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Thread: Attacking Ourselves: Top Doctors Reveal Vaccines Turn Our Immune System Against Us

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    Attacking Ourselves: Top Doctors Reveal Vaccines Turn Our Immune System Against Us

    Attacking Ourselves: Top Doctors Reveal Vaccines Turn Our Immune System Against Us

    Published 3 days ago on November 26, 2018
    By Collective Evolution


    The Facts:Vaccines can trigger autoimmunity with a laundry list of diseases to follow. With harmful and toxic metals as some vaccine ingredients, who is susceptible and which individuals are more at risk? A new study shows what they do to our immune system.

    Reflect On:With so many scientists and publications emerging showing multiple concerns with vaccines, why are they marketed as completely life-saving and necessary when that's actually not the case?

    No one would accuse Yehuda Shoenfeld of being a quack. The Israeli clinician has spent more than three decades studying the human immune system and is at the pinnacle of his profession. You might say he is more foundation than fringe in his specialty; he wrote the textbooks. The Mosaic of Autoimmunity, Autoantibodies, Diagnostic Criteria in Autoimmune Diseases, Infection and Autoimmunity, Cancer and Autoimmunity – the list is 25 titles long and some of them are cornerstones of clinical practice. Hardly surprising that Shoenfeld has been called the “Godfather of Autoimmunology” – the study of the immune system turned on itself in a wide array of diseases from type 1 diabetes to ulcerative colitis and multiple sclerosis.

    But something strange is happening in the world of immunology lately and a small evidence of it is that the Godfather of Autoimmunology is pointing to vaccines – specifically, some of their ingredients including the toxic metal aluminum – as a significant contributor to the growing global epidemic of autoimmune diseases. The bigger evidence is a huge body of research that’s poured in in the past 15 years, and particularly in the past five years. Take for example, a recent article published in the journal Pharmacological Research in which Shoenfeld and colleagues issue unprecedented guidelines naming four categories of people who are most at risk for vaccine-induced autoimmunity.

    “On one hand,” vaccines prevent infections which can trigger autoimmunity, say the paper’s authors, Alessandra Soriano, of the Department of Clinical Medicine and Rheumatology at the Campus Bio-Medico University in Rome, Gideon Nesher, of the Hebrew University Medical School in Jerusalem and Shoenfeld, founder and head of the Zabludowicz Center of Autoimmune Diseases in the Sheba Medical Center at Tel Hashomer. He is also editor of three medical journals and author of more than 1,500 research papers across the spectrum of medical journalism and founder of the International Congress on Autoimmunology. “On the other hand, many reports that describe post-vaccination autoimmunity strongly suggest that vaccines can indeed trigger autoimmunity. Defined autoimmune diseases that may occur following vaccinations include arthritis, lupus (systemic lupus erythematosus, SLE) diabetes mellitus, thrombocytopenia, vasculitis, dermatomyosiositis, Guillain-Barre syndrome and demyelinating disorders. Almost all types of vaccines have been reported to be associated with the onset of ASIA.”

    ASIA – or Autoimmune/Inflammatory Syndrome Induced by Adjuvants (also known as Shoenfeld’s syndrome) — first appeared in the Journal of Autoimmunology four years ago. It is an umbrella term for a collection of similar symptoms, including Chronic Fatigue Syndrome, that result after exposure to an adjuvant – an environmental agent including common vaccine ingredients that stimulate the immune system. Since then an enormous body of research, using ASIA as a paradigm, has begun to unravel the mystery of how environmental toxins, particularly the metal aluminum used in vaccines, can trigger an immune system chain reaction in susceptible individuals and may lead to overt autoimmune disease.

    Autoimmune disease results when the body’s system meant to attack foreign invaders turns instead to attack part of the body it belongs to (auto is Greek for self). If the immune system is like a national defence system, antibodies are like drones programmed to recognize a certain type of invader (a bacteria say) and to destroy them or mark them for destruction by other special forces. Autoantibodies are like drones that are misidentifying a component of the human body and have launched a sustained attack on it. If they mistakenly target a component of the conductive sheath around neurons, for example, nerve impulses stop conducting properly, muscles go into spasm and coordination fails; multiple sclerosis results. If autoantibodies erroneously focus on joint tissue; rheumatoid arthritis results. If they target the islets of Langerhans in the pancreas, Type 1 diabetes, and so on

    “Throughout our lifetime the normal immune system walks a fine line between preserving normal immune reactions and developing autoimmune diseases,” says the paper. “The healthy immune system is tolerant to self-antigens. When self-tolerance is disturbed, dysregulation of the immune system follows, resulting in emergence of an autoimmune disease. Vaccination is one of the conditions that may disturb this homeostasis in susceptible individuals, resulting in autoimmune phenomena and ASIA.”

    Who is “susceptible” is the subject of the paper entitled, “Predicting post-vaccination autoimmunity: Who might be at risk?” It lists four categories of people: 1) those who have had a previous autoimmune reaction to a vaccine, 2) anyone with a medical history of autoimmunity, 3) patients with a history of allergic reactions, 4) anyone at high risk of developing autoimmune disease including anyone with a family history of autoimmunity, presence of autoantibodies which are detectable by blood tests and other factors including low vitamin D and smoking.

