Drug Overdose Is Now The LEADING Cause Of Death For Americans Under 50… Big Pharma’s Opioid Death Machine Marches on

Source: NaturalNews.com
Vicki Batts
June 10, 2017

The drug epidemic plaguing the United States seems to only get worse as time trudges on. Deputy Attorney General Rod Rosenstein announced recently that drug overdose is now the leading cause of death for American adults under the age of 50.

At the helm of this devastating surge in drug-related deaths are, of course, opioids. Opioids are a class of drugs that includes heroin, fentanyl and many legal prescription painkillers such as oxycodone and hydrocodone. According to the CDC, oxycodone, hydrocodone and methadone are the most common prescription drugs used in overdose deaths. The agency reports that at least 1 out of every 4 people prescribed an opioid is estimated to struggle with addiction, and that emergency rooms are treating over 1,000 people who have misused an opioid every day.

During his announcement, Rosenstein stated that fentanyl — a synthetic opioid — is becoming increasingly problematic, in large part due to its extreme potency. “Fentanyl is especially dangerous. It is 40 to 50 times more deadly than heroin. Just two milligrams, a few grains of salt, an amount you could fit on the tip of your finger, can be lethal. Fentanyl exposure can injure or kill innocent law enforcement officers and first responders. Inhaling a few airborne particles can have dramatic effects,” he explained.

NPR reports that approximately 75 percent of people who died from an accidental overdose in 2016 had fentanyl in their systems. One of the biggest threats posed by fentanyl is that other drugs are often cut with it, meaning that users may not be aware of the potential danger.

While loath to admit it, one of the driving factors behind this heartbreaking epidemic is indeed prescription opioid use. Not only are the prescription drugs themselves contributing to the massive death toll, they are indirectly increasing the number of people who use street drugs like heroin. The National Institute on Drug Abuse reports that an estimated 80 percent of heroin users started out using prescription pain-killers.

In other words, opioid pain-killers are not just responsible for the deaths of people who overdose on a prescription drug, they are also responsible for the deaths of an overwhelming majority of heroin users.

As Amy Goodman from Democracy Now! reports, it’s been estimated that a staggering 52,000 people died from a drug overdose in 2015 — and over half of those deaths were related to opioid pain medications, heroin or fentanyl. Goodman explains further, “To put the death toll in perspective, opioid deaths have surpassed the peak in death by car crash in 1972, AIDS deaths in 1995 and gun deaths in 1993. After 20 years of heavy combat in South Vietnam, U.S. military casualties represented only one-third of the death toll from 10 years of opioid overdoses.”

ASAM.org breaks it down even further, noting that while 12,990 of overdose deaths were related to heroin, a shocking 20,101 overdose deaths were related to prescription opioids.

To put it simply, prescription opioids are, without a doubt, a driving force behind the rising rates of drug addiction and overdose in the US. Several US states, as well as cities and counties, have brought the Big Pharma corporations responsible for these drugs to court for their involvement in creating this outbreak of addiction. For example, the state of Ohio recently launched a lawsuit against several pharmaceutical companies for purporting that the drugs had benefits unsupported by science, promoting fraudulent information and misleading patients.

Opioids are extremely dangerous drugs; even Pfizer has admitted that they carry a substantial risk for addiction when used “properly.”

While it’s clear that the opioid epidemic will sadly not be ending anytime soon, hopefully more states will continue to take action against Big Pharma. Keep up with the latest stories about drugs and drug-makers at DangerousMedicine.com.

Sources: 

Breitbart.com

CDC.gov

NPR.org

DrugAbuse.gov

DemocracyNow.org

ASAM.org [PDF]
Read More at: NaturalNews.com

Whopping Vaccine Injury Payouts for US Fiscal Year 2017 Released

Source: WakingTimes.com
Brendan D. Murphy
May 9, 2017

Yet another shocking blow has been delivered to people who still ardently claim that vaccines are “safe and effective,” and that the only complications they can cause are “mild.” The US government department for Health Resources and Services Administration has recently released the running tally of the just-past-half-way-complete US Fiscal Year (FY) of 2017 for compensable vaccine injuries. It currently stands at over $142 million dollars. You read that right. That covers the 377 cases that were thus far successful in obtaining compensation in fiscal year 2017 through the heavily biased (to put it politely) system allegedly in place to redress damage done by vaccines in the USA.

At the rate things are going, we might expect the Vaccine Injury Compensation Program to pay out around $220 million or more by the close of FY 2017. To clarify, US Fiscal Year 2017 runs from October 1st, 2016 to September 30th, 2017 – there’s still over four months remaining to rack up more carnage.

Screenshot source: http://www.hrsa.gov/vaccinecompensation/data/monthlywebsitestats04_01_17.pdf

The National Childhood Vaccine Injury Act of 1986 was created to “reduce liability and respond to public health concerns.” It granted immunity to pharmaceutical companies and prevented parents from suing vaccine makers for vaccine injuries or death. What other industry has such exceptional standards applied to it? Why the special privilege a.k.a. license to injure and kill with impunity?

According to the CDC’s website, there are “limitations in our knowledge of the risks associated with vaccines” and vaccinations have “the following problems”:

1. Limited understanding of biological processes that underlie adverse events
2. Incomplete and inconsistent information from individual reports
3. Poorly constructed research studies (not enough people enrolled for the period of time)
4. Inadequate systems to track vaccine side effects
5. Few experimental studies were published in the medical literature.”¹ (emphasis added)

The above very revealing admissions from the US Centers for Disease Control (CDC) completely undercut the pathological overconfidence exhibited in the extreme portions of the community pushing for mandatory vaccination.

Similarly, the Vaccine Injury Compensation Program compensation numbers are, not only not reassuring, but, frankly astonishing, and should give not just all parents, but all people in general, serious pause. If vaccines are “safe and effective” as our medical practitioners and politicians constantly tell us via mainstream media outlets, then why are there already over 370 compensated cases in fiscal year 2017? Why is there a running payout total from 1988 up to now of “around $3.6 billion,” according to the US Health Resources and Services Administration?

Why, if vaccines are just so gosh darned safe, does the HRSA government website state (see image above) that, “Since influenza vaccines (vaccines administered to large numbers of adults each year) were added to the VICP in 2005, many adult petitions related to that vaccine have been filed, thus changing the proportion of children to adults receiving compensation”?²

It seems to make some sense that the true purpose of the Vaccine Injury Compensation Program is simply to pay lip service to justice and decency, while allowing pharmaceutical companies to receive a minor slap on the wrist (largely in the form of bad PR) before they go right on with business as usual – “pay to play” or something like that (but then I’m a cynic.). The economic losses are affordable and “worth it”; the human losses are an inconvenient public relations issue to be “managed.”

So Many Questions, So Few Answers

Why, if “many” fully grown adults are seeking injury compensation should we make the blanket assumption that these same vaccines will be “safe and effective” for babies and small children? The doses are not weight adjusted. No vaccines are weight adjusted to account for the much smaller and more fragile physiology of a baby. Why? Why does a baby receive the same amount of heavy metals, carcinogens, and the many other toxic ingredients (such as polysorbate-80) that a full grown 200 pound man receives? Where else in medicine is such a lack of dose control not only tolerated, by blindly promoted and held as sacred?

Why are we not seeing any double-blind randomized controlled trials with true placebo groups demonstrating clearly and honestly that flu (or other) vaccines are safe and not causing children any harm – as well as being “effective”? Until 2005, based on the HRSA document, the ONLY petitions filed for flu vaccine injuries were on behalf of injured children. Where are those safety studies again? Where are the weight adjusted doses again? Why isn’t anyone taking up RFK Jr’s $100,000 mercury challenge if mercury-containing vaccines are so demonstrably safe? Why, why, why, Mr Anderson?

A recent peer-reviewed study published in the Pace Environmental Law Review looked at cases of vaccine injury that have been monetarily compensated by the VICP.

The study investigated approximately 1300 cases of childhood brain injury as a result of vaccines in which the Special Masters ruled for the plaintiffs, looking for references to autism, symptoms of autism or disorders commonly associated with autism. It reports that twenty-one cases actually stated “autism or autism-like symptoms” in the court records.  The researchers then identified and contacted 150 more compensated families to find out whether the children had autism.  They were able to find an additional 62 cases (greater than 40% of their sample) for a total of 83 cases of autism.  In 39 cases (47%) there was confirmation of autism beyond parental report.³ (Emphasis added. Autism is a proven vaccine adverse event. It is also listed in vaccine inserts as one of many possible abreactions.)

Since 1988, when the Vaccine Injury Compensation Program began, 5,353 petitions were assessed as compensable out of the 18,072 filed since then. Nearly 1-in-3 is actually fairly impressive, given the incredible medical, social, and legal bias against recognizing vaccine harm when it occurs, as well as the determined efforts by pharmaceutical companies in court to distort reality and manufacture false doubt in defending their products and controlling perception.

This doesn’t look good at a time when proponents of removing freedom of health choice are campaigning for “no jab no fly” policies that would prevent much of Australia from functioning (particularly economically). This fear-mongering and vaccine hysteria is all the more absurd when one pauses to consider that in Australia, as in the US, the clear majority of adults are FAR from being “up to date” with their shots – and have been for decades. We simply don’t worry about it. And yet, the much-feared epidemics never seem to materialize. In fact, most outbreaks seem to follow in the wake of intensive vaccination campaigns – but that’s just a coincidence, right? Just as it’s a coincidence that within hours of getting your baby home from the doctor’s surgery they were seizing, turning blue, and in the nascent stages of encephalopathy…Right?

Because clearly, after $3.6 billion dollars worth of legal payouts in the US alone since 1988 – and with adverse events being under-reported (in the VAERS) to the extent of 90% or more, and with mature adults and children alike being injured by flu (and the other) vaccines to the extent of requiring compensation, clearly, vaccines are simply “safe and effective.”

Logically, if we mandated vaccination across the board, the only possible outcome is an explosion of vaccine injuries and people seeking compensation. It’s simple math. More vaccines means more vaccine injuries and deaths. Aside from the immeasurable human psychological cost and loss of quality of life, who is going to fund the payouts? Is Big Pharma stepping up to the plate and preparing to own the harm it is causing? Not likely, since pharmaceutical companies are legally immune (at least in America). Vaccine Injury Compensation Program funding comes from an excise tax charged on each vaccine:

Vaccine Injury claims are paid from the Vaccine Injury Compensation Trust Fund, managed by the U.S. Department of Treasury.

