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Archive for medical hazards – Page 4

Petrochemical Detox Information

By Administrator on June 30, 2010 No Comments

Natural Solutions Foundation
The Voice of Global Health Freedom™
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
July 1, 2010

YOUR TOXIC ENVIRONMENT AND YOUR FREEDOM…

As an environmental physician, Dr. Rima has warned about the threats to our health, especially the health of children, from the increasing toxification of our environment. Among these threats we include GMO (genetically modified) products, vaccine toxins and all sorts of toxic industrial chemicals allowed to contaminate our environment. Sadly, we must now add the petrochemical soup being brewed in the Gulf of Mexico as gushing crude is admixed with all sorts of contaminants in a desperate attempt to save the oil well and field for future Big Oil profits. As a public service, we repost this powerful discussion of Therapies for Airborne Poisons.

Therapies for Airborne Poisons
Marc Sircus

The IMVA is doing what no other medical or health organization is doing – sending out an emergency alert to doctors to prepare for a serious public health threat from aerosolized oil and associated gases. This report and treatment recommendations are meant to maximize survival and health under adverse environmental conditions. The key to avoiding long-term harm is to help the body deal with the chemical assault from the very first moments when one notices foul smell, taste or flu-like symptoms.

When exposure to toxins is dramatically increased, as is the case for people in the Gulf area, the body rapidly becomes overwhelmed and the detoxification pathways normally used to excrete toxins cannot keep up with the exposure. It is well known that airborne toxins documented to be present in a number of Gulf communities are at levels that are many times the maximum allowed by the EPA.

These toxins are coming from both the oil leak and from the chemical dispersants being used to mitigate the accumulation of oil on the water surface. When the body becomes overwhelmed by this level of exposure, it will then “scramble” to store these excess fat soluble toxins in fat cells throughout the body. As these toxins accumulate, the increasing toxic burden can trigger a multitude of health problems.

This document suggests emergency medical treatments with safe non-toxic substances for anyone feeling the signs and symptoms being reported in the Gulf region. The offered protocol outlines basic treatments to capitalize on the body’s own ability to excrete toxic oil substances. By assisting the body in eliminating these toxins before they build up to critical levels, we can protect ourselves from developing the health challenges associated with exposure to these toxins. The process of detoxification is just that – a process. It is imperative to assist the body in eliminating these toxins.

See this map of complaints to see what geographic areas are most threatened.

Today we smelled for about the tenth time in a couple of months a chemical smell. It smells a bit like paint thinner- not an oil smell. We seem to smell this on less windy days here in NOLA. Usually the smell lasts a few hours, but today it was most of the day. Today is June 27.

Emergency medical treatments should be initiated immediately if you want to neutralize the hazardous toxicity from the beginning before too much damage is done. Don’t listen to any doctor or healthcare official who says negative effects are temporary. If you can smell it you are in danger. When you are poisoned with oil compounds, some of which are the nastiest chemicals on earth, like benzene, the damage is deep enough to breakup your DNA. Dr. Blanca Laffon at the University of A Coruna in Spain tested several hundred cleanup workers, both professionals and volunteers, for evidence of DNA damage in the nuclei of their cells. Laffon says exposure to oil did induce DNA damage that was greater in those with more exposure. So again do not listen to anyone who suggests exposure is not dangerous to your long-term health.

Dan Rather, reporting in the Huffington Post, says (incorrectly), “What will be the long-term effects of those large oil plumes, now called clouds, far below the surface? We don’t know. What is the toxicity of all that chemical dispersant being used at the site of the gusher and in the open waters of the Gulf? We don’t know.” We do know and the medical community has to know with precision what is going on or our ignorance is going to hurt a lot of people. We can look at worse-case scenarios and see situations that exceed anything medicine has ever faced. It is ill-prepared for this emergency that will gather itself up with each million gallons more leaked into the Gulf.

The United States government should organize a worldwide effort to provide to the citizens of the affected area large tonnages of sodium bicarbonate and magnesium salts of different types. Clay also should be provided for both internal and external cleansing. Glutathione suppositories need to be taken instantly upon symptom onset. For intense exposure, glutathione IVs are required; selenium IVs should be high on the list as well, though oral dosing will do for mild cases. Highly concentrated medicinal baths with baking soda and magnesium is also an excellent emergency procedure that can be done at home. The government needs to be called in or perhaps some rich family will have a heart and organize relief efforts for the exposed. Some organized help is necessary for if even only a small percent of the people in affected areas try to order necessary supplies stocks will be overwhelmed quite quickly.

There are several ways to increase your glutathione levels. It is a good idea to proceed slowly at first if your glutathione has been depleted for an extended period of time (months to years), because toxins and infections may have been allowed to build up in the absence of sufficient glutathione to keep them under control. If glutathione is then brought up rapidly, the mobilization of toxins can produce a Jarisch Herxheimer reaction, which is an exacerbation of symptoms that can make a person feel very unpleasant.

Intravenous glutathione is best for emergency application but our recommendation for treating Gulf Toxicity Syndrome is to use suppositories, which are about 60 percent as effective as IVs. Transdermal application would probably come in at around 40 percent with oral glutathione supplements being of questionable use. The highly vascular intestines provide a perfect way for beneficial substances to be absorbed into the bloodstream without being broken down by the stomach’s acids or deactivated by the enzymes in the liver. My recommendation is to start doses at one suppository a day of 500 mg to monitor for reactions, then work up to 3-4 a day if exposure levels are high, and do this for an extended period of time.

