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If what you are about to read is true of the mystery plague supposedly decimating the Ukraine and heading, according to the highly unreliable and dangerous WHO (and its handmaidens, the FDA and CDC), there is even less reason to consider for more than the space of an eye blink receiving a vaccination for the Swine Flu. First of all, as we all know by now, the H1N1 vaccines, all 5 of them, so precipitously and profitably approved by the FDA, are untested, unsafe and unnecessary. Second of all, IF the H1N1 virus has mutated, or has BEEN mutated (by Baxter, perhaps, in its Ukraine lab as many people have speculated), and IF it spreads, or IS spread, then IF the vaccines were effective for the earlier H1N1 virus, with or without dangerous adjuvants, then they would no longer be effective against the mutated virus.
Question: IF Dr. Victor Bachinsky, a leading Ukrainian pathologist, is correct and the virus that has killed a few, yes, only a few (not the legions of people news reports have suggested), people in the Ukraine is, in fact, a combined H1N1 and parainfluenza virus, could that re-assortment or recombination of genes have taken place naturally? The WHO says that although there has been a change in the H1N1 virus, it is enough to kill horrifyingly large numbers of people, but NOT enough to change the H1N1 virus enough to make the billions and billions of dollars spent on the Swine Flu vaccines and injectable adjuvants (over $7 Billion in the US alone at last count) a sort of TARP bailout for a pharmaceutical industry which needed no bailing out, thank you very much.
A quick note on Parainfluenza Viruses:
Human parainfluenza viruses (HPIVs) are a group of four distinct serotypes of single-stranded RNA viruses belonging to the paramyxovirus family. They are the second most common cause of lower respiratory tract infection in younger children. Repeated infection throughout the life of the host is not uncommon. Symptoms of later breakouts include upper respiratory tract illness as in a cold and sore throat. The incubation period of all four serotypes is 1 to 7 days. Parainfluenza viruses can be detected via cell culture, immunofluorescent microscopy, and PCR. Though no vaccines currently exist, research into vaccines for HPIV-1, -2, and -3 is underway. Parainfluenza viruses last only a few hours in the environment and are inactivated by soap and water.
http://encyclopedia.thefreedictionary.com/Parainfluenza+virus+1,+human
Dr. Bachinsky says that the mystery illness which has claimed horrifying numbers of victims because their lungs turn black and are totally destroyed in the course of a pneumonic plague-like disease is no such thing, calling the reported mystery plague descriptions “nonsense”.
He also points out that with more than 60,000 hospitalizations in his region of the Ukraine, a mere 23 deaths have occurred. This makes the death rate among hospitalized persons 1 in 2609 persons hospitalized. This is hardly an impressive “mystery plague”.
Making reports of a doomsday plague even more absurd, he points out that antibiotics are not effective since there is no inflammation of the lungs, meaning no pneumonia develops, and that Tamiflu should not be used prophylactically because of its serious toxicity. He attributes the deaths in this disease to the use of antibiotics!
The answer? A good immune system. Unlike the WHO which advises people NOT to build up their immune systems lest they succumb to a cytokine storm, or exuberant immune response which is so strong that it winds up killing the owner of the immune system that it is precisely a strong immune system that allows people to survive. Those with strong immune systems fight off the virus when it attacks the lungs so bleeding in the lung does not take place. If that does not happen, you can have the virus in your system, as we have so many others which we are unaware of, and not have either bleeding or clinical disease.
Dr. Bachinsky recommends immune enhancements like garlic, honey and herbs. I would add nutrient support for the immune system like Vitamin C plus Vitamins E and A along with zinc, nano silver (we at the Natural Solutions Foundation are particularly enthusiastic about Silver Biotics, available at www.Nutronix.com/naturalsolutions), glutathione, Vitamin D (General Bert and I personally take 10,000 IU per day on a log-term basis). The immune supporting, viral suppressing benefits of each of these inexpensive nutrients is abundantly documented.
We have all heard that it is the cytokine storm that kills the healthy in weaponized viral attacks like those initiated by the H5N1 and H1N1 viruses. However, before a virus can impact your body, the immune defenses that keep your body safe from invaders 24/7 must fail. The logic is inescapable to me, at least: if the immune system does its job, the virus that then turns on an overwhelming and dis-coordinated immune response to itself will not be able to do do.
When it comes to plagues, manufactured in a laboratory or not, take everything you hear, especially from official organizations like the WHO, CDC and FDA, with much more than a grain of salt, and take immune supporting nutrients liberally.
Yours in health and freedom,
Dr. Rima
Rima E. Laibow, MD
Medical Director
Natural Solutions Foundation
www.HealthFreedomUSA.org
Valley of the MoonTM Eco Demonstration Project
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Professor Victor Bachinsky, PhD., is a coroner in the Chernivtsi region of Ukraine. He provides evidence which indicates that parainfluenza mixed with the H1N1 virus, not pneumonic plague, has caused so much illness in Ukraine. Yet more strains of influenza which have combined, a strong indication that we are dealing with a laboratory developed bio-weapon.
[Translated from Russian]
Ukraine; Virus Is Mixture Of H1N1 And Parainfluenza, Causes Cardiopulmonary Failure; Indicates BioWeapon
http://www.doomdaily.com/2009/ukraine-virus-is-mixture-of-h1n1-and-parainfluenza-causes-cardiopulmonary-failure-indicates-bioweapon/
Based on autopsies, we have come to the conclusion: it’s not pneumonia, but cardiopulmonary insufficiency and cardiogenic shock … The virus enters directly into the lungs, there is bleeding … Antibiotics should not be used …
Why do we have such a high mortality rate in the country? Because people are going to pharmacies to get medicine instead of going to their doctors to be treated … No it is not pneumonic plague. It’s all nonsense … antibiotics do not help … Those with strong immune systems will survive. People with weak immune systems will succumb to the illness … Face Masks provide 30% extra protection. Wearing glasses gives an additional 10% protection, that is 40%, because the virus penetrates the mucus membranes.
The Head of the Chernivtsi regional forensic bureau, Professor Victor Bachinsky PhD, makes a strong statement: all the victims of the virus in Bukovina (22 persons aged 20 to 40 years) died not from bilateral (double) pneumonia, as previously thought, but as a result of viral distress syndrome, i.e. the total destruction of the lungs. We caught up with Professor Bachinsky, to find out how he came to this conclusion, and how people can protect themselves from this disease.
Professor, you said earlier that the virus, from which many people have died – is a mixture of types of parainfluenza and influenza A/H1N1. How do you cure this disease?
The question of how to treat this virus is not up to me. I am a pathologist. I just found out what it is and made an exact diagnosis. It is important to provide the correct treatment based on diagnosis.
There are strict protocols and standards of treatment in medicine. If a doctor treats a patient who dies, their relatives can make a complaint that they were not treated properly (misdiagnosed).The Ministry of Health has set the protocols and standards of treatment for each diagnosis. If diagnosed correctly, the treatment should be correct …
In the Chernivtsi region 18 people have died. We studied all the history and evidence from this disease, preclinical, clinical, resuscitation. When we perform an autopsy organs and tissues have histological studies (cell analysis) and we concluded that it was not pneumonia, and has no relation to pneumonia whatsoever.
These results are the foundation to ensure that doctors who treat this disease all over Ukraine, change their tactics and standards of care.
Can this new virus be cured?
It depends on the immune system. If a person’s immune system is strong, they will overcome it. There are people who carry this strain of H1N1 and remain on their feet and don’t even realize they are sick.
Antibiotics definitely should not be taken. Antibiotics are the reason we have such a high mortality and infection rate in this country, because people go to the pharmacy, describe their symptoms to the pharmacist and ask for drugs. They buy antibiotics, take them, this lowers their immune system and as a result they become sick. If prescriptions were required to buy these medications, like in other countries, this would not have happened. It is the ability to buy antibiotics over the counter without a prescription which has done so much harm to the State.
During autopsies, what did the lungs look like? Were they really black, which gave rise to so much talk of pulmonary plague?
No, they are not black … This is not pneumonic plague. It’s all nonsense. Pneumonic plague has a very different morphology. We have, for example, 60 thousand people who became sick and 23 have died. With pulmonary plague, we would now have a mortality rate of 59 thousand …
This is a viral attack that destroys the lungs.
It turns out that not only in Bukovina, but also throughout the Ukraine people did not die from pneumonia, but from this toxic strain?
Yes, It’s not pneumonia! This destruction of the lungs. This strain is very toxic, and if the immune system is weak, there is bleeding in the lungs. In the lungs there is a tiny structure – acinus, which looks like a bunch of grapes. When you breathe, oxygen enters this tiny “bunch of grapes” ( pulmonary alveoli ). On the surface of the acinus are the capillaries, where red blood cells saturate with oxygen and give blood, which supplies all tissues and organs in the body.
And once the virus enters the lungs – hemorrhaging begins immediately in the acinus. A continuous hemorrhage … It takes several hours. In the blood fibrin is formed, and from it – giolinovaya membrane, resembling a plastic bag. It envelops the acinus, and the person breathes in oxygen, but it is not transferred to the tissues. And people just gasp. There is a cardio-pulmonary insufficiency and cardiogenic shock. People die of cardiogenic shock. And there is no pneumonia. Pneumonia – an inflammation, which is treated with antibiotics. Antibiotics cannot help at any stage. There should be absolutely different treatment.