The [VICP] Trust Fund receives its money from a 75 cent excise tax on vaccines recommended by the [CDC] for routine administration to children. The excise tax is imposed on each dose, or preventable disease of a given vaccination. (central-pennsylvania.legalexaminer.com)

This reminds me of the carbon tax, which essentially allows “polluters” to simply pay a tax/”penalty” for their emissions and continue with business as usual. It isn’t a deterrent at all for vaccine manufacturers. They would factor it in to their costs of operating.

Disturbing Changes

In September 2014, the CDC notified federal vaccine advisory committees that soon they will no longer be accepting vaccine adverse event reports via phone, fax, or mail. Instead, officials have stated that they will only accept electronic reports of vaccine reactions, injuries, hospitalizations, and death. (vactruth.com)

According to VacTruth, “70 percent of VAERS reports are still filed the old-fashioned way, handwritten and submitted via mail or fax. A mere 30 percent of adverse event reports are submitted to VAERS online.”⁴ Therefore, the change to adverse event reporting seems designed to make it harder to keep accurate tabs on the true number of significant vaccine injuries by discouraging reporting them in general. Some parents dealing with a severe abreaction in a child may also be too overwhelmed and distressed to have the time or inner resources to file a report, a fact few people even consider. Other factors make obtaining compensation even harder:

…certain adverse reactions from vaccines have been removed from the injury tables, including encephalopathy (swelling of the brain) and seizure disorders resulting from specific vaccines, two very common adverse reactions…and autism as a primary injury. Injuries from anthrax and smallpox vaccines are not covered under the NVICP…Parents who file a report with VAERS must file a separate report if they wish to seek compensation for their child’s vaccine injury or death. Furthermore, if your child was hospitalized from a vaccine, but they did not require surgery, you would not be able to file a claim seeking compensation, unless you can prove with certain kinds of evidence that the effects of the injury have lasted longer than six months.⁵

You also need an attorney to file on your behalf. And did you know that injury claims may take from two to ten years to resolve through the VICP? Imagine being a bereaved parent and pondering that life-sucking prospect. The system is very clearly weighted against any kind of justice for vaccine-injured people. This is why I say that nearly 1-in-3 cases receiving compensation so far is actually quite an achievement – all things considered.

You may support blanket vaccination on the way IN to the doctor’s surgery, but you may not support it so much when your child is brain-dead (or just dead) 72 hours later. It happens. I personally know many vaccine-injured people – so many I’ve lost count. My partner is one (thank you very much, Gardasil). The media hides it. Politicians lie about it. Doctors parrot fallacious medical dogmas without thinking. Big Pharma continues doing what Big Pharma does best: poisoning us while we pay them for the privilege.

The x-factor is YOU, the wild card, the ghost in the machine, the one who can stop, think, and say “NO.” You have the power to recognise something that doesn’t make sense and to try a different way – and if you have children then, more to the point, you have the responsibility.

Next fiscal year, let’s aim for $0 in compensation payouts through 100% non-compliance – meaning no vaccine injuries and deaths at all – and a public that understands REAL disease risk and how to actually be resistant and robust rationally. Wouldn’t that be something?

Read More At: WakingTimes.com

---

Endnotes

1. http://www.cdc.gov/vaccinesafety/Vaccine_Monitoring/history.html
2. https://www.hrsa.gov/vaccinecompensation/data/monthlywebsitestats04_01_17.pdf
3. http://www.prnewswire.com/news-releases/83-cases-of-autism-associated-with-childhood-vaccine-injury-compensated-in-federal-vaccine-court-121570673.html
4. http://vactruth.com/2015/02/19/vaccine-injury-compensation/?utm_source=The+Vaccine+Truth+Newsletter&utm_campaign=080e55aa44-02_19_2015_vaers&utm_medium=email&utm_term=0_ce7860ee83-080e55aa44-408191918
5. Ibid.

About the Author

Brendan D. Murphy – Co-founder of Global Freedom Movement and host of GFM Radio, Brendan D. Murphy is a leading Australian author, researcher, activist, and musician. His acclaimed non-fiction epic The Grand Illusion: A Synthesis of Science & Spirituality – Book 1 is out now! Come and get your mind blown at www.brendandmurphy.net

“What a wonderful job of collating and integrating you have done! Every person in the field of ‘paranormal’ psychology or related topics should have this book as a major reference.” – Dr. Buryl Payne

“A masterpiece…The Grand Illusion is mind-blowing.” – Sol Luckman, author of Potentiate Your DNA.

“You’ve written the best synthesis of modern science and esoteric science that I’ve seen in 40 years of study in that area. Brilliant!”  – Michael K. Wade

Please visit – www.globalfreedommovement.org

American Academy of Pediatrics declares “no science” needed to prove vaccines are safe, because they BELIEVE

Source: JeremyHammond.com
Jeremy Hammond
May 7, 2017

When asked whether it could provide studies to support specific claims it made about vaccine safety, the American Academy of Pediatrics ultimately declined.

On January 10, 2017, the American Academy of Pediatrics (AAP) issued a press release to express its opposition to a federal commission that has been proposed by the Trump administration to examine vaccine safety and efficacy. The AAP argues that since we already know that vaccines are safe and effective, therefore there is no need for further examination into their safety and efficacy.

This argument, however, begs the question — it presumes in the premise the proposition to be proven (the petitio principii fallacy). And the press release itself illustrates why, apart from the question of whether there should be a federal commission, critical examination of public vaccine policy is very much warranted.

In its press release, among other things, the AAP stated that:

• Vaccines prevent cancer.
• Claims that vaccines are linked to autism “have been disproven by a robust body of medical literature”.
• Claims that vaccines “are unsafe when administered according to the [CDC’s] recommended schedule” have likewise “been disproven by a robust body of medical literature”.

According to the AAP, its own claims are backed by solid science. Yet when asked whether it could provide citations from the medical literature to support its claims, the AAP first failed to do so, then essentially offered a “No comment” when pressed for a comment about its failure to do so.

With respect to the claim that vaccines prevent some forms of cancer, the AAP was asked:

• Can you please direct me to any studies in the peer-reviewed medical literature showing any vaccine prevents cancer?

With respect to the other two, the AAP was asked the following questions:

• Can you please direct me to the studies you are referring to in this body of literature that took into account the possibility of a genetically susceptible subpopulation?
• Can you please point me to the studies in this body of literature that have compared health outcomes, including but not limited to developmental regression (i.e., autism), for children who’ve receive the CDC’s full schedule of vaccinations with children who’ve remained completely unvaccinated?

An initial email to the AAP containing these questions went unanswered.

The email was followed up with a phone call. Lisa Black, the AAP’s Media Relations Manager, assured that she would get back with answers to the questions. In a subsequent email, Ms. Black replied, “Please see information that AAP has posted for parents on this page”, which was followed by a link to a list of studies on the website HealthyChildren.org.

However, none of the listed studies on that page supports the AAP’s claim that “vaccines prevent … forms of cancer”.

None apparently considered the possibility of a susceptible subpopulation with a genetic susceptibility to adverse reactions to vaccines.

And none compared health outcomes of fully vaccinated children with completely unvaccinated children.

The list provided does contain numerous studies finding no association between vaccines and autism, but even the listed safety review by the Institute of Medicine (IOM) doesn’t go so far as to say that the hypothesis has been “disproven”.

On the contrary, the IOM acknowledges that it is biologically plausible that vaccines might cause autism in a genetically susceptible subpopulation, but characterizes this hypothesis is still “speculative” and “unsubstantiated”.

That is a world apart from saying it has been “disproven”.

One would think that the IOM’s conclusion, if its inquiry was a scientific one, would be that since this is such an important question and this specific hypothesis is plausible and not well studied, therefore there should be further study into this question of whether vaccines could trigger autism at least in some children with a genetic predisposition to vaccine injury.

But rather than calling for more research into this area, the IOM actually advocated that no further studies to test this hypothesis be done. Its stated reason for this was partly medical, but at least equally political — and certainly favorable to the profits of the pharmaceutical industry. The IOM’s reason was:

Using an unsubstantiated hypothesis to question the safety of vaccination and the ethical behavior of those governmental agencies and scientists who advocate for vaccination could lead to widespread rejection of vaccines and inevitable increases in incidences of serious infectious diseases like measles, whooping cough, and Hib bacterial meningitis.

In other words, since studying this hypothesis further would undermine public vaccine policy with its one-size-fits-all approach to disease prevention, therefore no further research to test the biologically plausible hypothesis should be done.

The AAP was sent a follow up email noting that none of the studies listed appeared to support the claims it made in the press release. The AAP was welcomed to correct the record, but did not dispute the observation that none of the studies listed showed that vaccines can prevent cancer, considered genetic susceptibility to vaccine injury, or compared health outcomes for vaccinated and unvaccinated children.

The additional follow up questions were also asked:

• If the AAP cannot produce one or more studies that considered the possibility of a genetically susceptible subpopulation, how can it claim that any association between vaccines and autism has been “disproven”?
• If the AAP cannot produce one or more studies that compared health outcomes between children vaccinated according to the CDC’s schedule and children who remained unvaccinated, how can it claim that any association between vaccines and autism has been “disproven”?

The AAP did not reply via email to the follow up questions.

In a second phone call requesting the AAP to produce such studies to support its claims, Ms. Black replied that she had provided everything the AAP was going to provide.

When confronted with the observation that none of the studies provided supported the AAP’s claim that vaccines can prevent cancer, she repeated that the AAP was not going to provide any additional information.

When asked whether the authors of the press release, AAP President Fernando Stein and Executive Vice President Karen Remley, would like to comment, Ms. Black abruptly ended the phone call by saying she was going to hang up and then doing so.

Questions Unanswered

The questions seem pertinent, particularly given the fact that the government has acknowledged that vaccines can cause brain damage resulting in developmental regression.

In 2008, then director of the CDC Julie Gerberding offered the following carefully worded acknowledgment:

Now, we all know that vaccines can occasionally cause fevers in kids. So if a child was immunized, got a fever, had other complications from the vaccines. And if you’re predisposed with a mitochondrial disorder, it can certainly set off some damage. Some of the symptoms can be symptoms that have characteristics of autism.

The context in which she was speaking was with respect to Hannah Poling, a child with a mitochondrial disorder who developed autism after receiving numerous vaccines on the same day and whose family was awarded compensation under the National Vaccine Injury Compensation Program (VICP).

The VICP was established in the mid-1980s under a law that granted broad legal immunity to vaccine manufacturers. The government’s reason for doing so was that vaccine injury lawsuits were threatening to undermine public policy by putting vaccine manufacturers out of business.

The Supreme Court has upheld that legal immunity on the grounds that certain adverse reactions are “unavoidable” and “design defects” are “not a basis for liability.”