    Regarding those who have had a previous adverse reaction to vaccines, the paper cites five relevant studies including the case of a death of a teenage girl six months following her third Gardasil injection against HPV virus. She had experienced a range of symptoms shortly after her first dose, including dizziness, numbness and tingling in her hands, and memory lapses. After her second injection, she developed “intermittent arm weakness, frequent tiredness requiring daytime naps,” worse tingling, night sweats, chest pain and palpitations. A full autopsy was unrevealing but blood and spleen tissue analysis revealed HPV-16 L1 gene DNA fragments – matching the DNA found in vials of the Gardasil vaccine against cervical cancer – “thus implicating the vaccine as a causal factor.” The DNA fragments had also been found to be “complexed with the aluminum adjuvant” which, according to the report, have been shown to persist for up to 8 to 10 years causing chronic immune system stimulation.

    “Although data is limited,” Shoenfeld and his colleagues concluded, “it seems preferable that individuals with prior autoimmune or autoimmune-like reactions to vaccinations, should not be immunized, at least not with the same type of vaccine.”

    The second group which the paper cites for vaccine exemption is patients with “established autoimmune conditions.” Vaccines don’t work so well in them, say Shoenfeld and his colleagues, and they are at “risk for flares following vaccination.” Inoculations that contain live viruses including chickenpox, yellow fever and the measles, mumps and rubella triple vaccine (MMR) are “generally contraindicated” for people with autoimmune conditions because of the risk of “uncontrolled viral replication.” But inactivated vaccines are not such a good idea either because they usually contain the added ingredient aluminum, linked to autoimmunity.

    The immunologists describe recent studies in which patients with autoimmune rheumatic disease given the influenza vaccine (without aluminum) suffered more joint pain and fever than controls and whose levels of autoantibodies (the drones that attack self) increased after receiving the flu vaccine. What’s more, they developed new types of autoantibodies that weren’t present before the vaccines, and those persisted. As the presence of autoantibodies can be predictive of developing autoimmune disease in patients without symptoms, even years ahead of disease onset, this is troubling to those who understand immunology.

    A number of studies claim vaccines are safe for the “overwhelming majority of patients with established autoimmune diseases,” the study allows, but they only looked at rheumatoid arthritis and lupus and not at severe and active cases so “the potential benefit of vaccination should be weighed against its potential risk,” they cautioned.

    Vaccine trials have usually excluded “vulnerable” individuals — only extremely healthy individuals with no allergies are recruited. It’s a “selection bias,” say Soriano and Shoenfeld, and has likely resulted in serious adverse events being “considerably underestimated” in “real life where vaccines are mandated to all individuals regardless of their susceptibility.” The true incidence of allergic reactions to vaccines, normally estimated at between one in 50,000 to one in a million doses, is probably much higher and particularly where gelatin or egg proteins are on the ingredients list, they say.

    There’s a long list of vaccine ingredients that are potential allergens: besides the infectious agents themselves, there are those from hen’s egg, horse serum, baker’s yeast, numerous antibiotics, formaldehyde and lactose, as well “inadvertent” ingredients such as latex. People’s allergic histories have to be taken before vaccination say the researchers. But some signs of reaction don’t show up until after the shot.

    The public health nurse or GP might tell patients that a long-lasting swelling around the injection site after a vaccine is a normal reaction, for example. But that is not what the immunologists say. “[A]luminum sensitization manifests as nodules [hard lumps] at the injection site that often regress after weeks or months, but may persist for years.” In such cases, they say, a patch test can be done to confirm sensitivity and to avoid vaccination.

    According to a growing body of research, though, allergy may be only the beginning of many dangerous aluminum-induced phenomena.

    Aluminum has been added to vaccines since about 1926 when Alexander Glenny and colleagues noticed it would produce better antibody responses in vaccines than the antigen alone. Glenny figured the alum was inducing what he called a “depot effect” – slowing the release of the antigen and heightening the immune response. For 60 years his theory was accepted dogma. And over the same time, the vaccine schedule grew decade on decade, but few ever questioned the effects of injecting aluminum into the body, which is strange considering its known toxicity.

    A PubMed search on aluminum and “toxicity” turns up 4,258 entries. Its neurotoxicity is well documented. It affects memory, cognition, psychomotor control; it damages the blood brain barrier, activates brain inflammation, depresses mitochondrial function and plenty of research suggests it is a key player in the formation of the amyloid “plaques” and tangles in the brains of Alzheimer’s patients. It’s been implicated in Amyotrophic Lateral Sclerosis and autism and demonstrated to induce allergy.

    When kidney dialysis patients were accidentally infused with aluminum, the “dialysis-induced encephalopathy” (DAE) they developed neurological symptoms: speech abnormalities, tremors, memory loss, impaired concentration and behavioural changes. Many of the patients eventually went into comas and died. The lucky ones survived: when the source of toxicity, aluminum, was removed from their dialysis they recovered rapidly.

    With these new observations, researchers began investigating the adjuvant effects of aluminum and in the past decade there has been a flurry of research. Far from being a sandbag that holds the antigen for a while and then gets excreted, it turns out that aluminum salts trigger a storm of defence action. Within hours of injection of the same aluminum oxyhydroxide in vaccines into mice, for example, armies of specialized immune cells are on the move, calling in grid coordinates for more specialist assault forces. Within a day, a whole host of immune system commandos are in play — neutrophils, eosinophils, inflammatory monocytes, myeloid and dendritic cells, activating lymphocytes and secreting proteins called cytokines. The cytokines themselves cause collateral damage but they send out signals, directing cell-to-cell communication and recruiting other cells into action. If the next phase of the attack is launched: fibroblast growth factor, interferons, interleukins, platelet derived growth factor, transforming growth factor and tumour necrosis factor might all be engaged. There’s evidence that poorly understood and pesky inflammasomes, (currently a topic of cutting- edge cancer causation research) such as the Nod-like receptor 3( NLRP) are activated too, but it’s all still too early to say exactly what they’re doing.