And how about “Tamiflu(c)” – does it help?
This is not an antibiotic, it is an antiviral drug, which should be applied on the second or third day of the disease. But you can not use Tamiflu as a preventative, because it is toxic, http://www.infowars.com/tamiflu-toxic-causes-mental-disorders-in-teenagers/.
What are the best measures to resist the disease? Is it advisable to use a mask, garlic, vitamin C?
The primary method of prevention is a face mask. This give 30% extra protection. If you wear glasses – it is 40%, because the virus enters through the mucous membranes.
It is necessary to improve the human immune system. Not only now, but in general. Garlic, onions, wild rose, viburnum (guelder rose), raspberries, citrus fruit, honey, and other fruits and vegetables – whatever you want. Those with a strong immune system will survive. Those with weaker immune systems will succumb to the disease.
We have a lot of people in Ukraine who like shopping at the open markets. If we can avoid open markets, the less people will be in contact with each other and more lives will be saved.
You have contacted the Health Ministry and advised them to review the standards for treatment of patients. What did they say?
We sent them all our data, the necessary protocols and standards of treatment, our diagnosis. But it is clear that decisions cannot be instantaneous.
And why until now has nobody else known about this disease? What were the leading specialists in the Ministry of Health doing all this time?
Perhaps this is due to the fact that there are scientists who are working on a purely theoretical basis. And there are scientists who have seen the autopsy results. I practice as head of the regional forensic bureau and as a professor. The fact that we have established this diagnosis – it is not just to my credit, and this is not my personal opinion. This is the opinion of specialists, morphologists and doctors in Bukovina. There are five professors in our group – I just head the group.
Original article in Russian by Anna Yashchenko here: www.unian.net/rus/news/news-346721.html
This important article highlights three different problems: First, drugs and vaccines which have NOT been either studied or approved for pregnant woman are being used as if their unique biochemical and physiological needs (remember, their bodies have adapted to the unique stress of feeding and forming another being within their own bodies) and those of the baby within can be ignored because it is more convenient to forget about them and just use drugs and vaccines that are handy, or with which the doctor is familiar. Second, marketing pressures and propaganda lead doctors and their associates to use vaccines and drugs in pregnant woman and their babies EVEN THOUGH they are know to be dangerous to these woman and their babies. Third, safe, effective and well-known treatments exist for each of the conditions for which dangerous pharmaceutical treatments are widely, and unwisely, used. For example, if there were a danger from a virus like H1N1 or from urinary tract (or other) infections, the use of nano silver would eliminate it since it safely kills pathogens while leaving vital probiotics in place without danger to the fetus or mother.
Antibiotics, psychiatric medication and vaccines are three perfect examples of dangerous drugs widely, but unwisely, used in these vulnerable people: mothers and unborn babies. In the PDR (Physicians’ Desk Reference (R) ) and package inserts pertaining to such drugs, caution is urged stating that the drugs in these classes should be used in pregnant woman, and in the case of psychiatric drugs, in women of child bearing age, only where there are no other options or when the benefit overrides the risks to mother and child.
OK. Risks are supposed to outweigh benefits. But in the case of vaccines for H1N1, what benefits? The disease is mild and inconsequential despite the hype. There is no additional risk to pregnant women and their babies from H1N1 infection unless they are treated with the dangerous antiviral. None. A close investigation of the statistics, as Dr. Russell Blaylock has provided, http://articles.mercola.com/sites/articles/archive/2009/11/03/What-We-Have-Learned-About-the-Great-Swine-Flu-Pandemic.aspx, makes that clear.
What are the risks? Well, since no testing has been done on the safety of the vaccines in pregnant women and on fetuses, the risks are, as the vaccine package inserts make clear, totally unknown. ALL multidose vials of injectable H1N1 vaccine contain mercury and the risks of mercury to the fetus are well characterized and well known. Astonishingly, the FDA and CDC now say that pregnant women should expose their fetuses to the well established dangers of mercury in order to receive the “benefits” of the H1N1 vaccines without explaining how the risks of mercury have been either eliminated or overcome.
Additionally, GSK’s vaccine is adjuvanted with squalene and under an Emergency Use Authorization, the FDA now permits its store of injectable squalene to be used as an additive to the injectable vaccines in the 90,000 injection stations. Since the only way that squalene can be drawn up and mixed with the vaccine is to add it to the mercury-containing multi-does vials, and it is the multidose vials which contain mercury, this guarantees that mothers and babies will be dosed with high doses of mercury AND squalene.
Since squalene is known to cause severe disease when injected and has previously never been approved for injection in humans, there is little or nothing known about its impact on either pregnant mothers or their babies. What is known, however, is that squalene injected at the doses which are indicated in the 1998 patents for its use, which appear to be the same doses in the planned admixture with the vaccines, can also cause to cause permanent, irreversible sterility. That means that the pregnancies these woman are carrying will be their last. Will their children also be permanently and irreversibly sterile? We do not know.
Psychiatric drugs are strongly contraindicated in pregnant woman and in women who might become pregnant. Yet the United States Congress, under the influence, I presume, of the huge numbers of pharmaceutical lobbyists and their even more vast funding abilities have passed a bill which requires psychiatric “screening” to detect and drug pregnant women and new mothers with drugs to “treat” post partum depression with drugs whose impact on the fetus and nursing child can be literally cataclysmic.
This study makes it clear that antibiotics are similarly dangerous. They, like vaccines and psychiatric drugs, have been little studies in pregnant women, but what is known makes it clearly inadvisable to use any of them in pregnancy without the strongest of indications.
The article below makes it clear that drugs taken for granted by patients and doctors for safety in pregnancy should not be lightly regarded despite the general mistaken consensus that they are safe, effective and harmless. Vaccines, antibiotics, psychiatric drugs, and, indeed, all drugs require such caution and replacement by safe, effective and widely available non-pharmaceuticals for pregnant and nursing women. My own preference, of course, as a physician who has practiced drug-free medicine and psychiatry for the best part of 40 years, is that all drugs, except those in the ER, should be so replaced.
Yours in health and freedom,
Dr. Rima
Rima E. Laibow, MD
Medical Director
Natural Solutions Foundation
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
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Common antibiotics tied to birth defects
Study: Drugs to treat urinary infections could cause heart, brain problems
Mon., Nov . 2, 2009
CHICAGO – Researchers studying antibiotics in pregnancy have found a surprising link between common drugs used to treat urinary infections with birth defectshttp://images.intellitxt.com/ast/adTypes/2.gif. Reassuringly, the most-used antibiotics in early pregnancy — penicillins — appear to be the safest.
Bacterial infections themselves can cause problems for the fetus if left unchecked, experts said, so pregnant women shouldn’t avoid antibiotics entirely. Instead, women should discuss antibiotics choices with their doctors.
The new study is the first large analysis of antibiotic use in pregnancy. It found that mothers of babies with birth defects were more likely than mothers with healthy babies to report taking two types of antibiotics during pregnancy: sulfa drugs (brand names include Thiosulfil Forte and Bactrim) and urinary germicides called nitrofurantoins (brand names include Furadantin and Macrobid).
It was the first time an association had been seen between urinary tract treatments and birth defects, said lead author Krista Crider, a geneticist with the Centers for Disease Control and Preventionhttp://images.intellitxt.com/ast/adTypes/2.gif, which funded the research. “Additional studies are going to need to be done to confirm these findings.”
Before rigorous safety testing
Used for many decades, the antibiotics in question predate the Food and Drug Administration and its requirements for rigorous safety testing. The FDAhttp://images.intellitxt.com/ast/adTypes/2.gif now grades all drugs for safety to the fetus based on available research, but rigorous studies are so lacking in many cases, that no antibiotics get the highest grade of “A.”
Sulfa drugs are the oldest antibiotics and some animal studies have found harm during pregnancy. Nitrofurantoins previously have been viewed by doctors as safe to treat urinary tract infections during pregnancy.
The study, appearing in November’s Archives of Pediatrics and Adolescent Medicine, may cause doctors to change the drugs they choose to treat pregnant women with infections. The findings were released Monday.
Dr. Susan Mehnert-Kay, a family practice doctor in Tulsa, Okla., who has written about diagnosing and managing urinary tract infections, said the research is “very interesting” and would cause her to reconsider antibiotic choices in early pregnancy.
The study is important because it looked at drugs that have been used for decades without large studies of their safety in pregnant women, said Dr. Michael Katz of the March of Dimes.
“Some physicians are not as attuned to this as they ought to be, so patients have the right to ask questions,” Katz said.
The researchers analyzed data from more than 13,000 mothers whose infants had birth defects and nearly 5,000 women who lived in the same regions with healthy babies.
The women were interviewed by phone from six weeks to two years after their pregnancies. Those who remembered taking antibiotics during the month before conception through the first three months of pregnancy were identified as exposed to antibiotics.
The women’s memories could have been faulty, a substantial weakness of the study, which the authors acknowledged. About one-third of the women who took antibiotics couldn’t remember the specific type of drug they took.
It’s also unclear whether the birth defects were caused by the drugs or by the underlying infections being treated, Crider said.
Birth defects linked to sulfa drugs included rare brain and heart problems, and shortened limbs. Those linked to nitrofurantoins included heart problems and cleft palate. The drugs seemed to double or triple the risk, depending on the defect.