Around the same time as Gerberding’s admission, a former director of the National Institutes of Health, the late Bernadine Healy, criticized the refrain that any link between vaccines and autism has been debunked. She pointed out the kinds of studies that would be necessary in order to confidently draw that conclusion hadn’t yet been done.

Specifically, she noted the lack of studies taking into consideration a genetically susceptible subpopulation.

Ms. Healy also slammed the IOM for advocating that no further research be done and noted that as a potential cause of autism, “vaccines carry a ring of both historical and biological plausibility”.

Similarly, in contrast to the AAP’s claim that any association between vaccines and autism has been “disproven”, one of the CDC’s lead researchers on that very question, CDC Director of Immunization Safety Dr. Frank DeStefano, admitted in an interview in 2014 that “it’s a possibility” that vaccines could trigger autism in genetically susceptible individuals.

“It’s hard to predict who those children might be”, DeStefano observed, and trying to determine what underling conditions put children at risk of vaccine injury is “very difficult to do”.

Acknowledging the lack of studies in this area, he added that, “if we ever get to that point, then that kind of research might be fruitful.”

The AAP’s list of studies includes one or more for which DeStefano was an author.

The CDC also admits the need for further study in this area. Its website at the time of this writing acknowledges that “More research is needed to determine if there are rare cases where underlying mitochondrial disorders are triggered by anything related to vaccines.”

So how can the AAP claim that any association between vaccines and autism has been “disproven” when the studies that would be necessary to invalidate the hypothesis haven’t been done?

No comment.

That’s the AAP’s answer to the question, anyway.

The AAP’s attitude should perhaps come as no surprise, given its close relationship with the vaccine industry.

As CBS News reported in 2008, “The vaccine industry gives millions to the Academy of Pediatrics for conferences, grants, medical education classes and even helped build their headquarters.”

A Discussion to Be Had

The AAP argues in its press release against the formation of a federal commission, but its argument would apply to any public debate about the safety and efficacy of vaccines. By the AAP’s logic, like the IOM’s, also unnecessary are any discussion about it in the media and any further scientific inquiry.

But as Daniel Sarewitz observes, “as science approaches the cutting edge, it tends to raise as many questions as it resolves, so there is always room for debate about what the science is actually saying.”

Parents dubbed “anti-science” by the media are naturally curious why that label doesn’t seem to apply to those calling for no further inquiry into pertinent questions.

Parents aren’t just asking legitimate questions about vaccines. They’re doing what most doctors haven’t and spending a lot of time researching vaccines themselves. And they’re not just going to “anti-vaccine” websites to research it. They’re organizing, sharing information, and digging into the medical literature for themselves.

Parents can see the fundamental contradiction between public health officials and the media constantly insisting that vaccines are harmless even while the government grants legal immunity to the vaccine manufacturers on the grounds that vaccines are unavoidably unsafe and while the government manages a Vaccine Injury Compensation Program in order to shift the costs for damages and keep the vaccine manufacturers profitable — all to maintain public policy.

Parents understand how government and industry funding influences the direction and findings of scientific research, and how the medical establishment that has given us soaring costs and a population in which nearly 40 percent are chronically ill will tend to justify itself despite its abysmal performance and a long history of being wrong time and again, from tobacco science (older generations may remember how the industry used to get product endorsements from doctors) to the USDA recommended high-carb diet (which has contributed to the obesity epidemic and is more about satisfying food industry lobbyists than providing science-based advise) to the role of cholesterol in heart disease (scientific research no longer supports the hypothesis that dietary cholesterol contributes to blood cholesterol and heart disease risk).

Parents are aware of how government agencies like the FDA and the CDC serve the financial interests of the pharmaceutical industry. They see the corruption and the “revolving door” of Washington, such as how Julie Gerberding left her government job pushing vaccines as head of CDC to become president of the vaccine division for the pharmaceutical giant Merck.

They see how the AAP, too, has an incestuous relationship with “Big Pharma”. They understand how willful ignorance goes beyond the individual operating within the system and becomes institutionalized. And they watch as an organization that influences how their child’s pediatrician practices medicine accepts money from an industry they feel the AAP ought to be protecting them from.

They can witness how the AAP makes statements it claims are solidly backed by science, but which it is unwilling or unable to provide any studies to support. They understand that the truly “anti-science” position is the one that says no further scientific inquiry into an admittedly biologically plausible hypothesis is necessary.

Parents know there are many studies that have found no association between vaccines and autism. They don’t need the AAP to point this out to them. But they wonder why the AAP ignores all the studies that do support the hypothesis.

They wonder how the AAP can claim that the vaccine-autism hypothesis has been “disproven” when the most any of the studies it cites have concluded is that those particular studies, with their own particular focus, designed around their own particular assumptions, using a particular methodology, did not find an association between vaccines and autism.

And parents are asking questions like: What was the actual purpose of the study? What were the underlying assumptions made by the authors? What vaccines were being studied, and what outcomes? Who were the study groups? What were the criteria for their selection? What was the study’s methodology? What are its strengths and weaknesses? Do the conclusions drawn follow from the actual findings? How conclusive is it? What does the study actually prove, if anything?

Parents can see for themselves the huge disparity between what they are told science has to say about vaccines  — by public health officials, the medical establishment, and the mainstream media — and what science actually has to say about it.

The parents who are choosing not to vaccinate their children aren’t doing so because they are uneducated or unintelligent. On the contrary, studies show that they tend to be wealthier and more highly educated than the general population.

They aren’t choosing not to vaccinate because they are ignorant of the science. They are choosing not to vaccinate because they are digging into the medical literature (which can be searched via PubMed.gov) and awakening to the deceit they see coming out of the government and the mainstream media.

They see how mainstream journalists, rather than seriously investigating what the science actually says, rely on statements from agencies like the CDC and industry-funded organizations like the AAP to “inform” the public about the subject.

They see how the establishment is seeking to stifle debate not by respectfully addressing their legitimate questions, but by bullying them into silence and conformity, and they understand how such a phenomenon can arise because institutions with a life of their own feel threatened by the truth and act to preserve the status quo.

The AAP and other actors interested in preserving the public vaccine policy so far seem to have assumed that they can end the discussion by declaring authoritatively that there is no need for further discussion.

But if they ever hope to truly end the discussion, they are going to have to start taking parents’ concerns seriously and answering their legitimate questions with more than disingenuous public relations talking points that might as well have been written by the vaccine industry.

Read More At: NaturalNews.com

Why Isn’t There A Medical Snowden?

Source: NoMoreFakeNews.com | JonRappoport.wordpress.com
By: Jon Rappoport
May 5, 2017

The US press is aware that medically caused death is the third leading cause of death in America. But nothing happens in their elite corner of the “information age.”

For years, I’ve been pointing out that the medical apparatus is best-protected structure in the US and the world.

One piece of evidence for that statement: we haven’t had, symbolically speaking, a medical Edward Snowden. Indeed, if you go to WikiLeaks or some other source that routinely exposes leaks, you’ll be hard pressed to find anything substantial about the inner workings of what I call the medical cartel.

And when I say inner workings, I mean memos, emails, and other documents that irrevocably reveal:

* How medical studies are routinely twisted and cooked to achieve a predetermined outcome in contradiction to the facts;

* How virus-hunters casually claim to have discovered “the virus” that causes a disease, when they have not followed standard procedure, and are merely making insupportable and self-serving assumptions;

* How researchers ignore evidence that a “new disease” is indistinguishable from an old disease that has been on the scene for decades or even longer; there is money in new diseases;

* How medical drugs are having grave toxic effects on patients and delivering no visible results;

* How government health officials are conspiring with drug companies to bring medicines to market, despite the fact that there is every reason to assume the drugs are worthless and destructive;

* How public health agencies, researchers, and pharmaceutical companies cover up the widespread harm vaccines are causing;

* How fake epidemics are launched to convince the public that they must follow prescribed vaccination schedules.

These are just a few of the many issues we would expect an insider to expose in blowing the whistle. We would expect to see these issues (crimes) revealed in numerous and detailed and irrefutable paper trails.

What the CDC whistleblower, William Thompson, exposed in 2014 (see the film Vaxxed) mainly concerned one study that falsely exonerated one vaccine (the MMR) from a role in causing autism. That is just the tip of the iceberg.

Over the years, I’ve gone after the medical cartel from many angles. There is a surprising amount of open-source material. I have also interviewed medical “dissidents,” doctors who have left the fold and are ready to talk. And using straightforward logic, I’ve discovered deep flaws in spurious medical arguments, and those flaws have led to deeper flaws and lies.

I could easily do a week-long course for honest and independent medical reporters on what I’ve found and how I’ve found it. Connecting the dots often requires a prior knowledge of basic fallacies in the medical framework of “knowledge.”

I have never encountered a medical insider who had access to miles and miles of damning data and was prepared to release it to the world.

Understand: I’m NOT talking about practicing physicians who are willing to talk about medical lies. I’m talking about people who are buried deep in the heart of the pharmaceutical/government agency/research establishment, who are ready to step forward with documents that turn the establishment upside down, as a matter of duty to their various oaths.

This absence of deep insiders speaks to the wall that has been built around the medical cartel. We’re not just talking about insiders’ fear of going public. We’re talking about more. For example, the refusal of major media to cover deep revelations that threaten to torpedo the whole medical structure. A potential whistleblower pauses for thought in the face of that. He could risk everything, and then—silence from the press. No “Snowden coverage.” There would be unanimous press attacks on his person, accusations that the documents are forged or inconclusive, and he is mentally unbalanced. Accusations that he is preventing people from believing in a system that saves lives every day. And so on and so forth.

But that isn’t the end of it. The wall around the medical cartel is, in its origin, a Rockefeller wall. Modern medicine is a Rockefeller production, jump-started in the early 20th century with the famous Flexner Report. On the basis of the Report, medical systems devoted to discovering and treating disease were gradually transformed into a machine that routinely kills 225,000 Americans a year—and that is a conservative estimate.

Rockefeller influence is no small thing.

The march to include every human on the planet under the umbrella of modern diagnosis and treatment is relentless. It is part and parcel of an agenda to weaken, debilitate, confuse, control, and destroy populations. I do not make that statement lightly.

I have shown, in past investigations, that medical-cartel players are surely aware of the damaging effects of their drugs, and yet, for decades, they have stood by and done nothing. The profit motive is one thing; but this is, at the least, indifference to human suffering and death. You could call it reckless endangerment, negligent homicide, but these are euphemisms for assault with deadly weapons (the drugs) and murder.

You could say the reason medical insiders do not step forward and reveal key data is fear for their own lives; but this is true of whistleblowers in other professions who do step forward.