The foundation of our protocol is based in nutritional not pharmaceutical medicine. Using toxic drugs on top of the toxic exposure does not make any sense. People new to this type of medicine might be comforted to know that some of the best emergency room and intensive care medicines are in reality nutritional medicines. Sodium bicarbonate and magnesium chloride are both used to save lives every day but the medical industrial complex does not like to brag about this because there is no money in these common substances. We have a real problem though for doctors can’t hold an intelligent conversation about nutrition.

“For every molecule of pesticide that your body detoxifies, you throw away or use up forever a molecule of glutathione, magnesium and more,” says Dr. Sherry Rogers, who goes on to say that, “Your body uses nutrients to make this glutathione and it uses up energy as well. Every time we detoxify a chemical, we use up, lose, throw away forever a certain amount of nutrients.”

Under No Circumstance Underestimate the Danger

“People, including pregnant women, can be exposed to these chemicals by breathing them (air), by swallowing them (water, food), or by touching them (skin). If possible, everyone, including pregnant women, should avoid the oil and spill-affected areas,” writes the CDC (Center for Disease Control). They suggest that people stay indoors and turn their air conditioners to internal venting to avoid exposure when they can smell it.

The President’s Cancer Panel issued a landmark report last month suggesting that public health officials have “grossly underestimated” the extent of environmentally-induced cancer among the 1.5 million Americans diagnosed with the disease annually. So don’t believe a word more you read on the CDC site for surrounding their clear statement of warning and danger – everything else they say detracts and makes light of the threat.

Acute inhalation exposure to high levels of methylene chloride in humans has resulted in effects on the central nervous system (CNS) including decreased visual, auditory, and psychomotor functions.” – EPA

Protocol

This document outlines a basic core protocol using, in order of priority: sodium bicarbonate, magnesium chloride, selenium, glutathione, clay, concentrated superfoods like spirulina and chlorella, and formulations like Rejuvenate. The entire cadre of essential nutrients is needed for detoxification to work properly (e.g. vitamins, minerals, essential fats, antioxidants such as vitamin C and bioflavonoids). Most of these are in the spirulina and chlorella, but many more are in the Rejuvenate, which tastes a whole lot better.

Sodium bicarbonate is a vitally important part of the detoxification process because of its ability to modulate body pH. But that is only one of the many reasons everyone needs to turn their attention to the single most helpful substance in an environmental disaster. That good old Arm and Hammer baking soda can save the day. It is very important for doctors to know that even a slightly over acidity in the body can impede detoxification.

Activated charcoal and distilled (or other very pure water) are other super essential substances to have on hand to maximize the body’s ability to excrete highly toxic oil gases. Instructions on teaching people how to make homemade gas masks is on the list of poison gas threats so one will really need that charcoal for anyone downwind of the Gulf disaster. A testimony in John Dinsley book Charcoal Remedies tells an important story about severe benzene exposure. “After taking the charcoal capsules, I made an appointment with my family doctor. I told him about the benzene and asked for another blood test. When the test came back a week later, it showed that I had no benzene in my system.” There is also the coffee enema (organic), which detoxifies the liver, our most important toxin filter.

According to Parris Kidd, PhD and nutritional researcher, “Detoxification capacity varies widely from person to person and what one person can effectively detoxify may cause liver damage or cancer in another. The liver relies heavily on antioxidants and antioxidant cofactors for its detoxification work, so supplementation with vitamins B (complex), C, E, and glutathione precursors have top priority.”[1] Dr. Kidd recommends glutathione precursors alpha-lipoic acid (100 mg/day) and N-acetylcysteine (600 mg/day) along with B, E and C vitamins, phosphatidylcholine and taurine.

The Rejuvenate formulas cover all of this nutritional territory in a most superb way. Spirulina and chlorella cover most but they do not contain any C. Full hydration with pure fluids is absolutely essential in any detoxification protocol thus organic juice fasts or eating very lightly as one flushes and nourishes the system with fluids with these superfoods dissolved is central to an effective protocol. Dr. Leonard Mehlmauer, a naturopath says that, “Each case would be different but diet would be a primary medical tool with the use of pure and raw liquids playing a large part in recovery. The more severe cases would very likely go on all pure raw liquids, especially green smoothies laced with superfoods.”

One needs to know how vitally important magnesium and selenium are for increasing glutathione, the cornerstone enzyme that we need to detoxify chemicals and heavy metals from our body’s tissues. Order a supply of glutathione suppositories as well as supplies for IVs if you are a doctor that uses them. Activated charcoal should also be brought into the area in large quantities for it holds the potential to help a lot of people in the Gulf Region.

It is crucially important that in our diagnostic model of Gulf Toxicity Syndrome the local populations of the southern states are already exposed to the highest airborne mercury levels; so these people’s toxic levels are unusually high and their immune and detoxification systems are unusually low. Glutathione levels have been diminished and then crashed down even further due to inhaled VOCs. Thus, replenishing glutathione levels quickly is an essential foundation for appropriate emergency and long-term treatment.

Dr. Garry Gordon agrees, suggesting, “IV Glutathione is at the top of the list for effective detoxification for virtually every toxic exposure. Those who are already showing serious symptoms need IV glutathione and vitamin C and extra magnesium – often called a MYER’s cocktail. The doses of C we like are from 8 to 16 grams a day and there are specialized products that most people can tolerate in those higher levels without upsetting the intestine too much. When we give vitamin C IVs we use from 25 to 100 grams in a slow drip and do this 2-4 times a week for as long as needed; but always use high dosages of oral C too. I am very impressed with NAC (N-acetyl cysteine); take 500-600 mg capsules at least twice a day for a few months.