    New research emerging from University of British Columbia has found that aluminum adjuvant injected into mice can alter the expression of genes associated with autoimmunity. And in their recent study published in the Proceedings of the National Academy of Sciences, immunologists at the University of Colorado found that even host DNA is recruited into the aluminum assault, that it rapidly coats injected alum, triggering effects that scientists have barely scratched the surface of understanding.

    This mobility or “translocation” of aluminum in the body is perhaps the most disturbing of the mounting evidence in current aluminum research. In 1998, French researcher Romain Gherardi and his colleagues observed an emerging condition of unknown origin which presented in patients post-vaccination with Chronic Fatigue like symptoms including swollen lymph nodes, joint and muscle pain and exhaustion. Tissue biopsies of the patients’ deltoid revealed lesions up to 1 cm in diameter and unique from similar lesions of other diseases. They went to the lab for analysis and to Gherardi’s astonishment, they mainly consisted of macrophages – large white blood cells in the immune system whose job is to swallow up foreign invaders in the body. Enclosed in the cellular fluid of these phagocytes were agglomerates of nanocrystals of aluminum.

    Gherardi and his colleagues began injecting mice with aluminum to see what happened. Their research published in 2013 revealed that the metal particles were engulfed by macrophages and formed MMF-like granulomas that dispersed — to distant lymph nodes, spleen, liver and eventually the brain.

    “This strongly suggests that long-term adjuvant biopersistence within phagocytic cells is a prerequisite of slow brain translocation and delayed neurotoxicity,” writes Gherardi in his February 2015 review of the relevant research in Frontiers in Neurology.

    A more frightening animal study of aluminum is that of Spanish veterinary researcher Lluis Lujan’s study of ovine ASIA. After huge numbers of sheep in Spain died in 2008 in the wake of compulsory multiple vaccine campaigns against bluetongue in Spain in 2008, Lujan set out to find out what killed them – and he began by inoculating them with aluminum.

    His 2013 study found that only 0.5% of sheep inoculated with aluminum vaccines showed immediate reactions of lethargy, transient blindness, stupor, prostration and seizures – “characterized by a severe meningoencephalitis, similar to post-vaccine reactions seen in humans.” Most of them recovered, temporarily, but postmortem exams of the ones who didn’t reveal acute brain inflammation.

    The delayed onset “chronic” phase of the disease affected far more of the sheep — 50-70% of flocks and sometimes virtually 100% of animals within a given flock, usually including all of those who had previously recovered. The reaction was frequently triggered by exposure to cold and began with restlessness and compulsive wool-biting, then progressed to acute redness of the skin, generalized weakness, extreme weight loss and muscle tremors, and finally, entered the terminal phase where the animals went down on their front quarters, became comatose and died. Post-mortem examinations revealed “severe neuron necrosis” and aluminum in the nerve tissue.

    The immune system’s reaction to aluminum “represents a major health challenge,” Gerhardi declares in his recent review, and he adds that “attempts to seriously examine safety concerns raised by the bio-persistent character and brain accumulation of alum particles have not been made… A lot must be done to understand how, in certain individuals, alum-containing vaccines may become insidiously unsafe.”

    Back to the problem of which “certain individuals” should avoid vaccination to avoid autoimmune disease.

    Soriano and Shoenfeld’s identify a final category: anyone at risk of developing autoimmune disease. Since a number of them have been shown to have genetic factors that would include anyone with a family history of autoimmune disease. It also includes anyone who has tested positive for autoantibodies which can indicate disease years before symptoms show up. Vaccinations, the doctors say, “may trigger or worsen the disease.”

    Smokers too, have an exceptionally high risk of developing an autoimmune disease, says the report. The American Cancer Society estimates that about 18% of Americans smoke. That means about 42 million Americans have an elevated risk of developing an autoimmune disease and they’re stacking the odds with every vaccine.

    And finally, factors that Shoenfeld and Soriano associate with high risk of developing autoimmunity are high estrogen and low vitamin D — which means anyone taking birth control or hormone replacement therapy and, according to one 2009 study of vitamin D status, about three quarters of American teens and adults should be wary of vaccines.

    Shoenfeld doesn’t seem to mean to exclude all of these people from immunization, however. The paper concludes that “for the overwhelming majority of individuals, vaccines carry no risk of systemic autoimmune disease and should be administered according to current recommendations.” Which is in stark contrast to the body of the paper. The final word is cautionary about weighing the “potential benefit of vaccination…against its potential risk.”

    It’s exemplary of a strange sort of schizophrenia in a wide range of recent immunology papers. The doctors seem to be trying to reconcile a century of “safe and effective” vaccine dogma with the last decade’s worth of terrifying research findings. There’s a lot of “on the one hand” and “on the other hand” in them.

    The new research seems about to gain the upper hand, however. A 2013 overview of ASIA by six immunologists including Shoenfeld, for example, is a catalogue of vaccine side effects from Gardasil deaths, narcolepsy epidemics, infertility, chronic fatigue, dead sheep and aluminum-addled brains. It is rife with statements that would have been virtually unheard of inside mainstream medicine a decade ago.