“These defects are rare. Even with a threefold increase in risk, the risk for the individual is still quite low,” Crider said.
Katz of the March of Dimes said anencephaly, a fatal brain problem linked to sulfas, affects about 1 in 10,000 births in the United States. Cleft palate occurs about 20 per 10,000 births.
Crider said the findings give doctors another opportunity to caution against overuse of antibiotics. Viral illnesses like colds and flus shouldn’t be treated with antibiotics, she said.
Women in 10 states, including California, Texas and New York, were interviewed as part of the National Birth Defects Prevention Study.
The FDA recommends that pregnant women discuss medications with their doctors, said FDA spokeswoman Sandy Walsh. The agency has proposed changes to prescription drug labeling that would require more complete information for women of childbearing age, pregnant women and those who breastfeed, Walsh said.
http://msnbcmedia1.msn.com/i/msnbc/Components/Sources/Art/APTRANS.gif
Money Bomb! Rima and Bert on the Way to Codex:
http://drrimatruthreports.com/?p=3686
Health Freedom eAlert
News, alerts, and other information related to your health freedom.
Action Items You Can Take Now October 28, 2009
The Voice of Global Health Freedom™
Permalink to this blast: http://drrimatruthreports.com/?p=3903
Dr. Laibow and Gen. Stubblebine are “in the air” right now, on their way to a Codex Alimentarius (so-called, World Food Code) meeting in Germany. Stay tuned for reports, YouTube videos and tweets… www.twitter.com/healthfreedomus
Stop the Shot Law Suit: Judge Issues ‘Show Cause Order’ to Prove We Have a Right to Be in Court
There are many wrongs under the law, but not everyone has the right to contest them all. Law suits can require plaintiffs (that’s us – the people bringing the suit and making the formal complaint) to show that they have a reason to bring this suit, or, in legal terms,that we have “standing”. We believe that this Show Cause Order is a positive move that gets the issue of standing, which the other side will surely use to try to get the suit dismissed, out of the way before our November 5 hearing.
Yesterday, Judge Reggie B. Walton of the US District Court, District of Columbia, issued a “Show Cause Order” giving us 48 hours to show why we have standing so that the case 1:09-cv–1924-RBW v. U.S. Food and Drug Administration, the “STOP THE SHOT” law suit, can continue.
You can imagine that we have a team of highly skilled, dedicated lawyers and scholars working very hard, indeed right now to create . What’s at stake? Out ability to stop the FDA from releasing any more of the dangerous vaccines for a non-existent pandemic and, in fact, a powerful legal challenge against ALL influenza vaccines. They don’t work, they are not safe and they cause harm. We want them off the market.
We are doing our part to Stop the Shot. What’s your part?
You know that good immune function requires large amounts of Vitamin D. Did you know that health freedom requires the Three Vitamin D’s of Activism?
To keep your health freedom intact, you need to take large doses of them. The Three D’s of Health Freedom are:
Do
Disseminate
Donate
Do These Action Items:
1. Tell President Obama to Rescind Dangerous, Unnecessary Health Emergency giving unprecedented powers to Secretary Sebelius to set us a medical internment system without appeal or protections. Take this item once for every member of your household
http://salsa.democracyinaction.org/o/568/t/1128/p/dia/action/public/?action_KEY=1610
2. If you are a Health Care Worker, student or in any allied profession, take the Health Keeper’s Oath
now to prevent the Medical System from becoming a tool to imprison and kill as happened in Nazi Germany. Whether you are a Health Care Worker or not, forward this information to every Health Care Worker you can reach:
http://salsa.democracyinaction.org/o/568/p/dia/action/public/?action_KEY=1614
Disseminate This Information Far and Wide
Our impact is enormous because our voices are raised in a chorus millions strong. Push Back is a numbers game: you have to be right AND have might. The other side has enormous resources and buys public policy. We have the courage, the information and the will to correct that dangerous public policy and to protect ourselves from its impact. But that means spreading the word and mobilizing people who still believe that we are too small to make REAL change we can survive with happen.
Send this email to everyone you know with a brief note telling them that this is vitally important to you, and to them, as well.
Donate
Health Freedom Money Bomb
Helps to Keep Health Freedom Free!
Watch the Money Bomb here:
http://drrimatruthreports.com/?p=3686
Donate here: http://drrimatruthreports.com/?page_id=189
Our Money Bomb has given us the resources to go to Codex (we are leaving for the airport in just 6 hours as I write this) and we thank you. We’ll be there for you, observing, building alliances for health and reporting daily. Thank you.
We are not anywhere near the funding mark, however, to prosecute this case for you so that you do not have to face the threat of what these dangerous vaccines can do to you and your loved ones, or the threat of living in a society devastated by either a man-made plague or the devastation of medical gulags and a police state.
We need you continuing help, large or small. If you have already donated to help STOP THE SHOT, thank you. If not, do it now. The law suit is for us all. We all need to do our part.
All donations to the Natural Solutions Foundation are 100% tax deductible.
http://drrimatruthreports.com/?page_id=189
Thanks for taking the Triple Dose of Vitamin D!
Correction and Repeat Opportunity
In our last Health Freedom Action eAlert I told you about the book written by my remarkable friend, Dr. Leonard Coldwell, The Only Answer to Cancer. I urge you to get a copy of this remarkable book now for yourself and another for anyone you know facing the threat of cancer. But you cannot do it at the link I gave you: I made a mistake. Here is the correct link:
www.instinctbasedmedicinestore.com
Click here to watch Dr. Coldwell’s critically important video: http://www.youtube.com/user/
HealingNaturePress
Cancer is a terrifying diagnosis. Dr. Coldwell has a better idea: cure cancer quickly and permanently. I strongly suggest that you get this remarkable book into your hands.
Giving Silver to Save Silver
www.Nutronix.com/naturalsolutions
Nano Silver is safe, effective and a profound threat to the massive antibiotic industry. Most antibiotics are fed to animals to keep them alive in factory “farm” conditions, creating superbugs and sick food for you and your family. Human antibiotics are over used and increasingly ineffective. Your donations will help us prepare comments for, attend, and, we hope, testify at the EPA’s Scientific Advisory Committee 3 day hearing. Their intent is to ban Nano Silver in the US. Ours is to preserve your right to use it if you so choose. Help us keep this part of your health freedom free.
Donate Here
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Important Article
Dr. Gary Null, one of the plaintiffs in the STOP THE SHOT lawsuit, and Richard Gale have written an important summary of why the Swine Flu vaccines are a scientific travesty, including the statement from Dr. Laver, who invented influenza vaccines, saying that they are worthless. It is a must read. Click here, http://drrimatruthreports.com/?p=3901.
Thanks for your activism. Thanks for being able to handle tough facts and take action. Thanks for being the Voice of Global Health Freedom.
Oh, one more thing: Health Freedom’s Coffee. The holidays are coming – what better gift for yourself, your corporate clients, your friends and your family than Valley of the Moon Coffee, www.ValleyoftheMoonCoffee.org. It is the visible, drinkable evidence that the Natural Solutions Foundation is helping to reclaim the production of food.
We grow it without any toxic chemicals on our shade grown, GMO free, pesticide free magnificent coffee farm in the Highlands of Panama. It is Friendly Food Certified because it is friendly to the workers, the environment and you, the consumer.
Wake up to Health Freedom – Valley of the Moon Coffee. Every bag supports the Natural Solutions Foundation and is 80% tax deductible. It’s a little bit of heaven in a cup (TM) www.ValleyoftheMoonCoffee.org.
Yours in health and freedom,
Dr. Rima
Rima E. Laibow, MD
Medical Director
Natural Solutions Foundation
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
Valley of the Moon Eco Demonstration Project
www.NaturalSolutionsFoundation.org
www.Organics4U.org
www.NaturalSolutionsMarketPlace.org
Natural Solutions Foundation
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
URGENT ACTION ITEM for everyone you can reach: Say “NO!” to “Voluntary” vaccines when refusal means incarceration and indefinite quarantine. http://salsa.democracyinaction.org/o/568/campaign.jsp?campaign_KEY=27275 Sign once for every member of your household, then activate your community of influence.
Natural Solutions Foundation suing FDA to prevent release of Swine Flu vaccines. We’ll be entering our papers this week. We are restricting our suit to a narrow objection although we know that the vaccines are genocidal (see below) and worse. But we have to use what the law gives us and that is the fact that the law was broken on September 15, 2009 when the vaccines were licensed without any safety testing being completed (or even carried out).
Be aware that we are not satisfied with a mere delay, but it is where we start tactically. Winning this suit would prevent the release of the vaccines until next June or July, 2010. That is not shabby since it would give us time for more permanent action.
Federal Court Cases are expensive! Please make two recurring tax deductible donations, large or small: Click here, http://drrimatruthreports.com/?page_id=189, to make a donation ending in the number 6 to earmark you donation for the legal case. Now click the link again and make a donation ending in any other number to support the Natural Solutions Foundation so we can continue to serve you and help keep health freedom free. Thanks!
Want to support the Natural Solutions Foundation by drinking Health Freedom’s own coffee (or detoxing with it) and giving it to lucky personal and corporate recipients this Holiday season? Visit http://ValleyoftheMoonCoffee.org and Wake Up to Health Freedom (TM) with pure, clean coffee from our teaching farm in Panama’s Valley of the Moon Eco Demonstration Project, www.NaturalSolutionsFoundation.org. Want to volunteer at the Valley of the Moon? Glad to have you. Visit http://www.natsol.org.