A great part of the idea is to increase cell adaptability and resistance to chemical stress, open detoxification pathways, increase cell wall permeability to allow more nutrients to enter and toxic wastes to exit, increase available glutathione, and provide a large influx of minerals that will increase enzyme activity and help neutralize heavy metals and noxious chemicals from the system. We concentrate on high oral intake of medicinals with high ORAC values. The idea is to increase Oxygen Radical Absorption Capacity (ORAC), an assay that measures the degree of inhibition of peroxy-radical-induced oxidation by the compounds of interest in a chemical milieu. One of the Rejuvenate formulas has an ORAC reading of 14,300 for a 41-gram serving. An equal amount of spirulina measures around 3,600. For reference sake approximately 5 servings of fruits and vegetables would typically have an ORAC value in the range of 3,000-5000 units.

There are many ways that spirulina and chlorella helps us and both have always been known to facilitate detoxification during fasting and thus they are also very useful during chelation. One of their functions, through their high concentration of amino acids and carotenes, is to raise glutathione levels, thus reducing kidney and liver toxicity caused by the heavy metals, pharmaceutical drugs and other toxins. One of the reasons that spirulina and chlorella are so effective in cases of radioactivity is the discovery that they do in fact increase glutathione levels.[2]

A large adult man would probably want to take as many as fifty tablets of 500 mgs of spirulina or chlorella (25 grams) but would have to work up to that and be taking lots of fluids. With a Rejuvenate I would easily double or triple the serving, which would then add up to 90 grams. This gets expensive and British Petroleum should be paying for all of this but they won’t of course.

The influence of spirulina extracts significantly increased GSH (glutathione) levels compared with untreated cells according to Dr. H. Hana et al at the National Research Center in Cairo, Egypt. The GSH level of untreated cells was 6.1µg10G cells while those treated with S. plantensis and S. maxima increased the GSH level to 70.32µg10G and even higher. Mike Adams recommends taking chlorella powder in a jar of strong unsweetened lime or lemon water creating a mix that bypasses the unpleasant taste.

Detoxification through the skin is also a very important pathway for healing oneself from chemical overexposure. Besides the bicarbonate and magnesium salt baths the two most useful methods of transdermal elimination are clay baths or clay packs and saunas. Taking a clay bath is one of the most effective methods in existence to help assist the body in the elimination of toxic substances which have accumulated in the body. Applied over one’s organs, such as the liver, clay poultices and packs aid in detoxification and not quite as messy as a bath. Once you have used the clay, it will be full of toxins, so please dispose of it and wash your skin off with a good natural soap.

Clay is very important to have on hand for medical, environmental and nuclear emergencies. Clay baths are a very strong way of removing heavy metals from the body and would increase our chances of survival if exposed to nuclear fallout. In addition, clay can be ingested and is very effective in removing toxins through the process of elimination. For ingestion, I recommend the daily use of a product called Edible Clay from LL’s Magnetic Clay. The use of clay for both internal and external use puts in our hands the healing power of mother earth and there is little that can compare or compete in the world of medicine.I explain this fully in my recent essay Edible Clay; Healing with Mother Earth. For general health, one heaping teaspoon of Edible Earth in an 8 oz glass of water daily is sufficient. And study your iodine, you will need that on hand as well.

Far Infrared saunas (FIR) in particular stimulate multiple pathways in the body including the liver detoxification metabolic pathways. They also supports kidney filtration and elimination. Most importantly far infrared sauna triggers subcutaneous toxin release via perspiration – thereby bringing “online” this additional detoxification pathway. Families and organizations can share the cost of a FIR sauna, which can be used round the clock by many when situations call for such use.

First Steps

One can be overwhelmed when first introduced to nutritional medicine, detoxification principles and chelation of heavy metals. There is a lot to learn and a lot of people say different things about it. Orthodox medicine has taken a strong stand against any of these processes so it will be impotent in its response to this expanding health nightmare. Almost forty thousand people are working in or around the Gulf and a few million on shore are in harm’s way.

The average life span of a person who did cleanup on the Exxon Valdez is 51 years meaning almost all of them are already dead yet British Petroleum is not informing doctors nor making communications that help the public.

It’s important to always remember that the first rule is to avoid exposure for even the very best protocol cannot save you if you have been hit by a toxic truck. When told by the CDC not to touch the oil it is good to remember one of the greatest lessons in the field of toxicology. There once was a scientist, Karen Wetterhahn who was an internationally respected Professor of Chemistry, an expert researcher in the field of the effects of heavy metals upon living systems, especially in their role in causing cancer. Wetterhahn spilling a drop or two of Dimethylmercury ((CH3)2Hg) on her gloved hand. Less than a year later, she was dead from the effects of mercury poisoning.

Dimethylmercury, a colorless liquid, is one of the strongest known neurotoxins. It is described as having a slightly sweet smell, although inhaling enough vapors to detect its odor would be extremely hazardous. Test showed subsequently that Dimethylmercury would have penetrated the glove and started entering her skin within 15 seconds.