    Like this shocker:

    “Perhaps, in twenty years, physicians will be duelling with better-characterized particles of autoimmunity, and the vaccines may become fully safe as well as effective. Nonetheless, the recognition of ASIA has initiated the change to put more efforts in identifying the good, the bad and the ugly of vaccines and in particular of adjuvants as triggers of autoimmunity.” Bad and ugly of vaccines? What’s wrong with the adjuvants? That’s not in the CDC hand-out.

    Or how about this one:
    “Despite the huge amount of money invested in studying vaccines, there are few observational studies and virtually no randomized clinical trials documenting the effect on mortality of any of the existing vaccines. One recent paper found an increased hospitalization rate with the increase of the number of vaccine doses and a mortality rate ratio for 5-8 vaccine doses to 1-4 doses of 1.5, indicating a statistically significant increase of deaths associated with higher vaccine doses. Since vaccines are given to millions of infants annually, it is imperative that health authorities have scientific data from synergistic toxicity studies on all combinations of vaccines…” That could be any anti-vaxxer jabbering on…but it’s not.

    But here is the topper:
    “The US Supreme Court ruled that vaccines makers are immune from lawsuits charging that the design of the vaccine is defective. Thus there is need for innovative clinical trial design and the vaccines themselves should be redesigned.” Immunologists including the world’s leading authority on autoimmunity are saying it is time to take vaccines back to the drawing board.

    Autoimmune disease is the third leading cause of morbidity and mortality worldwide and now among the top 10 killers of young American women. The American Autoimmune Related Diseases Association estimates that 50 million Americans suffer from one of 88 autoimmune diseases — from type 1 diabetes to systemic lupus erythematosus — and some research puts the figure at one in five globally. At least 40 more diseases are suspected to be immune-mediated. Most of them are devastating — frequently crippling, expensive to treat and incurable. And they are increasing at an astonishing pace.

    At this stage, it looks like the more the research pours in, the harder it is going to get for pro-vaccine immunologists to keep multiple personality disorder – or complete nervous breakdown — at bay. Ten years of cutting edge research into aluminum’s effects on the immune system has revealed primarily how wrong they were. And how little they know. If, after 90 years, doctors finally have begun to seriously examine the mechanism and question the merits of injecting metal toxins into newborn babies, what have they yet to discover? ASIA sounds awful. (Too bad for all the people whose kids suffered through chronic fatigue when it was just a Freudian yearning to sleep with their mother.) But what if, like Lujan’s sheep, the “negligible” minority that has been paying the price for the good of humanity is actually only the tip of the iceberg? What if some people with no apparent adverse immune reactions still have nanocrystals of aluminum silently depositing in their brains? What if ASIA really includes Alzheimer’s? ALS, autism? ADD? And that’s just the A’s.

    Even if immunologists keep wearing their rose coloured glasses, and vaccine ingredients are only responsible for a tiny fraction of the exploding autoimmunity, the “ugly” in vaccines will still get harder and harder to ignore. When everyone on the planet is getting injected, 20 years is a long time for disabled people to stack up while scientists “duel with the characterized particles of autoimmunity.” In the fury over the Disneyland measles outbreak that is gripping the world’s vaccine promoters, time is running out for doctors and researchers who see the “bad and ugly” side of vaccines and their adjuvants to do something about it. There’s slim chance of a vaccine redesign in the absence of a profit incentive and a strong chance of universal vaccine mandates for one and all — previous anaphylactic shock reaction or not.

    This article was written by Sayer Ji, Founder of His work is reproduced and distributed here with the permission. Want to learn more from GreenMedInfo? Sign up for the newsletter here:”
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    No, they didn't. And no, they don't.

    Garbage post.
    * Enforce Border Security – America should be guarding her own borders and enforcing her own laws instead of policing the world and implementing UN mandates.

    * No Amnesty - The Obama Administration’s endorsement of so-called “Comprehensive Immigration Reform,” granting amnesty to millions of illegal immigrants, will only encourage more law-breaking.

    * Abolish the Welfare State – Taxpayers cannot continue to pay the high costs to sustain this powerful incentive for illegal immigration. As Milton Friedman famously said, you can’t have open borders and a welfare state.

    * End Birthright Citizenship – As long as illegal immigrants know their children born here will be granted U.S. citizenship, we’ll never be able to control our immigration problem.

    Reprinted from [Nov. 29, 2011]

  4. #3
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    Why should anyone listen to top doctors when government workers at the CDC say that all vaccines are perfectly safe?
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  5. #4
    Quote Originally Posted by Cleaner44 View Post
    Why should anyone listen to top doctors when government workers at the CDC say that all vaccines are perfectly safe?
    The CDC is a subsidiary of the pharmaceutical industry. The agency owns more than 20 vaccine patents and purchases and sells $4.1 billion in vaccines annually. Congressman Dave Weldon has pointed out that the primary metric for success across the CDC is how many vaccines the agency sells and how successfully the agency expands its vaccine program—regardless of any negative effects on human health.

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  6. #5
    Quote Originally Posted by Cleaner44 View Post
    Why should anyone listen to top doctors when government workers at the CDC say that all vaccines are perfectly safe?
    Hint: There's no such thing as "TOP" doctors. That should be a major clue that the article is relying on fabrications, opinions and omissions to get high school dropouts to click it.
    * Enforce Border Security – America should be guarding her own borders and enforcing her own laws instead of policing the world and implementing UN mandates.

    * No Amnesty - The Obama Administration’s endorsement of so-called “Comprehensive Immigration Reform,” granting amnesty to millions of illegal immigrants, will only encourage more law-breaking.