OK. Now for the tough stuff
The article below details the horrific reality that I wish were not true. The Natural Solutions Foundation has been saying for quite some time that we see clear evidence of a genocidal intention in the overblown, clearly intentional Swine Flu “Pandemic”. When WHO moved the “Pandemic” from Level 4 to Level 5 the disease was so mild and inconsequential that they literally had to change the definition of a Pandemic at Level 5, leaving out the words “with the ability to cause serious illness and death” from the definition because it did not and could not. We believe that this must have been a great disappointment to the folks at the WHO who have been both predicting and involved with genetically engineering one failed pandemic after another. But WHO, you will remember, believes in a “sustainable planet” and that sustainability (favor them, not us, of course) means that they believe, too, that 90% of the world’s population needs to die.
Die
They do not much care how we die as long as we do it on demand and they manage to squeeze out a good dollop of profit as we do so. Some of us, however, will die because we are never born. That, too, is part of the genocidal plan. You may recall that we reported some time back that we had seen official WHO documents from 1985 stating that the real purpose of the current vaccination program taking place in Africa at that time was not disease control (they know perfectly well that vaccines are hokum, without a shred of valid scientific evidence behind them) or prevention, but the dissemination of materials which cause infertility in the women into whom it is injected. At that time, they were using vaccines with strong response patterns laced with Human Chorionic Gonadotrophin (HCG), a reproductive hormone (a glycoprotein, by the way – that figures into this true horror story a little later on). When you train the immune system through injecting it with adjuvants to “break tolerance” or attack the molecules as “not me” that it normally recognizes as “me”, if you prime it properly, you can create an immune intolerance to the hormones or other molecules of your own body.
In this case, and the same system has been used against untold millions (billions?) of women in many third world countries all over the world, the body attacks every molecule of HCG it encounters after that. The problem is that without HCG, the uterus cannot retain the embryo, or the fetus and it will expel the future baby if she were pregnant at the time of the injection. If she were not pregnant, she will never again become a mother. Her body now destroys the very hormone without which she cannot sustain a pregnancy. This damage is irreversible.
But not universal. Apparently, that is the problem: there are still a few people whose immune response is not sufficient to destroy all of their fertility. So now we move, in the march of mad science, propelled by forces of such deep inhumanity that it is difficulty to confront them with clear, calm eyes, to another infertility system.
In 1998 a Patent Application was made for a system which uses a person’s own immune system to render them permanently infertile, sterile, unable to have children. The system is irreversible, once injected.
Knowing that:
– Both Novartis and GSK vaccines “against” the trivial Swine Flu both contain 1 million times more squalene than the devastatingly dangerous Vaccine A which crippled and killed so many Gulf War I military personnel (See Squalene: Be Very Afraid Part I, http://drrimatruthreports.com/?p=3592)
– Even a few molecules of squalene injected into the body causes it to “break tolerance” and attack the body’s own molecules to which it is now trained for attack, including the body’s own squalene, a vital component of the Central Nervous System (which accounts for the profound and cataclysmic neurological symptoms of squalene injection
– The WHO, UN and US governments agree on the “need” to reduce population to only 10% of its current levels
– When the WHO declared a Level 6 Pandemic on June 11, offical control of the political and health functions of all 194 countries in the WHO passed to that body, per an agreement signed in 2005 which took effect in 2007
– The haste with which this Level 6 Pandemic was declared makes it clear that the agenda was agreed to whether or not the genetically engineered virus did its job
– FDA/CDC has said that the $1/2 billion stock pile of injectable squalene adjuvant which the US Government admitted it was stock piling will be used to add the squalene to the bodies of people receiving the vaccines which do NOT have adjuvants in them at the time of injection
– The patents for a glycoprotein-containing, squalene adjuvanted H1N1 vaccine were filed in 2007 and 2008 by Novartis, Baxter International and GSK despite the fact that the virus did not yet officially exist, there had never been approval of a squalene adjuvanted vaccine and use of squalene in mass vaccines was illegal through the permanent restraining order of Judge Emmett Sullivan and through the fact that squalene was forbidden to even be tested in the US. The investment of billions of dollars into the development of these vaccines for a virus that did not yet exist, using substances which had never been approved for use in vaccines by 3 separate companies, allegedly competitors in the vaccine industry, is worthy of note all by itself
– The most vulnerable members of society, children and pregnant women, will be vaccinated first.
Now you know what the game is. Since the goal is infertility, what better target population could you choose? With one fell swoop of a needle, a whole generation of “useless eaters” is wiped off the map – the next one while this one is too sick to make much trouble and you clean up like the bandit that you are, if, of course, you are Big Pharma and the global genocidalists!
So now we have mandates for “Influenza vaccines” which are designed to roll the “Swine Flu” up under them. Understand clearly that although your State may offer you exemptions for philosophical, religious or medical reasons, there is every liklihood that there will be NO pandemic vaccination exemptions. The way the federal and state regulations are reading right now, that is the situation. The confusers really do want you to feel
– All vaccinations will be voluntary for the pandemic flu. This is true if by voluntary you really mean “under duress and pain of incarceration, fine and imprisonment.”
– Conventional exemptions will hold for the pandemic flu. This is not true. The pandemic vaccine is governed by separate regulations and laws which do not allow for exemptions.
– Parents will be given the choice of whether to vaccinate their children and themselves or not. This is utterly false unless we take back our freedom to make these decisions for ourselves and our children. Experimental medical procedures are never carried out on the most vulnerable and defenseless first, not until now, that is.
As an aside, do you suppose that President Obama’s children will get the same vaccine that yours and mine will? How would we know? How about the President himself, who bravely agreed to wait until near the bottom of the list. How courageous and public spirited. I will be happy to join him below the bottom of the list and, if all of us have any sense at all, we will all do so by making it abundantly clear to our legislators that this WILL not happen. That is the purpose of the action item, http://salsa.democracyinaction.org/o/568/campaign.jsp?campaign_KEY=27275. So far more than 2,222,940 of your emails have reached the legislative and decision making desks of this country. These people need to hear that the deception is broken, like immune tolerance when adjuvants are injected. We want the right to determine what happens to our bodies. We will not be sickened and die for the depopulationists. We will not be made infertile for the neo-aristocrats. We will not be brought into slavery through a diabolical brew in a syringe of illness, infertility and death..
Now, please read the following article and share it widely while you take the time and effort to mobilize every single person you can reach to help mobilize the groundswell to make it impossible for the vaccine effort to go forward as intended.
Yours in health and freedom,
Dr. Rima
Rima E. Laibow, MD
Medical Director
Natural Solutions Foundation
www.HealthFreedomusa.org
www.GlobalHealthFreedom.org
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Saturday, August 8, 2009
“Swine flu” vaccine has adjuvants that impair fertility, Making people infertile is part of eugenics, thus genocide.
http://dprogram.net/2009/08/07/“swine-flu”-vaccine-has-adjuvants-that-impair-fertility/
August 7, 2009
Daniel Solis from the Czech Republic has researched the side-effects of the adjuvant, squalene, and discovered it is known to destroy fertility as well as causing other forms of damage.
A patent for a vaccine to impair fertility in animals contains squalene.
The plan to use this fertility-impairing adjuvant in the “swine flu” vaccine against a flu that has so far been far less irksome than the ordinary seasonal flu underscores concerns that this H1N1 mass vaccination programme mandated by WHO with the support of pharma companies such as Baxter is designed primarily to cause death and injury, and so significantly reduce the global population.
Is it any wonder that these “vaccines” are classified as bioweapons by the regulators? ….
Daniel Solis has also made a formal complaint against the head of the Czech Republic’s FDA and the Deputy Health Minister for awarding a contract to Baxter worth 1,5 billion CZK without an open tender. More legal action in the Czech Republic is planned with the aim of getting Baxter’s license to manufacture the “swine flu” vaccine at Bohumil suspended and to make Baxter accountable for the incident at the BioTest lab, which detected the live bird flu virus in vaccine material from Baxter on February 6th. Members of the lab had to be treated preventatively for bird flu and were put in quarantine.
Also, a Czech translation of “Evidence-of-the-Use-of-Pandemic-Flu-to-Depopulate-USA” can be found here: http://www.outsidermedia.cz/Obvinuji-Vas-z-masove-vrazdy-1.aspx
http://www.outsidermedia.cz/Obvinuji-Vas-z-pripravy-masove-vrazdy-II-1.aspx
“I have focused on the adjuvants made of monophosforyl lipid A (MPL) MF59TM (containing a polysorbate TweenTM 80) or AS03, AS04 also known as squalene in the proposed vaccines, which are immunosterilant or an immunocontraceptive,” Daniel Solis writes.
“The patent of the veterinary FERTILITY IMPAIRING VACCINE can be found on-line. It mentions both, the lipoid adjuvants squalene and the polysorbate TM80.
Here are the quotes from the patent and further some clinical studies about the toxicity of both.