Shortly after the accident she began to notice definite symptoms that worried her – tingly fingers and toes, slurred speech. She began to have problems with her balance and her field of vision started to shrink. When one is exposed to oil smell and its accompanying chemicals or even oil on the beach or in puddles from rainfall should beware and take great care. Though oil toxicity might not be as dangerous as Dimethylmercury one should remember the lessons of Karen Wetterhahn, who was wearing protective gear. It was a great lesson because no one dreamed it was as dangerous as it is and they are repeating the same mistake in the Gulf.

A new chemical dispersant is being used in the cleanup effort — it’s toxic, it’s largely experimental, and it’s being sprayed in abundance into the ocean. It’s unclear at this point what exactly its long term impact on life. The active ingredient of the toxic chemical dispersant is a neurotoxin pesticide that is acutely toxic to both human and aquatic life, causes cancer, causes damage to internal organs such as the liver and kidneys simply by absorbing it through the skin and may cause reproductive side effects. The main ingredients of Corexit it is 2-Butoxyethanol, which is known to cause cancer, birth defects and has been found to cause genetic mutations and is a delayed chronic health hazard as well as an environmental hazardous material. Corexit also contains Arsenic, Cadmium, Chromium, Mercury, and Cyanide.

My suggestion for first steps is to read our site on sodium bicarbonate and then on magnesium chloride. Purchase and immediately get familiar with what is called magnesium oil and learn about trans-dermal medicine, for that’s how these medicinals are best applied. If you’re anywhere near where the wind could blow the poisons that are gathering in and above the Gulf, go to Costco or the supermarket and buy fifty pounds of bicarbonate, you just might need it. The affected area will eventually include much of the southern and southeastern United States – probably an area that includes upwards of 50 million people, so expect supplies to sell out from all possible domestic sources very quickly for most of the substances if this information gets out and the oil flow is not stopped, which no one at this point is indicating or promising.

Mark Sircus Ac., OMD
Director International Medical Veritas Association
http://publications.imva.info
http://blog.imva.info

[1] www.dockidd.com/articals/freedom.htmn
[2] Spirulina Species as a Source of Carotenoids and “-Tocopherol and its Anticarcinoma Factors. Hanaa H. Abd El-Baky, Farouk K. El Baz and Gamal S. El-Baroty National Research Center, Dokki, Cairo, Egypt Department of Biochemistry, Faculty of Agriculture, Cairo University, Egypt. Biotechnology, Volume 2 Number 3: 222-240, 2003 ISSN 1682-2978
www.ansinet.org/fulltext/biotech/biotech23222-240.pdf

Legal Notice:The Author specifically invokes the First Amendment rights of freedom of speech and of the press without prejudice. The information written is published for informational purposes only under the rights guaranteed by the First Amendment of the Constitution for the United States of America, and should not in any way be used as a substitute for the advice of a physician or other licensed health care practitioner. The statements contained herein have not been evaluated by the FDA. The products discussed herein are not intended to diagnose, cure, prevent or treat any disease. Images, text and logic are copyright protected. ALL rights are explicitly reserved without prejudice, and no part of this essay may be reproduced except by written consent. ©2009 by Mark Sircus

Copyright © IMVA International Medical Veritas Association 2009 all rights reserved
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Categories : Activism, Blog / Vlog, Disinformation, Get Involved, Medical Hazards, The Law & CODEX
Tags : Disinformation, Dr. Rima, Food Safety, Health, health freedom, Health Hazards, medical hazards, Natural Solutions Foundation, NSF, Rima E. Laibow, Rima E. Laibow MD, USDA

Are You Making A Difference Through the Natural Solutions Foundation?

By Administrator on June 27, 2010 No Comments

Natural Solutions Foundation
The Voice of Global Health Freedom™
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
Dr. Rima Reports: http://drrimatruthreports.com/?p=4850
DrRima.net

June 27, 2010

David Korten is both a change agent and an observer of change. He has written a provocative article called, :The Big Picture: 5 Ways to Know if You’re Making a Difference”.

He says that if you can answer “YES!” to ONE of the following criteria, you are making a difference.

Here are his criteria, taken from the article which you can read below:

1. Does it help discredit a false cultural story fabricated to legitimize relationships of domination and exploitation and to replace it with a true story describing unrealized possibilities for growing the real wealth of healthy communities?

2. Is it connecting others of the movement’s millions of leaders who didn’t previously know one another, helping them find common cause and build relationships of mutual trust that allow them to speak honestly from their hearts and to know that they can call on one another for support when needed?

3. Is it creating and expanding liberated social spaces in which people experience the freedom and support to experiment with living the creative, cooperative, self-organizing relationships of the new story they seek to bring into the larger culture?

4. Is it providing a public demonstration of the possibilities of a real-wealth economy?

5. Is it mobilizing support for a rule change that will shift the balance of power from the people and institutions of the Wall Street phantom-wealth economy to the people and institutions of living-wealth Main Street economies?

You, through the Natural Solutions Foundation, can answer
1. YES!!
2. YES!!
3. YES!!
4. YES!!
5. YES!! to this excellent assay of effectiveness.

Check out just a few of our accomplishments below and here, http://drrimatruthreports.com/?page_id=195. These accomplishments are yours and ours, together, because without you, there would be no meaning to our work. It is the community of empowered people that makes a difference, and that is what you, and we, are, together.

Frankly, our “Accomplishments” page is out of date because the Trustees of the Natural Solutions Foundation do not have time to get it up to date without taking time away from our rapid, profound and widely focused forward movement.