Suppose Edward Snowden, considering a plan to obtain and leak NSA data, felt strongly that the leaks would have no effect, that his revelations would be blacked out by the mainstream press, that no mainstream reporters would take his material and publish it?

Suppose there was no Glenn Greenwald to come to Snowden’s aid? Suppose the NSA had such a powerful propaganda arm that the public was utterly convinced the Agency was an angel with wings and was saving countless lives through its technology? Suppose, the public believed every act of NSA spying was comparable to doctors in an emergency room putting an accident victim back together after a car crash?

Snowden would have paused for thought. He would have wondered deeply about whether his leaks would have any effect at all.

Let me give you an example. For years, I have been writing articles about medically caused death in America. One of the key studies I’ve cited is decidedly mainstream. It was published on July 26, 2000, in the Journal of the American Medical Association. The author was Dr. Barbara Starfield, a revered and honored public health expert at the Johns Hopkins School of Public Health. Starfield concluded that the US medical system kills 225,000 Americans a year.

That would extrapolate to 2.25 MILLION deaths per decade.

Aside from a brief flurry of mainstream press articles that followed Dr. Starfield’s publication, in 2000, the press has been silent. My articles, which have been published at my site and other independent sites, have garnered no mainstream attention. Zero.

I’m not complaining. I’m merely pointing out the degree of mainstream censorship. The medical cartel has great influence.

A medical Edward Snowden, observing the media landscape, would have every reason to pause and consider his options. Why would he risk his reputation, his job, his paycheck, his future, his life, if the cartel he is exposing is so well protected that nothing would come of his bravery?

This is one reason why I write articles about the expanding power and influence of independent media. The day may come, and soon, when a medical Edward Snowden realizes he doesn’t have to find an editor at the New York Times who will look at his treasure trove of data and consider publishing it. Instead, he can pass along that data to any one of a hundred independent media operations and strike gold.

Or he can simply dump all the data on to a site he himself has created, comfortable in the knowledge that these same independent media sources will pick up the data, analyze it, and launch an unstoppable attack on the medical cartel.

Not one day’s coverage. A month, a year of coverage.

Operation Relentless Medical.

Then, the blind spot obscuring medical crimes will recede and vanish.

The public will no longer feel queasy about these revelations; the public will not feel they are witnessing a despicable attack on a wonderful messiah who has come to save the planet.

Eventually, the public will be able to make the distinction between emergency/crisis medicine, where competent and careful doctors (not sloppy and ignorant doctors) can save the lives of people who are lying on streets, after car wrecks, who need to be put back together—the public will be able to separate that from long-term fake medicine, where people are falsely diagnosed and drowned in toxic drugs which create a whole array of new symptoms which are then criminally diagnosed as new medical conditions, leading to the prescription of even more toxic drugs…all the way to the grave.

The public will understand how unnecessary and dangerous surgeries, and unnecessary and poisonous vaccines, are being foisted on them and those they love.

The public will understand. And will rise up.

This is not a pipe dream, if independent media continue to expand, and if they realize revelations of deep medical crimes are at least as important as exposures about the military industrial complex or the spying systems of national governments, or corporate pollution, or high-level money manipulation.

True medical insiders will step forward and reveal the secrets of the Temple.

I assure you, if we are alert, we are far more important and effective than “they” are.

A new day has dawned.

The sun is coming up.

Read More At: JonRappoport.wordpress.com
_______________________________________________________________

Jon Rappoport

The author of three explosive collections, THE MATRIX REVEALED, EXIT FROM THE MATRIX, and POWER OUTSIDE THE MATRIX, Jon was a candidate for a US Congressional seat in the 29^th District of California. He maintains a consulting practice for private clients, the purpose of which is the expansion of personal creative power. Nominated for a Pulitzer Prize, he has worked as an investigative reporter for 30 years, writing articles on politics, medicine, and health for CBS Healthwatch, LA Weekly, Spin Magazine, Stern, and other newspapers and magazines in the US and Europe. Jon has delivered lectures and seminars on global politics, health, logic, and creative power to audiences around the world. You can sign up for his free NoMoreFakeNews emails here or his free OutsideTheRealityMachine emails here.

New CDC Research Debunks Agency’s Assertion That Mercury in Vaccines Is Safe

Source: GreenMedInfo.com
Sayer Ji
April 17, 2017

Originally published on EcoWatch.com.

The U.S. Environmental Protection Agency (EPA) and U.S. Food and Drug Administration (FDA) once again advised pregnant women to curb consumption of fish in order to limit fetal exposures to neurotoxic mercury. This warning raises the baffling query: How can the Centers for Disease Control and Prevention (CDC) justify its recommendations that pregnant women get flu shots which are laden with far more mercury than what’s found in a can of tuna?

The CDC has long answered that nettlesome question with the controversial claim that ethylmercury in vaccines is not toxic to humans. Now, two CDC scientists have published research decisively debunking that assertion. As it turns out, there is no “good mercury” and “bad mercury.” Both forms are equally poisonous to the brain.

The CDC study, Alkyl Mercury-Induced Toxicity: Multiple Mechanisms of Action, appeared last month in the journal, Reviews of Environmental Contamination and Toxicology. The 45-page meta-review of relevant science examines the various ways that mercury harms the human body. Its authors, John F. Risher, PhD, and Pamela Tucker, MD, are researchers in the CDC’s Division of Toxicology and Human Health Sciences, Agency for Toxic Substances and Disease Registry.

“This scientific paper is the one of most important pieces of research to come out of the CDC in a decade,”

Paul Thomas, M.D., a Dartmouth-trained pediatrician who has been practicing medicine for 30 years, said.

“It confirms what so many already suspected: that public health officials have been making a terrible mistake in recommending that we expose babies and pregnant women to this neurotoxin. I regret to say that I gave these shots to children. The CDC led us all to believe that it was perfectly safe.”

Among the findings of the CDC’s new study:

• Methylmercury, the highly-regulated neurotoxin found in fish, and ethylmercury (found in medical products, including influenza and tetanus vaccines, ear drops and nasal sprays) are similarly toxic to humans. Methylmercury and ethylmercury share common chemical properties, and both significantly disrupt central nervous system development and function.
• Thimerosal is extremely toxic at very low exposures and is more damaging than methylmercury in some studies. For example, ethylmercury is even more destructive to the mitochondria in cells than methylmercury.
• The ethylmercury in thimerosal does not leave the body quickly as the CDC once claimed, but is metabolized into highly neurotoxic forms.

Despite this stark rejection of a decade of CDC safety assurances, CDC’s public relations machine is still bucking the new scientific consensus; the article concludes with a telling disclaimer in tiny font:

“The findings and conclusions in this report are those of the authors and do not necessarily represent the views of the Agency for Toxic Substances and Disease Registry.”

CDC’s website continues to feature now discredited safety assurances.

“Baldly dismissing the danger to humans from ethylmercury, has long been a reckless gambit,” said J.B. Handley, a Portland, Oregon, businessman who believes that his son received debilitating injuries from a mercury vaccine.

“With this study, by its own scientists, the CDC has now edged into the realm of criminal endangerment.”

Handley, the founder of Generation Rescue, a vaccine safety advocacy group, condemns the CDC for misleading the medical establishment.

“The CDC knows that pediatricians and physicians rely on its public pronouncements when they make treatment decisions for their patients; how can we escape the conclusion that the agency is knowingly causing the poisoning of tens of millions of American children,” Handley stated.

For example, CDC’s webpage still parrots the now discredited industry canard that:

“Thimerosal contains ethylmercury, which is cleared from the human body more quickly than methylmercury, and is therefore less likely to cause any harm.”

However, the new study makes the opposite conclusion:

“Thimerosal is quickly metabolized in vivo (in a living organism) due to its reactions with protein and non-protein thiols … so the effects of thimerosal reported in numerous articles are very likely the result of exposure to the metabolite ethylmercury.”

Ignoring the agency’s own scientific evidence, the CDC’s webpage stubbornly insists that the “two types of mercury to which people may be exposed—methylmercury and ethylmercury—are very different.” The new CDC study directly contradicts this assertion, “There are many commonalities/similarities in the mechanisms of toxic action of methylmercury and ethylmercury …”

The study meticulously details identical toxicity pathways shared by both forms of mercury:

• Both ethyl and methyl mercury cause DNA damage or impair DNA synthesis (Burke et al. 2006; Sharpe et al. 2012; Wu et al. 2008).
• Both cause oxidative stress/creation of reactive oxygen species (Dreiem and Seegal 2007; Garg and Chang 2006; Myhre et al. 2003; Sharpe et al. 2012; Yin et al. 2007).
• Both decrease glutathione activity, thus providing less protection from the oxidative stress caused by MeHg and EtHg (Carocci et al. 2014; Ndountse and Chan (2008); Choi et al. 1996; Franco et al. 2006; Mori et al. 2007; Muller et al. 2001; Ndountse and Chan 2008; Wu et al. 2008).
• Both cause effects on cell division by damaging the spindle apparatus during mitosis (Burke et al. 2006; Castoldi et al. 2000; Gribble et al. 2005; Kim et al. 2007; Ou et al. 1999b; Machaty et al. 1999; Rodier et al. 1984).
• Both MeHg and EtHg bind to the amino acid cysteine (Clarkson 1995; Wu et al. 2008).
• Both MeHg and EtHg strongly inhibit the reacylation of arachidonic acid, thus inhibiting the reincorporation of this fatty acid into membrane phospholipids (Shanker et al. 2002; Verity et al. 1994; Zarini et al. 2006).
• Both cause an increase in NOS, causing an overproduction of NO (Chen et al. 2003; Chuu et al. 2001; Shinyashiki et al. 1998).
• Both disrupt glutamate homeostasis (Farina et al. 2003a, b; Manfroi et al. 2004; Mutkus et al. 2005; Yin et al. 2007).
• Both alter intracellular calcium homeostasis (Elferink 1999; Hare et al. 1993;Kang et al. 2006; Limke et al. 2004b; Machaty et al. 1999; Marty and Atchison1997; Minnema et al. 1987; Peng et al. 2002; Sayers et al. 1993; Sirois and Atchison, 2000; Szalai et al. 1999; Tornquist et al. 1999; Zarini et al. 2006).
• Both cause effects on receptor binding/neurotransmitter release involving one or more transmitters (Basu et al. 2008; Coccini et al. 2000; Cooper et al. 2003; Fonfria et al. 2001; Ida-Eto et al. 2011; Ndountse and Chan 2008; Yuan and Atchison 2003).