    * Abolish the Welfare State – Taxpayers cannot continue to pay the high costs to sustain this powerful incentive for illegal immigration. As Milton Friedman famously said, you can’t have open borders and a welfare state.

    * End Birthright Citizenship – As long as illegal immigrants know their children born here will be granted U.S. citizenship, we’ll never be able to control our immigration problem.

    Reprinted from [Nov. 29, 2011]

  7. #6
    Quote Originally Posted by angelatc View Post
    Hint: There's no such thing as "TOP" doctors. That should be a major clue that the article is relying on fabrications, opinions and omissions to get high school dropouts to click it.
    Top Doctors

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  8. #7
    Yehuda Shoenfeld's study looked at 21 sheep in a non- ramdomized, non- blinded study of 21 sheep in three groups- only seven in a group- a very small sample and not humans. It attempted to observe changes in the sheep behavior which is difficult- you can't ask them any questions. Instead they had to rely on subjective observations. Since they knew which sheep received the vaccines and which didn't they could have imposed their own beliefs of what changes they saw. They sheep were also given doses hundreds of times higher than that a human would receive.

    A lousy study which cannot be used to apply to humans and normal vaccinations.

    Sheep vaccine study critique

    Despite the fact that the paper has a couple of discredited claims, about aluminum and ASIA, there are other significant issues with the paper. Let’s review:

    The researchers only looked at a total of 21 sheep in 3 groups. Important clinical and epidemiological studies have thousands or even millions of data points. It is difficult, if not impossible, to determine a causal link with such a tiny sample size.

    The animals in the two experimental groups, one vaccinated with the typical vaccines given to sheep and the other with just aluminum adjuvant. The animals received 16 vaccine doses within 12 months for a total of 70.861 mg of aluminum. These are the number of doses that a sheep receive over 6-7 years! Furthermore, if you’re prone to comparing sheep to humans, that’s 20X more aluminum adjuvant than a human receives over a year – of course, human infants are smaller. Nevertheless, even though I dismiss any link between injected aluminum and neurological issues, giving 6-7 years of vaccines over 12 months biases the results. In addition, I’m skeptical of the behavioral observations, but it is possible that the serum aluminum levels are so high that it exceeds the safe limit for aluminum.

    The study was not randomized or blinded (or they failed to mention it in the methods section). You might think that randomization on matters with humans, but the researchers could have biased the results by the way they treated the sheep.

    This study relied upon subjective observations of the sheep’s “behavior” post-vaccination. These are the type of issues that hinder many behavioral and neurological studies – a subjective analysis of change in behavior is almost impossible to quantify. And when there are just 21 animals, it’s almost impossible.

    Sheep are social animals and the process of vaccination itself, especially so many over a short period of time, may induce behavioral changes irrespective of any contents of the vaccine, although the control group did receive a placebo injection.

    This sheep vaccine study is a primary research article – that means it lacks any supporting data anywhere else. It’s like the old vaccines cause autism canard – one retracted study supported it. On the other hand, literally hundreds of clinical and epidemiological studies along with meta-reviews have debunked that claimed link. That’s why most real biomedical researchers ignore primary animal studies – they pique interest, but rarely form the foundations of science-based medicine. Since we have dozens of studies that show no behavioral changes post vaccination, how much does a very small, very poorly designed sheep study tell us? Next to nothing.

    In a 2013 study by the same research group, they observed that around 0.5-1.0 % of animals of a flock exhibit the type of behavioral symptoms, irrespective of vaccination, described in the newer paper – yet they conveniently ignore it. Given the tiny sample size, the lack of randomization or blinding, and other issues, it’s impossible to tell if this is background noise.
    Donald Trump: 'What you're seeing and what you're reading is not what's happening'

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  9. #8
    Sounds legit.
    Quote Originally Posted by dannno View Post
    Trump hasn't even been in 6 months, you can't call him a boondoggle President unless he has overseen a military boondoggle for at least a year or two.

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  11. #9
    Vaccine Realities That Big Pharma Doesn’t Teach Us Doctors (or Our Patients). The Plight of “Vaccine Damaged Children”
    And Why America’s Mandated Over-vaccination Schedules are Unsafe and of Questionable Usefulness

    By Dr. Gary G. Kohls

    “In 1986 a US law was passed that protected vaccine maker’s from ever being sued in a a regular court regardless of how many babies or children were injured of killed from the aluminum, mercury (aka Thimerosal), formaldehyde, aborted fetal cells, deadly peanut byproducts, cells of pigs, cows, monkeys, dogs, insects, MSG (monosodium glutamate), ether and other toxins that make up normal vaccines. At that time 1 in 10,000 children had Autism. Children went from 7 vaccines to more than 70. Today as many as 1 in 25 boys over age 12 has autism-which is really a term to hide the real condition: vaccine-induced encephalitis (inflammation of the brain) and 1 in 5 high school kids have ADHD, Tourette’s syndrome, epilepsy, asthma, diabetes and cancer has gone sky high. No vaccine is ever looked at for its ability to cause cancer-surely not the combination of vaccines and cancer is now the leading cause of death ion little children. There is a federal Vaccine court that has paid 3.3 BILLION dollars to families bright enough to learn the system and were able to prove that the autism was from the vaccines.” — Shelley Tzorfas, author of Recovering Autism, ADHD, & Special Needs

    Over the several decades since I really started studying vaccine issues in some depth – much too late for many of my vulnerable patients – I have come to see through the pervasive Big Pharma/Big Vaccine/Big Medicine propaganda that falsely and repeatedly asserted that all vaccines are safe, effective and necessary for the public health.