Consider: Our Codex eBook, http://drrimatruthreports.com/?page_id=220, was the first document to outline exactly how every country in the world, including, of course, the US!, could move to a higher standard for every class of food than Codex (which would not be hard!) without the dreaded World Trade Organization trade sanctions which are the club Codex waves to subdue countries that balk at degrading their food supply to make the globalists happy while their people die, just as we do, from toxic, degraded food and nutrients whose doses are so low that they have no beneficial impact worth noting – by design!

Our Codex DVD, “Nutricide“, http://drrimatruthreports.com/?page_id=156, is the lecture that has helped millions of people, including Codex delegates!, understand what Codex is about by understanding where it came from!

Our trips to the poorest countries all over the world resulted, for example, in their trusting our leadership so that we were able to block the US government’s attempt to get fluoride approved for inclusion at high levels in infant formula for normal babies at the Codex Committee for Nutrition and Foods for Special Dietary Uses (Thailand, 2007). This, alone, is a major victory in policy change!

The Natural Solutions Foundation, with its radio show, the Dr. Rima Reports, www.BlogTalkRadio.com/FreedomizerRadio, 9 PM to Midnight Eastern Standard Time, every Sunday night, is getting information out. Just look at the lineup of guests for the next couple of months! http://drrimatruthreports.com/?p=4850

Our Action Items generate hundreds of thousands to millions of your emails to decision makers!

Our Blogs are widely circulated and passed from reader to reader around the world!

Our Videos, like
Nutricide, http://video.google.com/videoplay?docid=-5266884912495233634#
Should the US Get Out of Codex? http://www.youtube.com/watch?v=AfCni-LuR_c
The Globalist Genocidal Agenda, http://www.youtube.com/watch?v=Y8f2P4GCJL8&feature=related
and dozens of others at www.Youtube.com/NaturalSolutions give people deeply researched, and deeply important information that they can use and share, changing local and leadership opinion. They, too, are passed from person to person around the world!

Radio appearances (on shows like Alex Jones, Jeff Rense and dozens of others), documentary film appearances (like “Making a Killing, Psychiatry, Industry of Death, and two of Governor Jesse Ventura’s Conspiracy Theories episodes, and other public information activities get the word out there. Uniquely, Natural Solutions Foundation gives people meaningful actions they can take – including growing their own food at www.FoodFreedomeJournal.org, for example.

And, uniquely among all the health freedom organizations we know of, we are actually creating a project to help the farmers of the world, the consumers of the world and the governments of the world to reclaim the production of clean, unadulterated food! It is called The Valley of the Moon™ Eco Demonstration Project, www.NaturalSolutionsFoundation.org, and it is a major forward step for people who want to live, to farm, to help or to enjoy a truly sustainable teaching community the temperate, beautiful Highlands of Panama.

Several governments have asked us to work with them to change their food supply to a clean, unadulterated, health-promoting one and, of course, we said “YES!”

On the eve of our departure for another grueling Codex meeting. Oh, Geneva is OK as a city. There are some decently priced restaurants for locals and the lake, surrounded by mountains is pretty enough. If I had my way, though, and if General Stubblebine had his, we would stay right here in Panama working on the development of the Valley of the Moon Eco Demonstration Project, www.NaturalSolutionsFoundation.org, getting ready for the Grand Opening of the Natural Solutions Center on August 7 and 8! By the way, consider this your invitation to join us for this event! If you are on the Health Freedom Action eAlert list (sign up here: www.HealthFreedomUSA.org) you’ll get all the details.

But we cannot stay here, much as we would like to. Hundreds of thousands of people -and more – want to know what the Codex Alimentarius Commission is doing to despoil the world’s foods to bring about the perpetual war on their bodies, their health and their freedom – indeed, their very existence, that Big Pharma, WHO, Big Chema and the other genocidal, callous and much-worse-than indifferent players on the global food scene, led by the US, of course. They wait for our live radio reports, our daily Codex Video and written updates and our analysis of what is happening so they can counter it.

They know, and they take action on, the dangers that bills like S. 510, the Food Fascism Bill (named, of course, the “Food SAFETY Bill”), http://salsa.democracyinaction.org/o/568/t/1128/campaign.jsp?campaign_KEY=26714, will bring to them if they remain inactive. And we’ve kept this horrible bill from being voted on since November, 2009! That’s impact.

They are willing to call for a complete ban on the dangerous technology which has invaded the world’s food and non-food plant and animal life forms – including US, our DNA. By clicking on this link, rapidly growing numbers of people are protecting their future, and that of every living thing on the planet: http://salsa.democracyinaction.org/o/568/p/dia/action/public/?action_KEY=2049

Millions of people demanded that they have the right NOT to receive the vaccine for the absurd and fraudulent “Level 6 Pandemic” nonsense known as H1N1 or Swine Flu and the US backed off from requiring mandatory vaccination.

Now we are demanding Congressional hearings and responsibility in controlling, stopping and reversing the loss of children because of devastating environmental toxicity, including vaccines that do not work, have no science behind them and are killing us and our kids, while rendering huge numbers of us infertile, http://salsa.democracyinaction.org/o/568/p/dia/action/public/?action_KEY=3688. And we are suing the FDA to prevent more vaccines from being used which have never, ever been either tested to make sure that they are safe OR effective, let alone both. That case, the Stop The Shot Case, is a companion case to the Ear Candle Case, which we are also suing the FDA in that one, too. http://salsa.democracyinaction.org/o/568/p/dia/action/public/?action_KEY=2521. You see, if they can innocuous ear candles, of which 20 million have been sold without a single meaningful adverse event, saying that they are a medical device for which there is no medical use, they can ban ANY device or nutrient claiming the same.