“This study is a nuclear bomb detonating over the CDC,” Boyd Haley, chairman emeritus of the University of Kentucky Chemistry Department, said. “It should be getting international, front page headlines.”

As one of the world’s leading authorities on mercury toxicity, Haley observed, “It’s a momentous rejection of a widely held medical orthodoxy dictating policy changes even more significant than the medical establishment’s reversals on thalidomide, calomel tooth powder, x-rays during pregnancy, or lead exposure to children. In each of these cases, thousands of children were injured or killed before an entrenched medical establishment was finally willing to abandon treatments that were unquestionably causing great harm.”

Ethylmercury vs. Methylmercury in Mass Poisonings

The revolutionary conclusions of the new CDC study actually reflect decades of work by mainstream independent scientists outside the agency. A rich scientific literature that emerged from accidental poisoning events has consistently documented—despite CDC’s official claims—that ethylmercury and methylmercury are equally toxic. In addition to the well-known Minamata and Iraq methylmercury-poisoning, many other large-scale food poisonings have occurred involving ethylmercury fungicides in Iraq in 1956 and 1960, in Pakistan in 1961, and in Russia in the 1960s as well. These episodes resulted in maladies ranging from basic tissue injury to heart and brain injury and even death.

Derban reported in 1974 on 144 cases of mercury poisoning from the use of ethylmercury fungicide on a southern Ghana state farm. Multiple other studies based on these poisoning events showed, as stated in a 1977 study by David Fagan, that the long-term neurological consequences produced by the “ingestion of either methyl or ethyl mercury-based fungicides are indistinguishable.”

A 1979 case report concerned a fifteen-year-old boy who had eaten the meat of a pig that had fed on ethylmercury fungicide−treated seed. Documented effects on the boy included debilitating brain damage and loss of coordination, with high toxicity for the brain as well as the spinal motor neurons, peripheral nerves, skeletal muscles, and heart muscle. The boy died about one month after becoming ill.

Ethylmercury’s use as pesticide was eventually banned in many countries, including the United States and those in the European Union, and for good reason: A 1977 study gauged ethylmercury chloride’s relative toxicity as a pesticide as the fifth most toxic of thirty substances tested, with a score of 12.7. That grade score almost matched that of DDT, at 14.2, an infamous pesticide banned in 1972.

In 1977 Fagan reported on 13 children suffering from exomphalos (a rare abdominal wall defect that allows the intestines to protrude from the abdomen) treated with gauze soaked applications of thimerosal to prevent infection. Of thirteen patients treated with thimerosal, 9 died. The authors tested mercury levels in the tissue of 8 of the children who died. They reported that “blood and tissue levels of mercury well above the threshold at which damage occurs in all other age groups, it is extremely unlikely that these infants escape neurological damage, which may be subtle.” One infant exposed to thimerosal and survived was later reported as being “restless, easily distracted, and not interested in schoolwork.” The authors recommended that “organic mercurial antiseptics should be heavily restricted or withdrawn from hospital use, as the fact that mercury readily penetrates intact membranes and is highly toxic seems to have been forgotten.”

Why Does the US EPA only Provide Guidelines for Exposure to Methylmercury and not Ethylmercury?

In 1995, based on research from outbreaks of poisonings and other research from the Faroe Islands and the Seychelles, the EPA established a safe “reference dose” for methyl mercury(RfD). An RfD is defined as “an estimate of a daily exposure to the human population (including sensitive subgroups) that is likely to be without an appreciable risk of adverse effects when experienced during a lifetime,” according to the EPA.

The EPA adopted for methylmercury an RfD of 0.1 microgram of mercury per kilogram of the individual’s body weight per day. Other health agencies set their own recommended limits for methylmercury exposure, including the FDA in 1979, the World Health Organization in 1989 and the US Agency for Toxic Substances and Disease Registry (ATSDR) in 1999. The highest of these limits was the WHO’s, at 0.47 microgram per kilogram of body weight per day.

In 1999 the US Congress directed the EPA to contract with the nonprofit, independent National Research Council (NRC) to prepare recommendations on an updated and appropriate RfD. The EPA commissioned the National Academy of Sciences (NAS) and the NRC to carry out a study on toxicological effects of methylmercury compounds. The goal was to review the process used by the EPA to establish national safety standards. The committee evaluated the literature, which demonstrated methylmercury compounds’ high toxicity to brain tissue, even at minute levels. The NAS ultimately agreed with the EPA‘s originally conceived RfD, which remains in place today. An RfD has never been established for ethylmercury.

The CDC has crossed ethical and perhaps even legal boundaries by purposefully blocking efforts by the National Institute of Environmental Health Science’s (NIEHS) National Toxicology Program (NTP) to test ethylmercury for toxicity – a process that would have lead to maximum exposure guidelines. In 2000, the FDA nominated thimerosal to the NTP for toxicity testing. However, CDC officials derailed the review telling the NTP committee that “There is a great concern within CDC about continued attacks from anti-vaccine groups questioning the integrity of CDC activities and recommendations regarding the use of thimerosal-containing vaccine.” In response to CDC pressure, the NTP put thimerosal on permanent deferred status. Thimerosal has, therefore, never been tested for safety or toxicity.

Ethyl Mercury Exposure Levels Based on Methyl Mercury Guidelines

A single Thimerosal-preserved flu vaccine contains 25 micrograms of ethylmercury. If the EPA RfD for ingested methylmercury is applied to this injected ethylmercury figure, an individual would have to weigh more than 250 kilograms (551 pounds) for the 25 microgram exposure to be considered safe. Back in the 1990s, a two-month-old child could have received 62.5 micrograms from three vaccines in a single doctor’s visit. Assuming the child weighed about 5 kilograms (11 pounds), he or she would have received 125 times the EPA RfD for methylmercury.

At least one study has suggested that the methylmercury RfD should be set lower for infants and also for fetuses. In 1995, Steven Gilbert and Kimberly Grant-Webster wrote:“Available information on the developmental neurotoxic effects of MeHg [methylmercury], particularly the neurobehavioral effects, indicates that the fetus and infant are more sensitive to adverse effects of MeHg. It is therefore recommended that pregnant women and women of childbearing age be strongly advised to limit their exposure to potential sources of MeHg. Based on results from human and animal studies on the developmental neurotoxic effects of methylmercury, the accepted reference dose should be lowered to 0.025 to 0.06 MeHg [microgram]/kg/day.”

What might this mean for a fetus today? We’ll take the low end of that estimate and apply it to an average 1.15-kilogram (2.54-pound) fetus at the start of the third trimester. A fetus exposed to 25 micrograms of mercury via a Thimerosal-preserved flu shot administered to its pregnant mother could be subject to 870 times the proposed lower reference dose.

Mainstream Science Suggests Ethylmercury is More Toxic than Methylmercury

New and old research support the caveat that “safe” levels of ethylmercury exposure might indeed be dramatically lower than the EPA’s RfD. A 2012 Italian study, for instance, showed that ethylmercury-containing Thimerosal diminished the viability of human cells in the lab at a concentration one-fiftieth that of methylmercury. By this measure, ethylmercury is 50 times as toxic as methylmercury to humans.

Japanese research on rats in 1968 showed that ethylmercury compounds, such as ethylmercuric chloride from which Thimerosal is made, clear the body more slowly than other mercury compounds including mercuric chloride and phenylmercuric chloride.

A book chapter in 1972 by Staffan Skerfving, an emeritus professor at Lund University in Sweden, reviewed literature on methylmercury versus ethylmercury, noting several instances where compounds of the latter appeared more toxic than the former in animal studies.

For example, ethylmercury chloride killed off half of a test population of mice—a classic “LD50” (lethal dose) study—within a week at a concentration of 12 milligrams of mercury per kilogram of body weight; methylmercury chloride’s LD50, meanwhile, lethal to half the mice was 14 milligrams. This study suggested that ethylmercury was twice as toxic.

Further examples abound. Pig studies by Tryphonas and Nielsen in 1973 showed that ethylmercury “proved much more toxic” than methylmercury. Meanwhile, another 1973 study that emerged from a 1971 international conference found the toxicity of ethylmercury compounds comparable to or even greater than that of methylmercury, as well as more persistent in the brain.

An advisory committee at the conference reported that the International Committee on Maximum Allowable Concentration for Mercury and Its Compounds grouped ethylmercury with methylmercury, and observed that accounts of human intoxication with ethylmercury have usually described neurological and other symptoms similar to those of methylmercury. The report noted that in studies of patients transfused with a commercial product of human plasma containing 0.01 percent Thimerosal, as well as in studies of mice injected with an ethylmercury solution, the increased level of inorganic mercury added to the mercury already existing in the body resulted in a “longer biological half-life of total mercury than that reported for methylmercury injection.”

Why do the CDC and WHO Report that Ethylmercury Exposure is Safe?

The WHO’s conclusion that ethylmercury is safer because of its “short” half-life may be based on observations that ethylmercury disappears from blood samples quicker than methylmercury. However, this tendency may be evidence not of ethylmercury’s comparative safety, but of its greater danger if, as science has suggested, ethylmercury is not leaving the body but simply migrating more rapidly to the organs, including the brain. Indeed, studies have shown that an ethylmercury compound’s short residence in the blood stems from its ability to more easily pass into the organs, where it can remain for long periods and possibly cause injury.

For example, Blair in 1975 dosed squirrel monkeys with intranasal saline or Thimerosal daily for six months, finding that, compared to the saline group, mercury concentrations in the Thimerosal group were significantly raised in the brain, liver, muscle, and kidney, though not in the blood. Although there were no signs of toxicity in the animals, Blair concluded that the “accumulation of mercury from chronic use of thiomersal-preserved medicines is viewed as a potential health hazard for man.”

Beyond a possibly greater capacity to have inorganic mercury accumulate in organs, Thimerosal also passes more easily from a mother’s bloodstream through the placenta into a developing baby than does methylmercury. That was the evaluation made in a 1983 review study by A. Leonard. In addition, a 1995 study demonstrated that both ethylmercury and methylmercury cause mutagenic changes at similar concentrations in bacterial cells.