    I have come to understand that my academic professors at the University of Minnesota Medical School that taught us naïve students about the alleged safety and alleged efficacy of mass vaccination campaigns had also been mis-taught by their own professors who probably only knew the historical myths about Jenner, cowpox and smallpox and the early myths about Salk and Sabin and their often failed, even disastrous experiments with polio vaccines

    I suspect also that by the mid-1960s my professors were increasingly coming under the corrupting influence of the pharmaceutical industry and their Wall Street cronies that were recognizing the enormous corporate profits to be made by selling more and more dependency-inducing and increasingly expensive, patentable, synthetic drugs and vaccines. In fairness to my now-deceased professors, there were far fewer drugs and only a miniscule number of toxic vaccines available back then (1964 – 1968).

    I last practiced family medicine in an under-served area of rural Minnesota about 20 years ago. Since then I have had more time and energy to understand how and why the academic doctors that wrote my med school text books also emphasized to us students – without corroborating evidence –that vaccines were always safe and effective. These textbook authors had also likely developed significant, undeclared conflicts of interest with the industries that provided the propaganda that made us easily-bamboozled student doctors into devoted life-long prescribers of their drugs and vaccines.

    Of course, nothing was taught to us back then about the multiple toxic ingredients that are in every vaccine dose or the lack of proof of efficacy when cocktails of several combinations of vaccines (or drugs) are injected simultaneously into the tiny muscles of our infant and toddler-age patients. But students, particularly medical students, aren’t known for questioning authority, especially if the authorities are esteemed and renowned (albeit often arrogant) professors. Most of us students weren’t aware that most of our professors had never suffered through the trials of being a self-employed, primary-care physician that had to deal with normal members of the community.

    These academics didn’t explain to us med students (and perhaps they didn’t understand it themselves) that the intentionally-deceptive “relative risk” statistics (as opposed to the more honest “absolute/actual risks”) came from Big Pharma’s statisticians and that those statistics consistently, intentionally and fraudulently over-rated the effectiveness and safety of their products. (Those products included not just their vaccines but also their dependency-inducing prescription drugs that frequently caused serious withdrawal effects that made stopping them both hard to do AND hazardous).

    So we naive future teachers of our equally naïve – and easily bamboozleable – future patients have all been brainwashed into trusting the untrustworthy Big Pharma cartel and their “authoritative” propaganda that was so good for business. Most people tend to be obedient to the orders of authoritative folks and physicians and their patients are no different.

    And then, after we students finally finished our internships or residency programs, we were employed by various for-profit private medical practices, and we found out that our clinics could make a lot of money getting parents to bring their previously well babies in for their “well-baby exams” and their obligatory, periodic cocktails of “well-baby shots”. It didn’t occur to us rookie physicians at the time that the clinics made far less money than the vaccine makers and marketers did. We just went on guiltlessly and happily doing what we had learned in school – and we rarely questioned anything that we had been taught.

    But most seriously, we students were never taught much immunology or even the basic science of how vaccines actually “work” while we were in med school. I myself only started trying to fully understand the little that I had been taught about vaccines after a close relative started having neurological issues after his 4 month well baby shots. (He was eventually diagnosed with Asperger’s syndrome). It was only then that I finally started listening to and trusting the many anguished and justifiably distraught and angry parents whose vaccine-sickened or vaccine-killed children had unequivocally been neurologically damaged by their baby shots.

    After hearing of the multitude of vaccine-damaged children, I have become more and more outraged over the fact that many of the parents – whose children and lives had been permanently devastated by vaccine injuries – have actually been fired from the previously-trusted medical practices whose vaccines had injured their children.

    The science of vaccine-induced neurotoxicity is actually quite understandable, even for laypeople – if they were ever taught the principles. It might even be easier for laypeople to learn than for indoctrinated physicians! I include a few of the principles in the last half of this column.

    For example, it is easy for anybody to understand that until the year 2000, the highly neurotoxic mercury, in the form of Thimerosal, was commonly used in many vaccines as a preservative that was included in order to prevent bacterial overgrowth in the commonly-used, rubber-stoppered multiple-dose vials. Mercury is the 2ndmost neurotoxic substance on the planet – right behind the highly radioactive element plutonium – and there is no known safe dose! The CDC, the AAP, the AMA and the media are correct in their admonitions to parents of children to have the kids avoid eating fish that might contain mercury but are to be condemned when they refuse to say anything about the mercury in vaccines. Mercury is still used in multidose influenza vaccine vials but, according to sources inside Big Pharma, trace amounts of it are still being found in other multidose, non-live virus vaccines as well.

    In addition, solid microparticles of the known neurotoxic metal aluminum are used in many vaccines as an adjuvant. Particulate aluminum compounds are known to exaggerate immune responses when incubated with the intended viral particles in the vaccine solutions. The number of antibodies produced in response to an aluminum-containing vaccine are orders of magnitude greater than can be achieved with a vaccine that has no aluminum in it. Again, just like mercury, there is no known safe dose of aluminum when it is injected intramuscularly.

    In addition, any of the live (albeit allegedly “attenuated”) measles viruses that are in the MMR vaccines are known to be capable of causing low-grade viral encephalitis or non-infectious encephalopathies that are diagnosed as brain disorders such as learning disorders, autism, Asperger’s disorder, ADHD, behavioral disorders, chronic headaches, epilepsy, allergies, asthma, narcolepsy, speech delays, low IQs, etc.