We backed them off this crazed behavior in March, 2008 when they first flew this particular idea to see what would happen. What happened was that we, 688,000 strong, roared NO!, HELL NO! They predictably went away and, just as predictably, came back with this absurd power-grab to make all natural health products and services illegal.

We were there that time, and we are there this time, too. By the way, your recurring tax deductible donations here, http://drrimatruthreports.com/?page_id=189, are the essential lubricant which allows the health freedom wheels to keep turning. These donations are the only way that we can do this work, get to Codex, sue agencies, etc.

We are there, every time, because YOU are there. YOU are the netroots and YOU are the solution, the natural solutions. Thanks for making the Natural Solutions Foundation the largest health freedom organization in the world. And thanks for making a big, big difference.

Thanks, too, for your generous tax deductible donations. http://drrimatruthreports.com/?page_id=189
If you are not already giving the cost of a month’s worth of coffee, tea, chai, latte, cappuccino, or your other pleasure items each month, let me suggest that you do so, on a recurring basis. That’s the life-blood that keeps our brains and our other working parts pumping!!!!!

Oh, yes, two other things: first, if you use coffee for health or pleasure, you will want to taste the Valley of the Moon(TM) Coffee – FREE coffee! Coffee that we grow here in Panama to teach other farmers how to grow coffee without ANY toxic chemicals, neither herbicides like Monsanto’s Roundup(C), nor paraquat, nor Agent Orange products like 2-4D, nor pesticides or herbicides – NOTHING but sun, rain, fish meal and a 10 ingredient fermented compost! Other farmers are beginning to grow coffee this way, but there is nothing like our Valley of the Moon Coffee! Support your health and health freedom at the same time by making a tax deductible contribution and getting the healthy coffee. Oh, by the way, you can give this superb coffee as a thoughtful gift at any time of the year. Supplies are strictly limited so order NOW!

The second thing: All of this is great but without YOU as the person who disseminates this information, the Action Items and takes them once for each member of your family and then passes them along to all your contact, this information would stay the private knowledge of the few, a sort of information elite. Nice, but not effective. It is YOUR dissemination which makes this heath freedom thrust take wing and shape local, national and international policy.

It’s your world. Thanks for making us effective so that we do, in fact, make a difference!

Yours in health and freedom,
Dr. Rima

Rima E. Laibow, MD
www.DrRima.net
Medical Director

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The Big Picture: 5 Ways to Know if You’re Making a Difference
David Korten

David Korten’s newly revised and greatly expanded 2nd edition of Agenda for a New Economy: From Phantom Wealth to Real Wealth, outlines an agenda to create a new kind of economy: locally-based, community oriented, and devoted to creating a better life for all.

In this special pre-publication excerpt Korten explains how to tell if your actions are helping to build the new economy that “must be lived into being from the bottom up.”

For the many millions of us working to create a better world, it is easy to feel discouraged by the seeming insignificance of even major successes relative to the scale of the problems we face as a nation and a species. Consumed by the details and challenges of our daily engagements, we may easily lose sight of the big picture of the powerful social dynamic to which our work is contributing.

Step back from time to time; take a breath, look out beyond the immediate horizon to bring that big picture back into perspective. Reflect in awe and wonder at the power of the larger social dynamic to which your work contributes.

In my career in international development, I saw, time and again, that the most successful projects were not the largest or the most carefully, centrally planned; they were the ones that arose from the bottom up. Likewise, successful social movements are emergent, evolving, radically self-organizing, and involve the dedicated efforts of many people, each finding the role that best uses his or her gifts and passions. Their scope and their success may not, at first, be readily apparent. Social movements grow and evolve around framing ideas and mutually supportive relationships instead of through top-down direction. New ideas gain traction, or not, depending on what works for those involved in the movement. Some alliances are fleeting; others endure.

The organism, not the machine, provides the appropriate metaphor. The relevant knowledge resides not in the heads of outside experts but in the people who populate the system. The challenge is to help them recognize, organize, and use that knowledge in ever more effective ways.

This is the model I think of when I think about what it will take to build the New Economy—one based on fulfilling the basic needs of people and planet—that we need. It’s also the way that that economy is already being built: step by step, in creative and surprising ways, by people looking for alternatives to a system that isn’t working for them.

To bring down the institutions of Empire, we must begin to build the rules, relationships, and institutions of a New Economy. These must be lived into being from the bottom up.

So how do you know whether your work is contributing to a big-picture outcome? If you can answer yes to any one of the following five questions, then be assured that it is.

1. Does it help discredit a false cultural story fabricated to legitimize relationships of domination and exploitation and to replace it with a true story describing unrealized possibilities for growing the real wealth of healthy communities?
2. Is it connecting others of the movement’s millions of leaders who didn’t previously know one another, helping them find common cause and build relationships of mutual trust that allow them to speak honestly from their hearts and to know that they can call on one another for support when needed?
3. Is it creating and expanding liberated social spaces in which people experience the freedom and support to experiment with living the creative, cooperative, self-organizing relationships of the new story they seek to bring into the larger culture?
4. Is it providing a public demonstration of the possibilities of a real-wealth economy?
5. Is it mobilizing support for a rule change that will shift the balance of power from the people and institutions of the Wall Street phantom-wealth economy to the people and institutions of living-wealth Main Street economies?