The Twisted Saga of Pichichero

With these and other studies as background, an important study in humans took place in the early 2000s. The study, by Michael Pichichero of the University of Rochester Medical Center and published in The Lancet in 2002, lent some apparent scientific credence to the idea that ethylmercury is safer than methylmercury. Pichichero, who helped develop the HiB vaccine and previously received grants and honoraria as a consultant for other vaccine makers, did not declare these conflicts of interest in a statement in his paper, as required by The Lancet’s peer review rules. The Pichichero study assessed mercury levels in the blood, urine, and feces of forty infants ages six months or younger three to twenty-eight days after they had received Thimerosal-preserved vaccines (DTaP, HepB, and in some cases Hib). For comparison, twenty-one similar infants who received Thimerosal-free vaccines were also evaluated. Although infants who received Thimerosal-preserved vaccines had higher levels of mercury in their blood, urine, and feces than did the infants who received Thimerosal-free vaccines, the authors concluded that the levels of mercury detected were not greater than what is considered safe. Most of the mercury from the injected Thimerosal seemed to have left the children’s bloodstreams more rapidly than methylmercury found in the blood of those eating fish in previous studies; the researchers estimated a half-life of seven days for ethylmercury in the blood. Pichichero concluded that ethylmercury, therefore, did not remain in children’s bodies long enough to possibly cause damage.

Pichichero’s study immediately came under attack by internationally respected scientists in a 2003 letter to The Lancet by Neal Halsey, of the Institute for Vaccine Safety at Johns Hopkins Bloomberg School of Public Health, and Lynn Goldman, also of the Bloomberg School of Public Health. Halsey and Goldman pointed out that Pichichero and colleagues “did not measure the peak blood concentrations that occurred within hours after the injections.” The concentration listed for one child in the study of 20.55 nanomoles per liter was obtained five days post-vaccination. Assuming Pichichero’s own estimate of an ethylmercury half-life in the blood of seven days, the peak blood concentration for this child was 29.4 nanomoles per liter—exceeding the conventional safety threshold of 29.0 nanomoles per liter, and contradicting the study’s claim that “no children had a concentration of blood mercury exceeding 29 nmol/L.” The child in question had received 37.5 micrograms of ethylmercury rather than the possible maximum exposure of 62.5 micrograms. In the latter scenario, the child’s peak blood mercury concentration would have hit 48.3 nanomoles per liter.

Another child in the study registered a 7 nanomole per liter blood concentration 21 days post-vaccination; extrapolating backwards, this child’s peak mercury level might have reached 42 nanomoles per liter. Halsey and Goldman’s letter further pointed out that Pichichero seemed to have cherry-picked the children in the study—some already with no margin of safety for further mercury exposure—seemed to have come from a population with low background environmental and maternal exposure to methylmercury.

Soon after publication of Pichichero’s study, alarming new evidence emerged that ethylmercury lingers in the body. In an unpublished letter submitted to Pediatrics, Dr. Boyd Haley, then-chairman of the chemistry department at the University of Kentuck, and Mark Blaxill challenged Pichichero’s hypothesis that ethylmercury is quickly excreted. Pichichero and colleagues had measured the excretion levels of mercury in the stools of 22 healthy infants exposed to Thimerosal-containing vaccines. Pichichero’s estimated range for the infants aged two and six months was 23 to 141 nanograms per gram of stool (dry weight). Assuming the excretion rate reported by Pichichero, Blaxill and Haley demonstrated that it could take children with low excretion rates of mercury in their stool almost four years to eliminate a 187.5 microgram mercury burden from their bodies.

In 2006, Luis Maya and Flora Luna further debunked Pichichero’s conclusions. The authors pointed out that while Pichichero’s team had found ethylmercury to be excreted in appreciable quantities in the feces, the researchers did not study other body parts beyond the blood, such as the central nervous system. In agreement with Halsey and Goldman, Maya and Luna criticized Pichichero for neglecting to measure the peak serum levels of ethylmercury after the first hours of inoculation, though other investigations had documented substantially elevated blood concentrations in the first 48 to 72 hours after administration in pediatric vaccines. Maya and Luna also pointed out that the study was small and measured variables of pharmacokinetics (the actions of a drug within the body over time), so it was not designed to measure the biological effect of Thimerosal as a preservative.

Pichichero Redux: Yes, Ethylmercury Rapidly Leaves the Blood, but Not the Body. It Lodges in the Brain!

By then, other research had clarified that, while ethylmercury disperses quickly from the bloodstream, this is not evidence of safety. For example, a 2004 study by G. Jean Harry of the National Institute of Environmental Health Sciences noted that mice injected with Thimerosal accumulated mercury in both the brain and kidneys. “By seven days” post-treatment, the study authors wrote, “mercury levels decreased in the blood but were unchanged in the brain” compared to levels measured just 24 hours after treatment, indicating slow clearance.

The landmark study in this regard was conducted by the University of Washington’s Thomas Burbacher and published in 2005. The researchers compared mercury levels in the blood and brains of infant macaques injected with Thimerosal-containing vaccines with monkeys who ingested equal amounts of methylmercury hydroxide via a feeding tube. The former group of primates were exposed to 20 micrograms of ethylmercury per kilogram of body weight on the day they were born and when they were seven, 14, and 21 days old, which was estimated to be within the range of doses that children at different developmental stages were receiving in the United States. The dosing methods were selected to mimic the routes of exposure in humans who eat mercury-containing foods and receive mercury-containing vaccines.

Subsequent tests showed a faster disappearance of mercury from the bloodstream of Thimerosal-injected monkeys than from the methylmercury group. Total mercury amounts in the brain were also threefold less for the Thimerosal-treated monkeys. However, the Thimerosal-injected monkeys had a higher ratio of brain-to-blood levels of mercury than the methylmercury group. In general, the primates injected with Thimerosal in the Burbacher study retained twice the level of inorganic mercury—a breakdown product of Thimerosal that has been suggested to be responsible for the brain damage associated with methylmercury—in their brains as the methylmercury-exposed primates. While all seventeen monkeys given Thimerosal had “readily” detectable levels of inorganic mercury in their brains, only nine of the seventeen exposed to methylmercury had detectable levels. Burbacher cited previous research ranging the half-life of inorganic mercury in various brain regions of primates from 227 to 540 days. In either case, that is a long time period for the toxic element to remain, especially if at higher levels from ethylmercury deposition versus methylmercury.

Burbacher and his colleagues wrote in summary that “[methylmercury] is not a suitable reference for risk assessment from exposure to thimerosal-derived [mercury]” and that: Data from the present study support the prediction that, although little accumulation of [mercury] in the blood occurs over time with repeated vaccinations, accumulation of [mercury] in the brain of infants will occur. Thus, conclusion [sic] regarding the safety of thimerosal drawn from blood [mercury] clearance data in human infants receiving vaccines may not be valid, given the significantly slower half-life of [mercury] in the brain as observed in the infant macaques.

A more recent 2012 study by Croatian researchers took a similar approach as Burbacher’s study, but in suckling rats. That study also discredits CDC’s claims of ethylmercury’s comparative safety. Maja Blanusa and colleagues gave rat pups either Thimerosal or inorganic mercury three times in their first 11 days of life, mimicking human infant vaccination schedules. The scientists then assessed the total retention of mercury and excretion over six days. The Thimerosal-exposed rats showed higher mercury retention rates in their brains. Furthermore, these Thimerosal-exposed rats exhibited similar fecal excretion and much lower urinary excretion compared to the inorganic mercury-exposed rats. That second group also demonstrated higher retention rates of mercury in organs other than the brain.

Two additional studies in the last few years by researchers in Brazil and Germany show, again, that methylmercury in particular should not be considered summarily more dangerous than ethylmercury. The studies found that cells similarly take up both forms of mercury. The former, by Luciana Zimmermann and colleagues, showed in 2013 that the methyl- and ethylmercury entered cultured rat cells in roughly equal measure and display similar toxicities. The 2014 German study led by Christoph Wehe used novel laboratory techniques in concluding that methylmercury and ethylmercury in the form of Thimerosal accumulated in equal measure in a type of cultured human neural cell.

Overwhelmingly, the literature presents clear evidence that ethylmercury is invasive and persistent in the brain. Emerging evidence suggests that ethylmercury is more toxic than methylmercury, in direct contrast with the CDC’s historic position. It’s time for CDC’s public relations department to catch up with mainstream science. Since the World Health Organization (WHO relies mainly on CDC’s vaccine safety science, the CDC’s unscientific pronouncements endanger, not just U.S. children, but hundreds of millions of children around the world. Knowing what we now know, the U.S. Federal agencies and the WHO should follow the precautionary principle and phase out the use of thimerosal in all medical products, including vaccines.

Read More At: GreenMedInfo.com

Julie & The Boys: CDC, Merck, Vaccines

Source: NoMoreFakeNews.com | JonRappoport.wordpress.com
Jon Rappoport
April 24, 2017

I write this story now to remind people there are several titanic unresolved issues surrounding research fraud at the CDC, involving the MMR vaccine.

We all know about CDC whistleblower William Thompson, a long-time researcher at the CDC. Thompson still works there.

On August 27, 2014, he released a statement through his lawyer, Rick Morgan, in which he admitted research fraud.

Thompson confessed he and his CDC co-authors cooked the data in a key 2004 study, thereby exonerating the MMR vaccine from any blame in causing autism.

Thompson has never been subpoenaed by Congress to confess what he knows about this case.

But what about Stephen Kraling and Joan Wlochowski?

Who?

They’re two former Merck virologists who filed a qui tam suit against Merck, the manufacturer of the very same MMR vaccine.

The suit claims Merck defrauded the US government by selling the vaccine, under a federal contract, when Merck knew the mumps component of the vaccine was far less effective than advertised.

Of course, Merck disputed this claim, but on September 5th, 2014, Judge Jones, of the Federal District Court for the Eastern District of Pennsylvania, gave the green light for the suit to move forward.

Kraling and Wlochowski assert several levels of Merck fraud:

To achieve a slam-dunk success, Merck tested the effectiveness of the MMR vaccine against the version of the virus in the vaccine, rather than against the natural mumps virus a person would catch in the real world.

Merck irrelevantly and deceptively added animal antibodies to the test results, thus giving the false appearance of strong human immune response to the vaccine.

On top of that, Merck faked the quantitative results of the tests to which the animal antibodies had been added.

Here is where these two Merck whistle blowers and Thompson, the CDC whistle blower, intersect:

In 2004, according to a report I have seen, Thompson wrote a letter to CDC Director, Julie Gerberding, warning her that he was about to present troubling and sensitive data about the MMR vaccine at an upcoming conference on vaccines and autism.

Thompson’s meaning was clear. He had found a connection between the MMR vaccine and autism.

Gerberding never answered his letter, and Thompson’s presentation at that conference was canceled.

Gerberding left the CDC in 2009.

She moved on to become…

The president of Merck Vaccines, the manufacturer of the MMR vaccine.

Major media consider this a non-story, on the level of a can of overflowing garbage on a quiet street corner.

Well, they have to consider it a non-story. If they reported it and pressed it and dug deep into it, they could fracture the pillars of the entire vaccine establishment.

