in which infants with acute bronchiolitis were being nursed. The amoebas were isolated at Booth Hall Children's Hospital in the cubicle occupied past a ten‐calendar week‐old infant with acute bronchiolitis. Showtime, only RSV was isolated and the child sent dwelling house, just later an unidentified cytopathic effect was noticed in the tissue cultures and was provisionally chosen "Ryan virus1" (81) past Pereira, and later besides noted in a post‐mortem bronchial swab of some other seven‐months old baby boy with RSV bronchiolitis.
Pereira'south paper describes the course of illness: Vi days earlier admission, the baby developed a sore throat and ulcers in the mouth which later spread over the face; he was unwell, could not suck and developed loose stools. The twenty-four hour period before access, he adult a cough and started vomiting. He was drowsy and dyspnoeic, made jerky movements and died soon subsequently admission. Necropsy showed some emphysema, petechiae, and small areas of congestion and alveolar haemorrhaging in the lungs, a fatty liver, prominent mesenteric nodes, and mucopus in the ears. Escherichia coli bacteria were cultured from his ears. Death was diagnosed equally due to a respiratory infection associated with encephalomyelitis and hepatitis. Vaccination status was not disclosed, although considering the historic period, the baby could have received up to iii doses of DPT and OPV vaccines.
Armstrong and Pereira identified the Ryan virus every bit Hartmanella castellanii. (82) They had no doubt that these amoebas came from the human being respiratory tract. In Australia, Fowler and Carter(83) Carter(84), and Carter et al.(85) described a number of cases in children and adults. Many cases all over the world occurred in children and adults, with and without histories of pond in lakes and public swimming pools. (86)
Even if polio vaccines were effective in preventing polio paralysis, their potentially continued contamination by undesirable microorganisms (monkey viruses and amoebas) should encourage the abandonment of their use.
Well‐pregnant Rotarians should study the relevant medical research first, earlier engaging in global polio vaccination.
The entire commodity, History and Scientific discipline Show Vaccines Exercise Not Prevent Disease, tin can be read hither.
Extracted from: A critique of the 16-page Australian pro-vaccination booklet entitled "The Science of Immunisation: Questions and Answers" –You can read the unabridged report here.
About the author
Dr Viera Scheibner is Principal Inquiry Scientist (Retired) with a doctorate in Natural Sciences from Comenius University in Bratislava. Later on an eminent scientific career in micropalaeontology during which she published three books and some 90 scientific papers in refereed scientific journals in Australia and overseas, she studied babies' breathing patterns with the Cotwatch breathing monitor developed past her late hubby Leif Karlsson in the mid 1980s. Babies had alarms after vaccination, indicating stress. This introduced her to the subject of vaccination. She so started systematically studying orthodox medical papers dealing with vaccination issues. To this day she has collected and studied more than than 100000 pages of medical papers.
Despite such extensive enquiry of orthodox medical papers published on vaccines over the past 100 years, she established that there is no scientific prove that these injections of highly baneful substances prevent diseases, quite to the contrary, that they increment susceptibility to the diseases which the vaccines are supposed to forbid and also to a host of related and unrelated viral and bacterial infections. Vaccines are involved in a great number of modern ills of babyhood such as immunoreactive diseases (asthma, allergies), autoimmune diseases (diabetes, multiple sclerosis, lupus erythematosis), cancers, leukaemia, degenerative diseases of bone and cartilage, behavioural and learning problems, to mention just the most of import conditions.
Her inquiry into vaccination has culminated so far in 2 books and a number of shorter and longer individual papers published in a variety of scientific and medical publications. She has likewise conducted frequent international lecture tours to present the results of her research to parents, wellness and medical professionals and anyone else who is interested. She has also provided a great number of practiced witness reports for court cases relating to deaths and injuries caused by vaccines, such as and so-called "shaken infant" syndrome.
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Published on Feb 19, 2013
Source: https://healthimpactnews.com/2013/the-real-history-behind-the-polio-vaccine/
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