These are useful guidelines for setting both individual and group priorities. Bear in mind that in a systems-change undertaking of this magnitude, there is no magic bullet and no one is going to make it happen on their own, so don’t be discouraged if the world looks much the same today despite your special and heroic effort yesterday. It took five thousand years to create the mess we are in today. It will take more than a few days to set it right.

David Korten adapted this article from the newly revised and expanded 2nd edition ofAgenda for a New Economy: From Phantom Wealth to Real Wealth, available for advance purchase from the YES! Magazine web store.

David is co-founder and board chair of YES! Magazine, co-chair of the New Economy Working Group, president of the People-Centered Development Forum, and a founding board member of the Business Alliance for Local Living Economies (BALLE). His books include Agenda for a New Economy: From Phantom Wealth to Real Wealth, The Great Turning: From Empire to Earth Community, and the international best seller When Corporations Rule the World.

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Polio VACCINE Causes Polio So We Have To Vaccinate More Kids! Say WHAT?

By Administrator on June 26, 2010 No Comments

Natural Solutions Foundation
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June 25, 2010

URGENT KIWANIS ALERT! IF YOU ARE A MEMBER OF THE KIWANIS SERVICE ORGANIZATION, http://sites.kiwanis.org/kiwanis/en/home.aspx, YOU MUST TAKE ACTION TO STOP YOUR ORGANIZATION FROM COLLABORATING WITH UNICEF IN “PREVENTING MATERNAL AND INFANT TETANUS”. THIS VACCINE IS THE ONE PIONEERED AND USED AROUND THE WORLD BY WHO TO CREATE PERMANENT INFERTILITY IN WOMEN AND GIRLS. PLEASE CONTACT THE KIWANIS ORGANIZATION AND ALERT THEM TO THIS USE OF VACCINATION. DEMAND THAT THEY SET UP CONTROLS TO MAKE SURE THAT THESE ARE NOT DEPOPULATION VACCINATIONS IF THEY ARE DETERMINED TO AID AND ABET A DANGEROUS ACTIVITY USED TO WEAKEN THE IMMUNE SYSTEM.
http://www.medicalnewstoday.com/articles/192937.php

Note: the Vaccine Adverse Event Reporting System, VAERS, reports 333451 adverse events associated with vaccines. This number is generally acknowledged to represent between 1 and 10% of all adverse events. ttp://www.medalerts.org/vaersdb/findfield.php
See also:
http://www.akha.org/content/medicaldocuments/tetanustoxoidcanadalabs.html
http://www.generationcedar.com/main/2009/07/population-control-through-tetanus-vaccine.html

Make sure you mark your calendar: Dr. Rima Reports, Every Sunday 9 PM to Midnight Eastern Standard Time at www.BlogTalkRadio.com/FreedomizerRadio
Find out about this week’s (and future) guests, check out the archives, at http://drrimatruthreports.com/?p=4850

Consider:
POLIOVICTIMS.2
POLIO VICTIMS, SIERRA LEONE

Polio virus
POLIO VIRUS

Poliovaccine crowd
CROWD AWAITING POLIO VACCINATION

Stanley Kops….has produced proof positive that the oral polio vaccine has always been contaminated with SV-40, a monkey virus which has been linked by the FDA and other organizations with cancers such as mesothelioma and meduloblastoma. Since 1963, we have been assured that polio vaccines have not contained this deadly contaminant. Stanley Kops shows that not only is this not the case, but that the vaccine regulators who are charged with keeping our families safe, have known all along that SV-40 was never removed from vaccines.

http://www.whale.to/a/sv40a.html

From the CDC: “Inevitable gaps in [Polio] vaccination coverage will give rise to cVDPVs [that is, polio cases caused by the vaccine itself – REL] as long as OPV [Oral Polio Vaccine] use continues”
http://www.cdc.gov/mmwr/preview/mmwrhtml/mm5540a3.htm

Polio outbreaks continue to be associated with circulating vaccine-derived polioviruses (cVDPVs) in areas with low oral poliovirus vaccine (OPV) coverage [Emphasis added-REL]. In addition, long-term excretion of neurovirulent immunodeficiency-associated vaccine-derived polioviruses (iVDPVs) can lead to poliovirus spread to contacts. Overcoming these obstacles is challenging. High rates of OPV coverage will prevent all poliovirus spread, including spread of VDPVs, but will not prevent establishment of prolonged VDPV infections in certain persons with B-cell immunodeficiencies (i.e., having defects in antibody production). Inevitable gaps in vaccination coverage will give rise to cVDPVs as long as OPV use continues.

and then consider that Elswood and Stricker, avid proponents of vaccination, presented evidence in 1994 that HIV was disseminated in polio vaccination by WHO in Africa. This evidence has never been refuted.
http://www.uow.edu.au/~bmartin/dissent/documents/AIDS/Elswood94.html

First, Blame the Victims!
If you read the article below, from the respected Science Daily, you will note that the vaccine establishment acknowledges that the cause of polio is, in many cases, the virus in the vaccine which was supposed to be so attenuated that it could not cause any disease. But the real reason, they assert, is that the people who get polio from the vaccines (mostly children under 5 years of age.