(WO/1999/034825) FERTILITY IMPAIRING VACCINE AND METHOD OF USE
This application claims the benefit of U. S. Provisional Application No. 60/070,375, filed January 2,1998, U. S. Provisional Application No. 60/071,406, filed January 15,1998
“The vaccine of the invention preferably additionally includes an immunological adjuvant to enhance the immunological response of the subject to the glycoprotein antigen. Examples of adjuvants include Freund’s Complete Adjuvant, Freund’s Incomplete Adjuvant, and an adjuvant comprising an immunostimulant such as synthetic trehalose dicorynomycolate (STDCM) and an oil such as squalene oil (see P. Willis et al., J. Equine Vet. Sci., 14,364-370 (1994)). An adjuvant comprising synthetic trehalose dicorynemycolate, squalene oil, and a surfactant such as lecithin is preferred. Lecithin typically includes phosphatidyl choline. In a preferred embodiment the vaccine comprises oil, preferably a biodegradable oil such as squalene oil. Typically, the vaccine is prepared using an adjuvant concentrate which contains lecithin in squalene oil. The aqueous solution glycoprotein is typically a phosphate-buffered saline (PBS) solution, and additionally preferably contains Tween 80.”
Abstract:
A vaccine comprising an antigen derived from a zona pellucida glycoprotein is effective to impair fertility in animals, preferably carnivores. The vaccine can be used as an immunosterilant or an immunocontraceptive.
http://www.wipo.int/pctdb/en/wo.jsp?wo=1999034825
Description:
http://www.wipo.int/pctdb/en/wo.jsp?IA=US1998027658&wo=1999034825&DISPLAY=DESC
__________________________________________________________
Annals of Allergy, Asthma and Immunology, Volume 95, Number 6, December 2005 , pp. 593-599(7)
“Polysorbate 80 was identified as the causative agent for the anaphylactoid reaction of nonimmunologic origin in the patient. Conclusions: Polysorbate 80 is a ubiquitously used solubilizing agent that can cause severe nonimmunologic anaphylactoid reactions.”
Gajdova M, Jakubovsky J, Valky J.
Institute of Preventive and Clinical Medicine, Limbová, Bratislava.
Delayed effects of neonatal exposure to Tween 80 on female reproductive organs in rats. Food Chem Toxicol. 1993 Mar;31(3):183-90. PMID: 8473002.
“Baby female rats were injected with polysorbate 80 at days 4-7 after birth. It accelerated the maturing of the rats and caused changes to the vagina and womb lining, hormonal changes, ovary deformities and degenerative follicles.”
http://www.ncbi.nlm.nih.gov/pubmed/8473002
The Endogenous Adjuvant Squalene Can Induce a Chronic T-Cell-Mediated Arthritis in Rats
Barbro C. Carlson*, Åsa M. Jansson*, Anders Larsson, Anders Bucht and Johnny C. Lorentzen*
http://ajp.amjpathol.org/cgi/content/abstract/156/6/2057
__________________________________________________________
Now, how can WHO claim the adjuvants is harmless:
http://www.who.int/vaccine_safety/topics/adjuvants/squalene/questions_and_answers/en/index.html
when there is clear evidence of its effects provoking AI diseases:
ANTI-SQUALENE ANTIBODIES LINK GULF WAR SYNDROME TO ANTHRAX VACCINE
http://www.autoimmune.com/GWSGen.html
or
“Dr. Jules Freund creator of this oil-based adjuvant warned in 1956 that animals injected with his formulation developed terrible, incurable conditions: allergic aspermatogenesis (stoppage of sperm production), experimental allergic encephalomyelitis (the animal version of MS), allergic neuritis (inflammation of the nerves that can lead to paralysis) and other severe autoimmune disorders.
Source: : Gary Matsumoto, Vaccine A-The Covert Government Experiment That’s Killing our Soldiers and Why GI’s are Only the First Victims, Kapitola 3. “The Greatest Story Never Told” http://www.vaccine-a.com/excerpt.html”
Daniel Solis, Prague, Czech Republic
http://www.denikpolitika.cz/politici/daniel-solis/blog#31
http://www.czechfp.cz/site/?p=8009
Natural Solutions Foundation
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
While we still have some time, I urge you to add your voice to the nearly 2 1/4 million emails which are flooding the boxes of legislators at the State and Federal levels, secretaries Sebelius of HHS and Napolitano of DHS and the White House. Our voices are loud, and becoming louder. There is not much time to make them heard. Please go to
http://salsa.democracyinaction.org/o/568/campaign.jsp?campaign_KEY=27275 and take action once for every one of your household members, then alert everyone you can reach to do the same. The push back is softening the response of the other side and that is of enormous significance. We need to make the use of these deadly vaccines simply unthinkable. In Germany, the first of the vaccine recipients are beginning to sicken and die from the shot. In Canada, Native Americans have received body bags along with their Swine Flu kits.
There are strong, but as yet unconfirmed, reports that 5 US Navy ships are under quaratine after a 96% flu outbreak rate following vaccination IN APRIL, 2009. Note that the vaccinations for Swine Flu were said to occur 5 months before the “was enough| Swine Flu vaccine, it was ready to test, it had been manufactured and the causative organism was known. We do not yet have information on which vaccine was used, sickening and killing so many healthy young people. But we do know that wherever it is used, it is designed to create the very disease that is being hyped and sold to the world as a fear source, without a shred of solid reason.
Perhaps it was Novartis H1N1 vaccine which the FDA pulled off the market place for labeling inconsistencies in February, 2009. Not enough vaccine? Needs adjuvants to make it go around? Balderdash!
This week coming we will try to make their use illegal, as well. Since the 1964 Keffauver Bill makes it mandatory for the FDA to require that a drug or vaccine be both safe and effective before it can be approved (although we all know how very lax that is), no such testing, lax or otherwise, was carried out before the 4 vaccines approved on September 15, 2009 by Secretary Sebelius were licensed for release into the general public.
Be aware, too, that the nasal mist vaccine by Medimmune is designed to create the flu, leaving immunocompromised people, children, cancer chemotherapy and radiation patients, children and adults on asthma medication, people with eczema and any other type of immune suppression, and babies less than a year old, vulnerable to the disease which will be spread by the nasal mist vaccine. Be aware, too, that this same preparation is to be avoided by pregnant women and the people mentioned above, including young children. Hmmm. How do you do that? How do you vaccinate First Responders, health care workers and pregnant women and children and keep the virus that they are involuntarily shedding from the patients in the hospital and the babies whom this virus will sicken and kill? Clearly, you don’t. Clearly the game is to make very sure that this novel virus, classified as a “Bio weapon” by the US Government, behaves better than SARS, Avian Fly and perhaps the 1976 Swine Flu.
When we enter this case in Washington DC this week, we know that we will likely be facing enormous legal expenses. So far our lawyers have been wonderful about fees BUT we cannot expect that largess forever. An appeal in Federal Court is a huge undertaking. We need two donations from you on a recurring basis, large or small.
The first ends in the number 6 and is thus earmarked for legal funds. The second ends in any other number and will help support us as we move forward on this and both are urgently needed. Click here, http://drrimatruthreports.com/?page_id=189, to keep your health freedom team fighting for you.
Of course, you could also purchase our outstanding all natural coffee at www.ValleyoftheMooncoffee.org. It is produced as part of our teaching effort to help reclaim the production of food here at the Valley of the Moon Eco Demonstration Project in Panama. It is free of GMOs, pesticides, herbicides, fungicides, suicides and it tastes like … well, it tastes like freedom! It is Health Freedom’s own Coffee and every bag you buy not only helps us, but brings you an 80% tax deduction discount as a “Thank you!|
Now would be a great time to select www.ValleyoftheMoon.org coffee as your personal and corporate gift for the 2009 Holiday Season! Large orders? No problem! Contact Gail Coba at “Gail Coba”
Squalene: Be Afraid, Part I
The following article by Edda West was published in 2005. Given the horrific threat of squalene laced vaccines for a mythical danger concocted in a lab, it is all the more relevant now. Please take time to read and share this post and the one that follows it.
This outstanding article details the mechanism of action, and the enormous dangers, of vaccines which contain squalene in any of its forms. But bare in mind as you read this clear, and enormously important article below, that the adjuvanted vaccine approved by the US Government on September 15, 2009, in the total absence of even a shred of safety testing, will contain 1 million times more squalene than even the deadly Vaccine A.
You may have encountered the squalene story before: how injected squalene, even a few molecules of injected squalene, causes the body to attack itself on a rampage of auto immune destruction like an army gone mad and turned on its country. And that is, in fact, exactly what triggered this onslaught of destruction: the US Department of Defense decided to experiment on its citizens, healthy young men and women who had made the terrible mistake of trusting their country to take care of them while they were willing to give their lives to defend it.
Instead, they were betrayed with unsafe vaccines for (or against, it depends on whom you asked) anthrax. The tragedy was that this was no experimental surprise which was revealed for the first time when the vaccine’s terrible consequences showed up over time. No, this adjuvant, or immune response enhancer molecule was known as “Freund’s Complete Adjuvant” and was used in animal experimentation to produce cataclysmic and lethal auto immune disorders in animals. 100% of the time when they were injected.
Fast forward to today’s news: On September 15, 2009 Health and Human Services Secretary Kathleen Sebelius announced the approval, in the total absence of any safety testing, of 4 new vaccines for the novel A/H1N1 Swine Flu virus which allegedly appeared in Mexico this past April for the very first time in the world’s history.