In order to get at the whole truth (or refute any of the charges raised in this article), Congress needs to hold hearings, and competent committee members need to question, at length, William Thompson, the two Merck whistle blowers, and Julie Gerberding.

I say the chance of that happening is close to zero. I’d love to be proven wrong, but I see no sign Congress is willing to step up to the plate.

Too many drug-company lobbyists, too much campaign money from the drug companies, too much fear of going up against entrenched “scientists” who keep claiming all vaccines are safe and effective.

We’ve heard, from sources other than President Trump, that he is going to order a task force to investigate vaccine safety. We’ll see if it happens.

Earlier this year, I wrote about a group of CDC employees who are anonymously chomping at the bit to expose criminal behavior at their agency.

They call themselves the Spider Group—Scientists Preserving Integrity, Diligence and Ethics in Research. They have penned a letter to the CDC’s chief of staff, Carmen S. Villar:

Here is the explosive accusation they make:

“We are a group of scientists at CDC that are very concerned about the current state of ethics at our agency. It appears that our mission is being influenced and shaped by outside parties and rogue interests. It seems that our mission and Congressional intent for our agency is being circumvented by some of our leaders. What concerns us most, is that it is becoming the norm and not the rare exception.”

“Some senior management officials at CDC are clearly aware and even condone these behaviors. Others see it and turn the other way. Some staff are intimidated and pressed to do things they know are not right.”

“We have representatives from across the agency that witness this unacceptable behavior. It occurs at all levels and in all of our respective units. These questionable and unethical practices threaten to undermine our credibility and reputation as a trusted leader in public health.”

Since this initial explosion, I have heard nothing from the Spider Group. Perhaps they are waiting for a signal from President Trump that it is safe to proceed.

There is too much waiting. Whistle blower William Thompson is waiting for Congress to subpoena him. Congress is sitting on its hands, waiting. The two Merck whistle blowers are waiting for their law suit to move forward.

Children’s futures and lives are on the line.

Every day that passes brings new vaccine damage.

Read More At: JonRappoport.wordpress.com
_______________________________________________________________

Jon Rappoport

The author of three explosive collections, THE MATRIX REVEALED, EXIT FROM THE MATRIX, and POWER OUTSIDE THE MATRIX, Jon was a candidate for a US Congressional seat in the 29^th District of California. He maintains a consulting practice for private clients, the purpose of which is the expansion of personal creative power. Nominated for a Pulitzer Prize, he has worked as an investigative reporter for 30 years, writing articles on politics, medicine, and health for CBS Healthwatch, LA Weekly, Spin Magazine, Stern, and other newspapers and magazines in the US and Europe. Jon has delivered lectures and seminars on global politics, health, logic, and creative power to audiences around the world. You can sign up for his free NoMoreFakeNews emails here or his free OutsideTheRealityMachine emails here.

What if a mandatory penicillin vaccine were forced onto every child in America starting tomorrow?

Source: NaturalNews.com
S.D. Wells
April 10, 2017

Currently, the state of California requires all children to be force vaccinated with the entire schedule of CDC “recommended” vaccines in order to be able to exercise their right to attend public school and get an education. It doesn’t matter if any of those children are allergic to mercury, aluminum, polysorbate 80, African green monkey kidney cells, genetically modified bacteria, neomycin (an antibiotic), human serum albumin (other people’s blood), formaldehyde, monosodium glutamate (MSG), bovine extract, gelatin, calf serum, or sodium chloride. Every child must be injected with all of these ingredients, without being tested for allergies against them first, as they are all listed and contained in the CDC’s “excipient” list of vaccine ingredients, in case you have any doubts. How many other U.S. states will soon demand forced vaccination for all children?

Even though penicillin, an antibiotic about 5 to 10% of the U.S. population is allergic to, is not currently a vaccine ingredient, does it matter? Did you know many vaccines are made with a peanut oil extract, but it’s not listed because only “trace amounts” remain? Nearly 2 million U.S. children have severe peanut allergies. Coincidence? Are those trace amounts enough to cause severe allergic reactions? You bet they are, along with unnatural, violent immune system reactions to injecting human blood, monkey kidney cells, cow’s blood, chicken embryo and live viruses combined from different strains.

Extreme vaccine-induced allergic reactions occur when your immune system reacts to foreign proteins and chemicals lodged in muscle tissue or that cross the blood/brain barrier

Penicillin allergy occurs because certain children’s immune systems mistake the drug as a harmful substance, often because the drug is injected with several viruses, bacteria, chemical adjuvants, foreign proteins, human pooled blood samples, and other experimental excipients that have never been tested for safety, allergies or for their neurotoxic effects on humans. Children in America are guinea pigs, including infants and babies still in the womb. Mercury is toxic to humans at any level, even if only eaten or when it touches the skin. Imagine what’s happening when it’s shot directly into body tissue through a needle.

If the human body detects and identifies these chemicals, drugs, and foreign proteins as harmful substances, it develops antibodies to them, even if they are mixed with powerful antibiotics. The second and third time those same drugs and chemicals are injected into the child, the reaction can be violent, brain damaging, central nervous system damaging, and yes, sometimes lethal, just like with penicillin.

Why the massive autism epidemic in 2017? Do the math…

Since 5 to 10% of the U.S. population is allergic to penicillin, if you injected everyone today with a penicillin-loaded vaccine, millions of people would suffer a severe allergic reaction, and many would die. There are more than 300 million Americans. If just 2% had a lethal allergic reaction to a penicillin inoculation, that would equate to about 6 million deaths. That’s how many people were murdered in the Holocaust. Now if you injected 300 million Americans with mercury, aluminum, formaldehyde, polysorbate 80, MSG, and African green monkey kidney cells, and just 2% of those people had a severe allergic reaction where their immune systems went into shock and their brains were damaged by the neurotoxins, there would be about 6 million people with autism spectrum disorder (ASD).

A new government survey of parents suggests that 1 in every 45 children ages 3 through 17 have already been diagnosed with ASD. This number is much higher than the CDC estimate, and for good reason. There are approximately 80 million children in the U.S.A. now. That means there are about 2 million children diagnosed with some form of autism, and many, many others who are suffering from vaccine damage that’s not diagnosed as ASD. When will that number equal or surpass 6 million? Statistics show that every other child in America will have some form of autism by 2032 – that’s 40 million children and just 15 years from right now.

Nearly 4 million American kids today have either severe peanut allergies or autism–wonder why?

The next time those autistic children are injected with the same drugs and chemicals, including the mercury-loaded influenza vaccine, a.k.a. the “flu shot,” specific antibodies will flag the dangerous concoction once injected into muscle tissue and blood, and the chemicals released by this activity cause the signs and symptoms associated with severe and often lethal allergic reactions, just like with penicillin. Get it?

Signs and symptoms of allergic reactions to injecting vaccine ingredients like peanut oil, formaldehyde, MSG, sodium chloride, aluminum, human albumin, aborted fetal cells, monkey kidney cells, gelatin, neomycin and mercury include: skin rash, hives, itching, fever, swelling, shortness of breath, wheezing, anaphylaxis, central nervous system damage, brain damage, nausea, abdominal cramps, rapid pulse, drop in blood pressure, seizures, loss of consciousness, coma, and death. Some severe allergic reactions to vaccines occur days or weeks after the concoction is injected.

Ask your doctor if vaccines contain experimental excipients. Ask the nurse for the vaccine ingredients insert and read every ingredient aloud in front of the doctor and your child. You should be aware of the biggest medical fraud cover up in the history of medicine. Here’s what you can do right now to combat the insanity.

Watch the highly informative whistle-blowing interview with the directors of the controversial film VAXXED that exposes the CDC’s known link between vaccines (such as the MMR–measles, mumps, rubella combo jab) and autism:

Sources for this article include:

NaturalNews.com

TruthWiki.org

NaturalNews.com

TheDoctorWithin.com

TruthWiki.org

CDC.gov

 

There are far more vaccine-damaged children in America than chemical weapons-damaged children in Syria

Source: NaturalNews.com
Mike Adams
April 8, 2017

By now, you are surely aware that the U.S. war machine, under President Donald J. Trump, has launched cruise missiles against the Syrian government. The emotionally-charged justification for all this is that “beautiful babies” were being killed by chemical weapons. While the pro-war factions of the establishment elite are celebrating the missile strike, virtually the entire independent media is convinced that the “chemical attack” narrative is little more than a convenient false flag to justify “regime replacement” activities desired by America’s deep state. Even Ron Paul and Paul Craig Roberts have both asserted this.

President Trump’s explanation for the attack included these words:

Assad choked out the lives of innocent men, women and children. It was a slow and brutal death for so many. Even beautiful babies were cruelly murdered in this very barbaric attack. No child of god should ever suffer such horror.

If you replace the word “Assad” with “CDC” or “the vaccine industry,” it all makes even more sense. Vastly higher numbers of children right here in America have been “cruelly murdered” in the “barbaric attack” of toxic vaccines than have ever been killed by chemical weapons in Syria.

I agree with the President that “No child of God should ever suffer such horror,” but I wonder when this President will start working to stop the chemical assault on America’s children that’s being waged every day by the vaccine industry.

Mercury in vaccines is a state-sponsored CHEMICAL WEAPON that’s used against America’s children every day

No chemical weapon should ever be deployed against any child: Not VX Nerve Gas, not Sarin Gas and not toxic, brain-damaging mercury. The destruction of biological tissue with devastating effect is accomplished by all three of those substances (and many more, including glyphosate herbicide). Yet mercury is the only chemical weapon that’s deliberately INJECTED into children with devastating effect. You might even call mercury a “biological cruise missile” attack on brain tissue.

On the science side, there’s no question whatsoever that mercury is extremely toxic to human neurology. Even the CDC’s own research has conclusively proven that mercury in vaccines is toxic to children. As I wrote in a Natural News article earlier this year, entitled Health Ranger exposes chemical violence of mercury vaccines: The “war on children” must be stopped:

The CDC is a criminal operation that preys upon innocent children using fraudulent science. The “Vaccine Holocaust,” as it is sometimes called, is a deliberate and widespread assault on children using chemical violence. This war on children must be brought to an end in the name of compassion, sanity and legitimate science (not the fraudulent corporate science pushed by vaccine companies and the corrupt CDC).

Right now, mercury is still used in vaccines given to children and expectant mothers in the United States. This practice is barbaric, highly unethical and stands in horrific opposition to all the known science on the neurotoxicity of mercury. Those engaged in the continued pushing of mercury vaccines onto children are knowingly taking part in the most gruesome and dishonest medical science cover-up in the history of our world. It is time that parents, citizens, independent scientists and compassionate protectors of life took a stand against the child poisoners who are pushing mercury vaccines that cause permanent neurological disorders in children (including autism in some children).