    Vaccine-induced diseases are all, of course, “iatrogenic” disorders which are defined as “caused by doctors, doctor-prescribed drugs, vaccines or surgery”. It is to be expected that any industry will try to downplay the toxic effects of its products in order to avoid legal liability and Big Medicine and Big Pharma are no different.

    How many things could possibly go wrong when even a highly-skilled nurse tries to inject cocktails of liquids containing a multitude of potentially toxic synthetic chemicals into the tiny muscles of a neurologically-vulnerable infant. Failing to hit tiny muscles of an infant with a needle has to be fairly common in average medical clinics and probably accounts for the significant variability of vaccine efficacy that has frequently been found in pharmaceutical industry-sponsored studies.

    But the Big Pharma cartels, the Big Medicine professional trade associations, the Big Pharma lobbyists and the Big Pharma-subsidized mainstream media voices easily out-spend, out-advertise and out-shout those of us who are trying to warn about the many dangers of the toxic substances that are in most vaccines.

    One of the major reasons why vaccines may actually do more harm than good can be understood if one understands that true immunity can only occur if both of the two essential aspects of immunity occur together.

    Cellular/mucosal Immunity and Serological/humoral Immunity

    Long-lasting or permanent immunity to any infectious disease is not achievable with vaccinations. Permanent immunity is ONLY achieved if there is exposure to – and at least a subclinical infection from – a wild-type virus or bacteria! Indeed, vaccinations can only cause short-lasting, partial immunity – hence the need for periodic booster shots for most vaccines to even achieve partial immunity. There are two essential realities that must go together if a person is to obtain full and long-lasting immunity to any infectious disease.

    These two essential factors are

    1) cellular (aka mucosal) immunity, which only occurs if and when the nasal or respiratory mucosa (or bowel mucosa) is exposed to a virus or bacteria (which never happens with an intramuscularly injectable vaccine!) and

    2) serological (aka humeral) immunity, which only occurs when the mucosal barrier is breached by the viral or bacterial antigen and the antigen gets into the bloodstream and comes in contact with the immunoglobulin-producing white blood cells.

    Thus intramuscular vaccinations can never induce cellular immunity, which may be the most important factor in human immune systems. In addition, intramuscular vaccinations cannot be expected to induce normal serological immunity because infectious diseases are never caused by intramuscular exposure. Any immunological effect will thus be of uncertain strength and duration.

    In addition, the intramuscularly-injected aluminum-adjuvanted vaccine or protein or DNA fragments are readily engulfed by phagocytes in the muscle and are capable of easily entering the central nervous system/brain (CNS) through the semi-permeable blood-brain barrier (which is more common in infants and children that adults)! Thus the brain can be poisoned with live viruses or toxic substances such as aluminum or mercury.

    The aluminum adjuvant is also known to form immune-stimulating fragments that can cause a hyper-immune response and therefore vaccine-induced autoimmune disorders, an increasingly common cause of chronic disorders in childhood.

    Why most physicians and patients have become so thoroughly convinced that vaccinations are effective is not just because of the massive propaganda from Big Pharma and Big Medicine that repeatedly supports that notion, but also because of the relative rarity of the infectious diseases that the vaccines allegedly prevent. See the list below for a multitude of examples regarding that reality.

    As just one example of the uselessness of vaccinating all pediatric patients with, for example, a mumps vaccine, is the fact that in the United States, only 6,000 cases of mumps were reported annually in recent years, most cases of which were in vaccinated individuals, which equates to the exceedingly rare incidence of 3 cases per 100,000 population! And yet the CDC and the AAP (American Academy of Pediatrics) mandate several doses of the live mumps virus-containing MMR vaccine for every pre-school child in America. Which means that for every child partially protected from the benign parotid gland infection there will be tens of thousands of children that will be unnecessarily vaccinated. Those patients will receive no benefit, will have to pay the substantial fees, will be unnecessarily exposed to the many toxic ingredients of the vaccine and will be at risk of developing a vaccine-induced autoimmune disorder that could last a life-time.

    A second example is the aluminum-adjuvanted Pneumovax shot and the fact that as few as 2 cases of invasive pneumococcal pneumonia occur annually in the US per 100,000 population. That means that 99.99% of the patients getting the Pneumovax shot will get no benefit but will also be at risk of suffering the considerable adverse effects from the neurotoxic aluminum. In addition, there are many strains of pneumococcal bacteria that are not targeted in the vaccine.

    Other examples abound (see further below).

    Would any rational person, whose physician did his duty and fully informed his patient about the risks (as physicians are supposed to do), accept the expense and the risks of being injected with aluminum-containing vaccines if the risk of getting pneumococcal pneumonia was so extremely low?

    Here are some sobering statistics that should give pause to anybody considering exposing themselves to unnecessary toxins for little or no benefit.

    Commonly-mandated Childhood Vaccines and the Incidence of the Diseases they are Supposed to Prevent

    DTaP: Diphtheria is non-existent in the US population
    DTaP: Tetanus is rare in the US population

    Pertussis (Bordetella pertussis – aka “whooping cough”) has an incidence of 55.2 cases per 100,000 infants less than 12 months of age; (98.2 cases per 100,000 6 month-old infants or younger).