But wait! Patents for this vaccines “against” this very virus were applied for by Medimmune (parent company to Sanofi Aventis), Novartis and Baxter International. Baxter and Novartis applied for patents using squalene-based adjuvants. Baxter and Novartis’ adjuvant of choice is called MF59, detailed in the article below as a powerful – and highly toxic – squalene compound. GSK’s adjuvant, MLP(AS04) [also identified as AS03 in company statements and, like AS01 and 2, contains MLP, or, in simple terms, squalene] is also a powerful and literally poisonous auto immune stimulant made from squalene.
Baxter knows that, as far as immune enhancement to prevent disease goes, squalene adjuvants do not even work. So we have to wonder if – hard, strong and long, if the introduction of squalene has anything to do, anything at all, with the avowed goal of preventing a pandemic.
Quoting Investigative Report Jane Burgermeister,
“On July 13th, WHO ordered the inclusion of oil-in-water adjuvants in the “swine flu” H1N1 vaccines to be distributed throughout the world this autumn on the recommendation of its vaccine advisory panel, packed with Baxter and pharmaceutical executives, in spite of the fact that clinical studies published by Baxter’s own scientific team that patented the H1N1 vaccine demonstrate that such adjuvants are, at best, useless.
‘SAGE [WHO’s advisory panel on Pandemic Vaccines, on which Baxter and other vaccine manufacturers sit – REL] recommended that promoting production and use of vaccines such as those that are formulated with oil-in-water adjuvants and live attenuated influenza vaccines was important,’ says the WHO pandemic briefing note.
http://www.who.int/csr/disease/swineflu/notes/h1n1_vaccine_20090713/en/index.html
In June 2008, Baxter’s Austrian-based scientists Ehrlich, Kistner and Barret published a clinical trial in the New England Journal of Medicine ((Previous Volume 358:2573-2584 June 12, 2008 Number 24) on the safety of an H5N1 whole-virus vaccine, in which they themselves go on record saying that the use of adjuvants did not improve the antibody response.
http://content.nejm.org/cgi/content/short/358/24/2573In spite of the evidence that adjuvants are at best useless, vaccine companies such as Baxter and Novartis are rolling out vaccines which contain adjuvants like squalene (MF59), a substance added to the anthrax vaccine given to US soldiers, causing tens of thousands of Iraq Desert Storm soldiers to suffer permanent neurological damage.
Also, WHO is reported to have advised the use of “antigen sparing” protocols which means they are calling for the use of not much virus and lots of adjuvant.
The effects of adjuvants are so destructive to the human body that some people say that adjuvants are part of the next generation of biological or pharmacological warfare.”
In Squalene: Be Afraid, Part II we will discuss what the underlying reason for this adjuvant and document why the greatest danger in this Pandemic may not even be the vaccine we all have so much reason to fear.
Yours in health and freedom,
Dr. Rima
Rima E. Laibow, MD
Medical Director
Natural Solutions Foundation
www.HealthFreedomusa.org
www.GlobalHealthFreedom.org
Valley of the Moon (TM) Eco Demonstration Project
www.NaturalSolutionsFoundation.org
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A Glimpse into the Scary World of Vaccine Adjuvants
By Edda West – Published in VRAN Newsletter – Winter 2005
Adjuvants are formulated compounds, which when combined with vaccine antigens intensify the body’s immune response. They are used to elicit an early, high and long-lasting immune response. “The chemical nature of adjuvants, their mode of action and their reactions (side effect) are highly variable in terms of how they affect the immune system and how serious their adverse effects are due to the resultant hyperactivation of the immune system. While adjuvants enable the use of less *antigen to achieve the desired immune response and reduce vaccine production costs, with few exceptions, adjuvants are foreign to the body and cause adverse reactions”, writes Australian scientist Viera Scheibner Ph.D, (1)
The most common adjuvant for human use is an aluminum salt called alum derived from aluminum hydroxide, or aluminum phosphate. A quick read of the scientific literature reveals that the neurotoxic effects of aluminum were recognized 100 years ago. Aluminum is a neurotoxicant and has been linked to Alzheimer’s disease and other neurological disorders. Prior to 1980, kidney patients undergoing long term dialysis treatments often suffered dialysis encephalopathy syndrome, the result of acute intoxication by the use of an aluminum-containing dialysate. This is now avoided using modern techniques of water purification. In preterm infants, prolonged intravenous feeding with solutions containing aluminum is associated with impaired neurologic development. Scientists speculate that aluminum neurotoxicity may be related to cell damage via free radical production, impairment of glucose metabolism, and effects on nerve signal transduction. (2) Vaccines which contain both aluminum adjuvants and mercury based preservative, greatly magnify the neurotoxic effects. (3)
Macrophagic myofasciitis (MMF) is a muscle disease first identified in 1993, and has been linked to vaccines containing aluminum adjuvants. Muscle pain is the most frequent symptom which can be localized to the limbs or be more diffuse. Other symptoms include joint pain, muscle weakness, fatigue, fever, and muscle tenderness. The disorder is associated with an altered immune system in some, but not all patients. A study published in the journal Brain (2001) revealed that 50 out of 50 patients had received vaccines against hepatitis B virus (86%), hepatitis A virus (19%) or tetanus toxoid (58%), 3-96 months (median 36 months) before biopsy. “We conclude that the MMF lesion is secondary to intramuscular injection of aluminum hydroxide-containing vaccines, shows both long-term persistence of aluminum hydroxide and an ongoing local immune reaction, and is detected in patients with systemic symptoms which appeared subsequently to vaccination”, write the authors of the study. (4)
But aluminum’s neurotoxicity is of less concern to the vaccine industry than the fact that it elicits a lesser antibody response to the so called purer recombinant or synthetic antigens used in modern day vaccines than in older style live or killed whole organism vaccines. “This has created a major need for improved and more powerful adjuvants for use in these vaccines.” (5)
For decades, vaccine developers have been tinkering with various substances to trick the body into heightened immune responses. The most effective adjuvants are formulated with oils but have long been considered too reactive for use in humans. Immunologists have known for decades that a microscopic dose of even a few molecules of adjuvant injected into the body can cause disturbances in the immune system and have known since the1930’s that oil based adjuvants are particularly dangerous, which is why their use has been restricted to experiments with animals.
The classic oil based adjuvant called Freund’s Complete Adjuvant can cause permanent organ damage and irreversible disease – specifically autoimmune diseases. When scientists want to induce autoimmune disease in a lab animal, they inject it with Freund’s Complete Adjuvant, which causes great suffering and is considered by some too inhumane to even inject into animals.
Dr. Jules Freund creator of this oil based adjuvant warned in 1956 that animals injected with his formulation developed terrible, incurable conditions: allergic aspermatogenesis (stoppage of sperm production), experimental allergic encephalomyelitis (the animal version of MS), allergic neuritis (inflammation of the nerves that can lead to paralysis) and other severe autoimmune disorders. (6)
Adjuvants can break “tolerance”, meaning they can disable the immune system to the degree that it loses its ability to distinguish what is “self” from what is foreign. Normally, the immune system ignores the constituents of one’s own body. Immunologists call this “tolerance”. But if something happens to break “tolerance”, then the immune system turns relentlessly self-destructive, attacking the body it is supposed to defend. (6)
Scientists theorize that oil based adjuvants have the ability to “hyperactivate” the immune system, and in doing so, create chaos by inducing such an extremely powerful response that the immune system literally goes haywire and starts attacking elements it would normally ignore. (6)
Another theory has to do with “specificity”. One of the great distinguishing characteristics of the immune system is something akin to a highly sensitive innate intelligence that has evolved over eons to be able to respond very precisely to what it deems to be a threat to the body. Because the body contains many types of oily molecules and lipids, it may be that when an oil is injected, the immune system responds to it not only specifically, but with heightened intensity because the oil adjuvant resembles so closely the natural oils found in the body. A “cross reaction” then happens, sending the immune system into chaos destroying any oils found anywhere in the body that resemble the adjuvant oil. Demyelinating diseases like multiple sclerosis are an example of this destructive autoimmune process. (6)
To deepen one’s understanding of the shadowy world of vaccine development, award winning investigative journalist Gary Matsumoto’s new book is a “must read.” It documents the secret human medical experimentation conducted on American citizens by doctors and scientists working for the U.S. military. It is a book about “betrayal of the most fundamental rules of medical ethics; and betrayal of the basic duty of military and civilian leaders to protect the people they govern.” Vaccine A: The Covert Government Experiment That’s Killing our Soldiers and Why GI’s are Only the First Victims, is a gripping read into the mad science world of the U.S. military’s biowarfare vaccine development program which, since 1987 has injected tens of thousands of U.S. troops with an experimental unlicensed anthrax vaccine containing squalene. An oil based adjuvant, squalene has been known for decades to cause severe autoimmune diseases in laboratory animals. Writes Matsumoto, “The unethical experiments detailed in this book are ongoing, with little prospect of being self-limiting because they have been shielded from scrutiny and public accountability by national security concerns.” Reading this book, one gets a permanent chill in the spine as we glimpse the “writing on the wall” of what is to come. (6,7)
“When UCLA Medical School’s Michael Whitehouse and Frances Beck injected squalene combined with other materials into rats and guinea pigs back in the 1970’s, few oils were more effective at causing the animal versions of arthritis and multiple sclerosis”, writes Matsumoto. In 1999, Dr. Johnny Lorentzen, an immunologist at Sweden’s Karolinska Institute proved that on injection, “otherwise benign molecules like squalene can stimulate a self-destructive immune response”, even though they occur naturally in the body. Other research institutes have also shown that the immune system makes antibodies to squalene, but only after it is injected (6) We now know that squalene, added to boost immune response in a formulation known as MF59, is the secret ingredient in certain lots of experimental anthrax vaccine that has caused devastating autoimmune diseases and death in countless Gulf War vets (Canadian, British and Australian troops were also injected with squalene laced vaccine), and continues to be used today. There is a “close match between the squalene-induced diseases in animals and those observed in humans injected with this oil: rheumatoid arthritis, multiple sclerosis and systemic lupus erythematosus”, writes Matsumoto. These three illnesses have been proven to be caused by this oil, but there is an additional long list of autoimmune diseases associated with squalene injection into humans. (6) “There are now data in more than two dozen peer-reviewed scientific papers, from ten different laboratories in the U.S., Europe, Asia and Australia, documenting that squalene-based adjuvants can induce autoimmune diseases in animals..observed in mice, rats, guinea pigs and rabbits. Sweden’s Karolinska Institute has demonstrated that squalene alone can induce the animal version of rheumatoid arthritis. The Polish Academy of Sciences has shown that in animals, squalene alone can produce catastrophic injury to the nervous system and the brain. The University of Florida Medical School has shown that in animals, squalene alone can induce production of antibodies specifically associated with systemic lupus erythematosus”, writes Matsumoto. (6)
Long List of Side Effects Referring to squalene in her extensive article on adjuvants, Dr. Scheibner writes, “This adjuvant contributed to the cascade of reactions called “Gulf War syndrome”, documented in the soldiers involved in the Gulf War. The symptoms they developed included arthritis, fibromyalgia, lymphadenopathy, rashes, photosensitive rashes, malar rashes, chronic fatigue, chronic headaches, abnormal body hair loss, non-healing skin lesions, aphthous ulcers, dizziness, weakness, memory loss, seizures, mood changes, neuropsychiatric problems, anti-thyroid effects, anemia, elevated ESR (erythrocyte sedimentation rate), systemic lupus erythematosus, multiple sclerosis, ALS (amyotrophic lateral sclerosis) also known as Lou Gehrig’s disease, Raynaud’s phenomenon, Sjorgren’s syndrome, chronic diarrhea, night sweats and low-grade fevers. (1)
Matsumoto punctuates his book with poignant interviews of military personnel who suffered many of these extreme and devastating syndromes, all of whom tested positive for anti-squalene antibodies which has become THE definitive marker for people who have been injected with this adjuvant and who have gone on to develop catastrophic diseases.