This is why I continue to remind America that Vaccine Injury Denialism is the denial of fundamental human dignity.

Continue Reading At: NaturalNews.com

How many African Green Monkeys are infected, euthanized and then organ harvested each year to make FDA-approved vaccines?

[Editor’s Note]

For those that think this is a joke, this very document at the CDC’s very own website shows this, and many other toxins within vaccines.  This is why its imperative people do their research, because if people really knew what vaccines had, they’d think they woke up in another reality.

Source: NaturalNews.com
Ethan Huff
March 26, 2017

Now that it’s been proven that vaccine manufacturers harvest kidney cells from African Green Monkeys to produce vaccines that are injected into children, many are now wondering just how many of these monkey are captured, euthanized, and processed into vaccine ingredients each year to make these FDA-approved poison jabs?

As you may recall, Natural News was falsely accused of spreading “fake news” after breaking the story on African Green Monkey kidney cells, and other horrific ingredients, being used in the manufacture of vaccines. For merely publishing the ingredients listed on the vaccine package inserts that manufacturers are required to provide with their vaccines, Natural News faced an unrelenting barrage of fact-less criticism.

Not long after, though, it was realized that Natural News was telling the truth: these ingredients are, indeed, being used in childhood vaccines, and many parents aren’t aware of this fact because their doctors and pediatricians aren’t showing them the vaccine package inserts. Now the outrage is going in the other direction, as it should, because people are realizing that they’ve been lied to by their government. (RELATED: You can stay informed on important vaccine issues by visiting Vaccines.news.)

“As Natural News correctly reported, one of the many animal-derived ingredients used in vaccines and openly admitted by the CDC is African Green Monkey kidney cells,” writes Mike Adams, the Health Ranger. “Apparently, this realization was just too much for the scientifically illiterate media (and wholly dishonest vaccine pushers) who insisted it couldn’t possibly be true.”

You can see the list of ingredients yourself, published by the CDC, at this Natural News article link.

Parents: are you aware of all the horrible things being injected into your children?

Knowing that millions of vaccine are produced and administered every single year for injection into children, it boggles the mind to consider just how many of these African Green Monkeys are being subjected to death in order to manufacture them. The number has to be at least into the thousands, though no official number has been released by the CDC.

Many of these same vaccines also contain cells from aborted human fetal tissue, which sheds a whole new light on Planned Parenthood’s illegal baby harvesting scheme that involved selling aborted baby body parts to biotechnology companies for use in manufacturing “medicines.” It is now abundantly obvious that Planned Parenthood was trafficking those baby body parts for potential use in vaccine manufacture.

This is in addition to all the viruses, heavy metals, chemical preservatives, food colorings, and other toxic ingredients used in making vaccines. Children today are being injected with some of the most disturbing and poisonous substances known to mankind, and very few people seem at all concerned with what’s going on.

It’s probably because so many people don’t even know what’s going on, thanks to the mainstream media’s dereliction of duty in reporting on this important subject. Every parent should be required to peruse a vaccine package insert before injecting his or her child with a vaccine, and yet this is rarely the case.

Most doctors fail to inform parents about the presence of both human and animal tissue in their children’s “medicine,” for instance. They rarely mention the use of toxic mercury (thimerosal) in vaccines, or other noxious ingredients like aluminum, genetically-modified (GM) byproducts, cow blood, chemical solvents, and more. These additives are certifiably NOT safe, and they serve no beneficial purpose for those into whom they’re being injected.

“Several vaccines currently available in the United States were developed using the Vero cell line, started from African green monkey kidney cells,” explains The History of Vaccines.

These include:

• Rotavirus vaccines (Rotarix by GlaxoSmithKline and RotaTeq by Merck & Co.)
• Polio vaccine (IPOL by Sanofi Pasteur)
• Smallpox vaccine (ACAM2000 by Sanofi Pasteur)
• Japanese encephalitis vaccine (Ixiaro by Intercell)

Read More At: NaturalNews.com

Sources for this article include:

NaturalNews.com

HistoryOfVaccines.org

The Vaccine Illusion: How Vaccination Compromises Our Natural Immunity and What We Can Do To Regain Our Health

Source: GreenMedInfo.com
Tetyana Obukhanych, PhD
March 23, 2017

Available for Immediate Free Download

This is the introduction to the new vaccine book by Tetyana Obukhanych (Ph.D. in immunology from Rockefeller University, New York, NY) Vaccine Illusion. Dr. Obukhaynch and GreenMedInfo.com are giving the book away for free for a limited time only. Get your copy here.  

Tetyana Obukhanych, Ph.D.

I know of many alternative health practitioners and even of a few pediatricians who have embraced the non-vaccination approach to health. However, I have yet to encounter one among my own kind: a scientist in the trenches of mainstream biomedical research who does not regard vaccines as the greatest invention of medicine.

I never imagined myself in this position, least so in the very beginning of my Ph.D. research training in immunology. In fact, at that time, I was very enthusiastic about the concept of vaccination, just like any typical immunologist. However, after years of doing research in immunology, observing scientific activities of my superiors, and analyzing vaccine issues, I realized that vaccination is one of the most deceptive inventions the science could ever convince the world to accept.

As we hear more and more about vaccine injuries, many individuals are starting to view vaccination as a necessary evil that has helped us initially to overcome raging epidemics but now causes more damage than benefit to our children.

As an immunologist, I have a different and perhaps a very unique perspective. I have realized that the invention of vaccination in the 18th century has precluded us from seeking to understand what naturally acquired immunity to diseases really is. Had we pursued a different route in the absence of that shortcut, we could have gained a thorough understanding of naturally acquired immunity and developed a truly effective and safe method of disease prevention compared to what vaccines can possibly offer.

The biological term immunity refers to a universally observed phenomenon of becoming unsusceptible to a number of infectious diseases through prior experience. Because of the phonetic similarity between the words immunology and immunity, it is tempting to assume that immunology is a science that studies the state of immunity, but this is not the case. Immunology is a science that studies an artificial process of immunization – i.e., the immune system’s response to injected foreign matter. Immunology does not attempt to study and therefore cannot provide understanding of natural diseases and immunity that follows them. Yet, the “knowledge” about the function of the immune system during the natural process of disease is recklessly inferred from contrived immunologic experiments, which typically consist of injecting laboratory-grown microorganisms (live or dead) or their isolated parts into research animals to represent the state of infection. Because immunologic experiments are unrealistic simulations of the natural process, immunologists’ understanding of nature is limited to understanding their own experimental models. Immunologists have confined the scope of their knowledge to the box of experimental modeling, and they do not wish to see beyond that box. Thinking within the box only reinforces the notion of vaccination and cannot provide any other solution to the problem of diseases.

Despite the fact that the biological basis of naturally acquired immunity is not understood, present day medical practices insist upon artificial manipulation of the immune response (a.k.a. immunization or vaccination) to secure “immunity” without going through the actual disease process. The vaccine-induced process, although not resembling a natural disease, is nevertheless still a disease process with its own risks. And it is not immunity that we gain via vaccination but a puny surrogate of immunity. For this reason, vaccination at its core is neither a safe nor an effective method of disease prevention. Yet, immunologists have nothing better to offer because they can only go as far as their deeply rooted immunologic dogma allows them.

Three important factors have contributed to my gradual disillusionment with immunologic paradigms and their applications – vaccines. First, several significant inconsistencies within immunologic theory made me quite unsatisfied with its attempted explanation of immunity. Second, I observed how some seasoned immunologists would omit mentioning the outcome of crucial experiments to make their publication on new vaccine development strategies look very promising. This made me suspicious about the vaccine development process in general and eager to take a look at the other side of the vaccination debate.

The third factor was the birth of my child. This event compelled me to take a break from laboratory research for a few years. I completely shed my identity of an immunologist and became a parent determined to raise a healthy child. I was amazed at how clueless I was about what really matters for health despite my proficiency in all those fancy immunologic theories amassed in the Ivory Tower. For the sake of my child, I had to reconsider everything I knew in immunology. I searched deeper and deeper for the root of vaccine problems we face today and it all came back to me in clear light.

This book is intended to give parents essential immunologic background for making vaccination decisions for their children. Making vaccination decisions is an important personal responsibility that should not be left to any medical or scientific authority. Parents should educate themselves about vaccines and diseases to the extent that they feel absolutely confident and well prepared for taking full responsibility for the consequences of their decisions.

It is important to estimate risks of vaccine injuries versus risks of exposure to vaccine-targeted microorganisms. But the analysis should not stop there. I urge every parent to consider how vaccines achieve their effects, and if the desired vaccine effects truly benefit our children and our society. The implications of vaccination were not acceptable to me, neither as a parent nor as a scientist, and this book is my effort to tell other parents why.

Another goal of this book is to raise awareness in our society about the urgent necessity to change basic immunologic research in a way that will finally bring us understanding of naturally acquired immunity. It is up to future generations of immunologists to rescue this science and put it on the right track. The benefits for humankind will be enormous, as this would make both vaccine injuries and fear of diseases a matter of the past. But to make this happen, the field of immunology must first be cleared from the weeds of immunologic dogma.

And finally, this book is my attempt to heal the schism in our society between those who oppose vaccines due to vaccine safety concerns and those who oppose the anti-vaccine movement due to the fear of diseases. This schism has brought us enormous suffering by dividing families, friends, and health provider communities. But we all have the same goal: we all want the best for our children. Only by uniting our efforts will we be able to find a solution to the problem of diseases without compromising our health by means of vaccines.

Download the book for FREE now and learn the following: 

• Why do vaccines fail to give us lasting immunity from viral diseases?
• Why do vaccines provide no guarantee of protection from bacterial diseases?
• Why is vaccine-based herd immunity not achievable?

Read More At: GreenMedInfo.com
_______________________________________________________

Tetyana Obukhanych earned her Ph.D. in Immunology at the Rockefeller University in New York, NY with her research dissertation focused on understanding immunologic memory, perceived by the mainstream biomedical establishment to be crucial to vaccination and immunity.  During her subsequent involvement in laboratory research as a postdoctoral fellow within leading biomedical institutions, such as Harvard Medical School and Stanford University School of Medicine, Dr. Obukhanych realized the flaws and limitations of current immunologic paradigms. Learn more about her work on her website.

________________________________________________________
© [March 23, 2017] GreenMedInfo LLC. This work is reproduced and distributed with the permission of GreenMedInfo LLC. Want to learn more from GreenMedInfo? Sign up for the newsletter here http://www.greenmedinfo.com/greenmed/newsletter.