    The incidence of pertussis has actually been gradually increasing since the early 1980s. A total of 25,827 cases was reported in 2004, the largest number since 1959. The reasons for the increase are not clear. A total of 27,550 pertussis cases and 27 pertussis-related deaths were reported in 2010. Case counts for 2012 have surpassed 2010, with 48,277 pertussis cases, with 13 deaths in infants (provisional).

    During 2001–2003, the highest average annual pertussis incidence was among infants younger than 1 year of age (55.2 cases per 100,000 population), and particularly among children younger than 6 months of age (98.2 per 100,000 population). In 2002, 24% of all reported cases were in this age group. However, in recent years, adolescents (11–18 years of age) and adults (19 years and older) have accounted for an increasing proportion of cases. During 2001–2003, the annual incidence of pertussis among persons aged 10–19 years increased from 5.5 per 100,000 in 2001, to 6.7 per 100,000 in 2002, and 10.9 per 100,000 in 2003.

    Hepatitis B

    Hepatitis B vaccine is a synthetic, non-infectious vaccine. The incidence of Hepatitis B is 2.1 cases per 100,000 population. The vaccine used to contain thimerosal (mercury) as a preservativeand now contains aluminum as an adjuvant.

    Based on data from CDC, the incidence of acute hepatitis B in the United States has declined steadily since the late 1980s. Between 1987 and 2004, the incidence of acute hepatitis B was recently reported by the CDC to be 2.1 per 100,000(6,212 cases reported).


    As few as 2 cases of invasive pneumococcal pneumonia occur annually per 100,000 population. It contains an aluminum adjuvant.

    CDC reported dramatic declines in invasive pneumococcal disease among children less than 5 years old. Overall, invasive pneumococcal disease decreased from 100 cases per 100,000 people in 1998 to 9 cases per 100,000 in 2015. Invasive pneumococcal disease caused by the 13 serotypes covered by PCV13 decreased from 91 cases per 100,000 people in 1998 to 2 cases per 100,000people in 2015.

    Hemophilus influenza b (Hib) vaccine

    The incidence of Hib infection is as low as 0.08 cases per 100,000 in children younger than 5 years of age.

    In the United States, Hib disease is uncommon. In 2015, the incidence of invasive Hib disease was 0.08 cases per 100,000 in children younger than 5 years of age. It occurs primarily in under-immunized children and in infants too young to have completed the primary immunization series.

    In 2015, the incidence of non-b H. influenzae invasive disease was 1.3 per 100,000 in children younger than 5 years of age.

    Non-typeable H. influenzae, for which there is no vaccine, now causes the majority of invasive H. influenzae disease in all age groups. In 2015, the incidence of invasive non-typeable H. influenzae disease was 7 cases per 100,000 in children younger than 5 years of age and 2 cases per 100,000 in adults 65 years of age and older.

    MMR (Measles)

    The MMR vaccine contains live (although allegedly attenuated) viruses and therefore contains no mercury. In the US, the incidence of measles is approximately 2 cases per million population.

    The incidence of measles has remained below one case per million since 1997, except in 2014, when 667 measles cases were reported, representing a reported incidence of 2.08 cases per million.

    MMR (Mumps)

    In the US, the incidence of mumps is less than 3 cases per 100,000 population.

    In the United States, approximately 6,000 cases of mumps were reported annually in recent years (3 cases per 100,000 population).

    MMR (Rubella)

    In the US, the incidence of rubella (German measles) is less than 0.5 cases per 100,000 population.

    The largest annual number of cases of rubella in the United States was in 1969, when 58 cases were reported per 100,000 population. In 1983, fewer than 1,000 cases per year were reported in the United States (less than 0.5 cases per 100,000 population).

    Varicella (Chicken Pox)

    The chicken pox vaccine is a live virus vaccine. The incidence of wild-type chicken pox is highly variable and not reportable.


    Flu viruses have 100 – 200 different strains and therefore influenza has an unpredictable and variable incidence. 80% of what is commonly diagnosed as “vaccine-preventable” influenza is actually “Influenza-Like Illnesses” (ILI) for which there is no vaccine. The commonly over-promoted annual influenza vaccines that come in multiple-dose vials contain the neurotoxic preservative mercury (thimerosal).

    Neurotoxic aluminum adjuvants hyper-stimulate immune responses to whatever protein molecules (look up the critically important concept of “Molecular Mimicry”) come to be attached, explaining the large number of vaccine-induced autoimmune (hyperimmune) disorders that are increasingly occurring in fully-vaccinated populations.

    Aluminum adjuvants are used in the following vaccines:

    DTaP (diphtheria/Tetanus/ Pertussis (whooping cough);
    Hepatitis A;
    Hepatitis B;
    Haemophilus influenza type b;
    Meningococcus; and
    Pneumococcal vaccines.

    Dr. Kohls is a retired family physician from Duluth, MN, USA. Since his retirement from his holistic mental health practice he has been writing his weekly Duty to Warn column for the Duluth Reader, northeast Minnesota’s alternative newsweekly magazine. His columns, which are re-published around the world, deal with the dangers of American fascism, corporatism, militarism, racism, malnutrition, Big Pharma’s over-drugging and Big Vaccine’s over-vaccination agendas, as well as other movements that threaten human health, the environment, democracy, civility and the sustainability of all life on earth. Many of his columns have been archived at a number of websites, including;; and

    The original source of this article is Global Research
    Copyright © Dr. Gary G. Kohls, Global Research, 2018
    My website:

    "No one is useless in this world who lightens the burdens of another.” ~ Charles Dickens

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