Immunologist, Dr. Pamela Asa was the first person to recognize that the autoimmune diseases she was seeing in military personnel mirrored those in experimental animals injected with oil formulated adjuvants. When she met a patient with similar autoimmune symptoms who had participated in an experimental herpes vaccine trial, who also knew he had been injected with MF59, a squalene adjuvant being used as a ‘placebo’ in that study, everything began to fall into place. Pam Asa contacted Dr. Robert Garry, a leading virologist at Tulane University Medical School, whose specialty is developing antibody tests and asked him to develop a test for the detection of anti-squalene antibodies – a test that ultimately became the most important forensic and diagnostic tool identifying patients whose autoimmune diseases followed injection with squalene laced anthrax vaccine. (6)
Juxtaposed to heart wrenching testimonies of shattered health and ruined lives is the military’s defiant stonewall and denial that a squalene laced anthrax vaccine was injected into thousands of its people without their informed consent – this despite the fact that the FDA and independent researchers have tested and identified varying amounts of squalene in specific lots of the vaccine.
Even more stunning is the fact that by 1997, hundreds of millions of dollars had already been spent testing vaccines formulated with squalene adjuvants by leading research institutes like NIH (National Institutes of Health) who tested its efficacy in HIV vaccines, the National Cancer Institute who for nearly two decades conducted research with squalene-boosted vaccines, and the National Institutes of Allergy and Infectious Diseases (NIAID) had been testing it in animals since 1988 and began human clinical trials in1991. Nineteen of NIAID’s 23 trials were for prototype HIV vaccines. Writes Matsumoto, ” Squalene adjuvants are a key ingredient in a whole new generation of vaccines intended for mass immunization around the globe.” (6)
Immune System Sees Squalene as an Enemy to Attack Researchers at Tulane Medical School and the Walter Reed Army Institute of Research “have both proven that the immune system responds specifically to the squalene molecule. Squalene’s pathway through the body has been tracked with a radioactive tracer in animals by none other than Chiron, (well known flu vaccine manufacturer) and maker of MF59, the squalene-based adjuvant, now also a component of FLUAD, an Italian influenza vaccine. (6)
The immune system does in fact “see” squalene and recognizes it as an oil molecule native to the body. The key is “route of administration”. As Gary Matsumoto says, “Squalene is not just a molecule found in a knee or elbow – it is found throughout the nervous system and the brain.” When it is injected into the body, the immune system sees it as an enemy to be attacked and eliminated.(6)
As any immunologist will tell you, the way an antigen encounters the immune system makes all the difference. You can eat squalene – no problem as it is an oil the body can easily digest. But studies in animals and humans show that injecting squalene will “galvanize the immune system into attacking it, which can produce a self-destructive cross reaction against the same molecule in the places where it occurs naturally in the body – and where it is critical to the health of the nervous system.” (6)
This phenomenon is also known as ‘molecular mimicry’, where the immune system forms antibodies against one of its own structures and will continue to attack the ‘self’ molecule in the body that resembles the one in the germ, or as is the case with squalene, an identical substance that is naturally present in the body. Once this self-destructive process begins, it never stops as the body continues to make the molecule the immune system is now trained to attack.
Another example involving autoimmune ‘molecular mimicry’ is when the immune system has been sensitized to attack myelin, the insulating fatty coating around nerve fibers which insures the smooth relay of nerve signals. The body would continue to make myelin in order to replenish and repair the protective sheath around its nerve endings. But says Matsumoto, “In the act of doing so, the body immunizes itself against itself, administering over and over again what amounts to a booster dose of something that the immune system now wants to get rid of. This vital constituent (myelin) is now the enemy, and the immune system is now programmed to obliterate it in an endless loop of self-destruction” – the process involved in MS (multiple sclerosis), and ALS (Lou Gehrig’s disease).(6)
Tying molecular mimicry to the autism epidemic, many children have regressed into autism spectrum disorders after injection with the triple live virus MMR (measles,mumps,rubella) vaccine. Dr.Vijendra Singh’s research at Utah State University suggests that auto-antibodies are attacking myelin in these children. He has shown that many autistic children have auto-antibodies to brain myelin basic protein (MBP) as well as elevated levels of measles virus antibodies. “Immunoblotting analysis showed the presence of an unusual MMR antibody in 60% (75 of 125) of autistic children, but none of the 92 normal children had this antibody. In addition, there was a positive correlation (greater than 90%) between MMR antibody and MBP auto-antibody, suggesting a causal association between MMR and brain autoimmunity in autism. This is one of the most important findings in autism to date, which prompted us to link measles virus in the etiology of the disorder”, writes Dr. Singh. (8,9,10)
Immunologist Dr. Bonnie Dunbar has also done extensive research on the mechanisms of injury inflicted by hepatitis B vaccine and has observed similar autoimmune processes involving molecular mimicry in people who developed devastating neuroimmune syndromes after injection with this vaccine. (11)
Molecular Mimicry as a Bio-Weapon Matsumoto reports that Soviet bioweaponeers used the principal of molecular mimicry in the 1980’s to engineer a ‘designer disease’ that would attack myelin. By splicing a fragment of myelin basic protein into legionella bacterium, they created what amounted to a living “nano-bomb”, which they injected into guinea pigs. What they found was that the immune system quickly cleared the legionella bacterium, but the myelin molecule, smuggled in by this microbial “Trojan horse” initiated a second wave of disease which caused experimental allergic encephalomyelitis, the animal version of MS. The Soviets recognized this creation for what it was – a biological time bomb!! (6)
“Squalene is a kind of trigger for the real biological weapon: the immune system. When the immune system’s full repertoire of cells and antibodies start attacking the tissues they are supposed to protect, the results can be catastrophic,” writes Matsumoto. His assessment is seconded by Dr. Pam Asa – “Oil adjuvants are the most insidious chemical weapon ever devised.” (6)
“Molecular mimicry, seen for its diabolical potential as a weapon by the Soviets as far back as the 1980’s, also applies to squalene. But the real problem with using squalene, of course, is not that it mimics a molecule found in the body; it is the same molecule,” writes Matsumoto. “So what American scientists conceived as a vaccine booster was another “nano-bomb”, instigating chronic, unpredictable and debilitating disease. When the NIH (National Institutes of Health) argued that squalene would be safe because it is native to the body, just the opposite was true. Squalene’s natural presence in the body made it one of the most dangerous molecules ever injected into man!” (6)
The main proponents for the use of squalene in vaccines have been the U.S Department of Defense and the NIH. The anti-squalene antibodies in sick American and British military personnel are evidence that military experimentation has caused an unprecedented health catastrophe in tens of thousands of people onto whom the vaccine was forced and who were denied the right to make an informed decision based on existing scientific knowledge of the dangers of injecting squalene. “By adding squalene to their new anthrax vaccine, they did not make a better vaccine, they made a biological weapon.” (6) .
Why , one would obviously ask, would anyone knowingly inject such a dangerous substance into humans? Certainly in terms of the U.S. military’s decision, they chose to turn a blind eye to the existing science, which for decades had documented the immune destructive properties of squalene. They justified its use because they knew they had a weak and ineffective vaccine which needed a serious boost. In the face of weaponized biowarfare agents like anthrax already developed by Russia and fear that it was also possessed by Iraq, they were desperate to increase the vaccine’s effectiveness as they launched into the first Gulf War. Additionally, explains Matsumoto, “scientists in the United States are now literally invested in squalene. Army scientists who developed the second generation anthrax vaccine have reputations to protect and licensing fees to reap for the army..[and] .worldwide rights to develop and commercialize the new recombinant vaccine for anthrax.” (6)
He goes on to explain, “the National Institutes of Health (NIH) has been supporting both animal and human research with squalene since the 1980’s. Squalene has become perhaps the most ubiquitous oil adjuvant on the planet, which is something that should concern everyone. Many of the cutting edge vaccines currently in development by the NIH and its corporate partners contain squalene in one formulation or another. There is squalene in the prototype recombinant vaccines for HIV, malaria, herpes, influenza, cytomegalovirus and human papillomavirus. Some of these prototypes like HIV, malaria and influenza are intended for mass immunization around the globe.” (6)
Squalene Adjuvants Enter the Global Market FLUAD, the squalene boosted flu vaccine has been licensed in Italy since 1997. It contains MF59, the squalene adjuvant made by Chiron. Although all the published papers co-authored by Chiron-employed scientists and Italian researchers have reported MF59 to be safe, Gary Matsumoto suggests a flaw in study designs may “prevent researchers from seeing the vaccine’s real risks.” Testing of FLUAD was limited to elderly people in nursing homes – average age was 71.5 which would tend to obscure autoimmune problems that might arise for a number of reasons. If autoimmune symptoms like joint pain and fatigue did occur in geriatric Italians, doctors might not connect these complaints to anything but old age. (6)
“Autoimmunity is notorious for taking years to diagnose because the early symptoms (e.g. headaches, joint and muscle pain and fatigue) are so vague; primary care physicians often fail to recognize it…a large Phase lV trial did not even bother to analyze the “common-post immunization reactions” in study participants, recording only those adverse events severe enough to require a doctor’s visit within 7 days of immunization.” In another study patients were observed for 180 days, but only serious events like “admission to hospital or death” qualified as a reaction – nothing else was recorded. Symptoms of adverse reactions listed in the FLUAD package insert are almost identical to the Air Force case-definition for Gulf War Syndrome, and include rashes, malaise, fever, myalgia, arthralgia, weakness, sweating and various autoimmune reactions and neurologic disturbances. (6)
“The question is whether scientists working for pharmaceutical companies are intentionally designing studies so as to miss adverse reactions that inconvenience their marketing strategy?” asks Matsumoto. “Chiron’s conclusion about squalene’s safety are at odds with recent data from studies in both animals and humans.” (6)
Just in from the newslists on February 9, 2005 is an item informing of the European “debut” of a new adjuvant approved for use in a new high-potency hepatitis B vaccine. Fendrix, the new enhanced hepB vaccine is being launched by pharma giant GlaxoSmithKline for use in people with poor immune responses (like dialysis patients) and those at high risk for developing hepatitis B. It is formulated with a new adjuvant that can “significantly improve the effectiveness of immunizations.” AS04, the ‘proprietary’ adjuvant based on MPL, originally developed by U.S. company Corixa, “increases the immune potency of the new vaccine, allowing two dose administration rather than three. It has been shown clinically to be more effective than alum, the most widely used adjuvant in vaccines.” (12)
So what exactly is this new high potency adjuvant? We’re told by the press release that MPL (AS04), is a “derivative of the lipid A molecule found in Gram-negative bacteria, is extracted from bacterial cell walls and is one of the most potent regulators of the immune response, used by the body to alert itself to bacterial infections.”(12) Full name of the lipid is monophosphoryl lipid A (MPL)
This news should put everyone on high alert because guess what? Lipids are oils/fatty acids and according to Matsumoto, MPL is identified in declassified documents as one of two squalene emulsions used in the Army’s new “recombinant protective antigen anthrax vaccine (rPA) which the FDA, the National Institutes of Health (NIH) and the Department of Defense fast-tracked into clinical trials in1998. The other squalene adjuvant they used was Chiron’s MF59. (6)
It appears that Fendrix is only the first of a whole new generation of “enhanced potency” vaccines coming down the pipeline using the new high potency lipid adjuvant, MPL. “The adjuvant is also being used in a number of GSK’s developmental vaccines, including one that could be the first effective vaccine for malaria”, says the article. MPL (AS04) adjuvant is also a component of GSK Bio’s genital herpes vaccine, as well as a component in their cervical cancer vaccine and a new tuberculosis vaccine.” (12)
In the unraveling of the squalene story, we find that a squalene emulsion first known as Triple Mix (based on Freund’s adjuvant) was later given the commercial name “Ribi”. Triple Mix (renamed Ribi) was tested by Dutch scientists on rabbits who found it caused “severe effects the largest number and most severe lesions when compared with the other adjuvants.”(6) Then in June 1999, Ribi ImmunoChem its manufacturer was acquired by Corixa Corporation for $56.3 million, who presumably also own the Ribi formulation. Whether MPL(AS04) is a formula related to Ribi is undoubtedly “proprietary” information, but from Matsumoto’s reseasrch, we know they are all squalene based. And it doesn’t end there. MPL, Corixa’s multi-million dollar baby, is slated for inclusion not only in the “enhanced potency” vaccines already mentioned, but will also be a strategic component of new allergy and autoimmune vaccines in development. (13)
From their inception, mass vaccinations have acted as a biological weapon, undermining health, manipulating and crippling the immune system, and instigating cycles of new and debilitating diseases. Monopoly medicine’s solution? Inject us with more powerful, genetically engineered high potency vaccines. Never mind they are seeding us with “nano-bombs” that will further attack our already compromised immune systems.
The concept of stimulating a hyperactive immune response by using oil-based adjuvants has clearly backfired since we now know that the stronger the antigenic response, the more damaging the adjuvant itself is to the normal functioning of the brain and nervous system. The precedent for mass medical experimentation via an ever increasing recommended vaccine schedule has been set. We can now predict the grim future of mankind: an epidemic of neurological disorders and autoimmune diseases never before imagined.
Notes & Resources
Adjuvants listed by Scheibner: “Today the most common adjuvants for human use are aluminum hydroxide, aluminum phosphate and calcium phosphate. However, there are a number of other adjuvants based on oil emulsions, products from bacteria (their synthetic derivatives as well as liposomes) or gram-negative bacteria, endotoxins, cholesterol, fatty acids, aliphatic amines, paraffinic and vegetable oils. Recently, monophosphoryl lipid A, ISCOMs with Quil-A, and Syntex adjuvant formulations (SAFs) containing the threonyl derivative or muramyl dipeptide have been under consideration for use in human vaccines
*Definition of Antigen (Scheibner): “Micro-organisms, either bacteria or viruses, thought to be causing certain infectious diseases and which the vaccine is supposed to prevent. These are whole-cell proteins or just the broken-cell protein envelopes, and are called antigens”
1.Viera Scheibner, Ph.D, The Adverse Effects of Adjuvants in Vaccines, Nexus Magazine Dec. 2000 vol.8, No.1
http://www.whale.to/vaccine/adjuvants.html
2. Aluminum Toxicity notes from Dr. Boyd Haley Toxic Test Foundation website: http://www.altcorp.com/DentalInformation/aluminumvaccines.htm
3. Boyd E. Haley, Professor of Chemistry: Thimerosal Containing Vaccines and Neurodevelopment Outcomes: http://64.41.99.118/vran/vaccines/mercury/mer_haley.htm
4. Brain, Vol. 124, No. 9, 1821-1831, September 2001, 2001 Oxford University Press http://brain.oupjournals.org/cgi/content/abstract/124/9/1821
5 Vaccine Adjuvants: current state and future trends, Volume 82: Issue Immunology and Cell Biology http://www.blackwellpublishing.com/abstract.asp ?ref=0818-9641&vid=82&iid=5&aid=5&s=&site=1
6.Gary Matsumoto, Vaccine A-
7.Gary Matsumoto Press Release and biography: www.vaccine-a.com
8 Vijendra K Singh, Ph.D, Abnormal Measles Serology and Autoimmunity in Autistic Children – Journal of Allergy & Clinical Immunol, 109 (1): S232, January 2002
9. Vijendra Singh – lecture at ATEDM Conference: http://iquebec.ifrance.com/autismemtl/2002/program_en.html
10. Institute of Medicine Meeting (IOM) on Vaccines and Autism, February 9, 2004
11.. Bonnie Dunbar, Ph.D – articles and research proposal – VRAN website: http://64.41.99.118/vran/vaccines/hepatitis/dunbar_research.htm
12.New adjuvant debuts in new hep B vaccine , February 9, 2005, In-Pharma Technologist.com http://www.in-pharmatechnologist.com/news/news-ng.asp ?n=57959-new-adjuvant-debuts
13. Corixa weblink to MPL press release on allergy & autoimmune applications: http://www.corixa.com/default.asp?pid=auto_capsule&id=22