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Polio is the classic case of “Problem, Solutions, Reaction” favored by those who drive systems, in this case, our nations and our freedom, into chaos to control and destroy them. Take an environmental toxicity which co-factors with a virus, create a vaccine which spreads the disease, vaccinate widely, cause ‘epidemics’ of small numbers of cases, scare the wits out of parents and community decision makers with false information, deny for decades that the vaccine CAUSES the disease it is supposed to prevent and then, when the market is flagging because it is clear that the vaccination program has not worked, BLAME THE VACCINE FOR SPREADING THE DISEASE IN PEOPLE WITH VULNERABLE IMMUNE SYSTEMS AND THEN CONVINCE PEOPLE, ESPECIALLY DOCTORS, WHO ARE, IN FACT, THE MOST GULLIBLE OF PEOPLE, THAT THE CURE FOR VACCINE-DISSEMINATED POLIO IS TO VACCINATE MORE PEOPLE, ESPECIALLY KIDS!

Oh, wait! While you are doing that, make sure that the vaccine that spreads polio, in this case, ALSO causes another, deferred, more serious disease, in this case ACUTE LYMPHOCYTIC LEUKEMIA! And perhaps just a bit of HIV thrown in for good measure? Sure. People with HIV, in addition to dying, also get lots and lots of cancer!
Money House
THE HOUSE THAT CANCER BUILT

Cancer is the most wildly financially productive disease ever encountered by humans. The 2008 cost of cancer in the US, according to the American Cancer Society, funded by Big Pharma itself, was a walloping $228.1 Billion. How many of those dollars were expended on children with vaccine induced cancer? And what is the non-fiscal cost of a child’s life? I do not know how to do that mathematical computation. And the vaccine industry does not care to do it.
Please visit http://drrimatruthreports.com/?p=5706 to learn more about how this works. Then please come back to this article, keep reading and take action!

Polio vaccination is as great a scam as any other vaccination: there is no scientific evidence -none!- that vaccines work to prevent, mitigate or cure any disease. There is vast evidence that they work to weaken the nervous systems and that they intentionally, yes, intentionally, spread diseases which are vast profit sources and shorten lives and eliminate fertility.

We know, from the personal admission of Maurice Hilleman, PhD, or Merck Pharmaceuticals, that the polio vaccine’s leukemia virus contamination has been known for decades while the vaccine was administered to children around the world. I know of nothing to suggest that current polio AND OTHER vaccines are not contaminated with deadly viruses in addition to seriously toxic constituents like mercury and aluminum, Tween 80, human DNA, animal DNA, viruses, formaldehyde, etc. In fact, there is a great deal to document that they are. http://www.thinktwice.com/multiple.htm

And there is also a good deal to document that it is vaccination itself, not just polio vaccination, that causes diseases for which the vaccine allegedly protects the vaccination victim. [Alexa Traffic Rank for http://drrimatruthreports.com/docs/Syringe_of_death.pdf: 149579] http://drrimatruthreports.com/docs/Syringe_of_death.pdf, etc., etc.! http://drrimatruthreports.com/?p=3198.

So read the article below and then share it with everyone you know. Ask them to take the action steps here and, just in case you have not already taken these steps, once for every member of your family, please take a few moments to do so now. Riding the freedom mouse can save your life and your freedom, all in the same swift, easy action step!

Thanks for your activism.
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
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Now, your activism. First take action below for every member of your family and then forward this email to your entire contact list, asking that they do the same:
1. Call for Congressional Hearing on Autism and Other Environmental Illness: Autism and other environmentally caused diseases, including asthma, MS, at least 85% of all cancers (and much more in children), emphysema, etc., are preventable. Preventable, that is, if Congress takes the bull by the horns, carries out the studies and hearing and then passes legislation to protect the population. Click here, , to demand exactly those actions from the Congress that We, the People, elected and which works for US, the most potent special interest group in existence, 310,000 strong! http://salsa.democracyinaction.org/o/568/p/dia/action/public/?action_KEY=3688

2. Stop the Food Fascism Bill, S. 510, which masquerades under the title of the “Food Safety” Bill. It makes food profits safe for the multinationals like Monsanto, and guarantees that your food will be contaminated and controlled by those multinationals, not local farmers, including organic farmers. FDA says we do not have the right to decide what we want to eat. Show them they are wrong!
http://salsa.democracyinaction.org/o/568/t/1128/campaign.jsp?campaign_KEY=26714
3. End GMO Contamination of Your Food, Your Body, Your Planet. FDA FORBIDS GMO LABELING so you have no idea how much of your food supply is contaminated. Worse yet, GMOs are contagious! The foreign DNA spreads within and between species and the contamination cannot be reversed by any technique we have now short of burning the contaminated material. NO significant safety testing is carried our, or permitted, by government agencies. Ban GMOs and set up a commission to find out how much damage has been done and develop new ways to fix the problem before there IS no fix!
http://salsa.democracyinaction.org/o/568/p/dia/action/public/?action_KEY=2049

Thanks for donating and taking the important Action Items above. You are a member of the distribution list for the free, secure and very important Health Freedom Action eAlerts, aren’t you? Quick, sign up here, http://drrimatruthreports.com/ (scroll down, sign up!)

Polio Research Gives New Insight Into Tackling Vaccine-Derived Poliovirus

ScienceDaily (June 24, 2010) — A vaccine-derived strain of poliovirus that has spread in recent years is serious but it can be tackled with an existing vaccine, according to a new study published today in the New England Journal of Medicine.

Vaccine-derived polioviruses can emerge on rare occasions in under-immunized populations, when the attenuated virus contained in a vaccine mutates and recombines with other viruses, to create a circulating vaccine-derived strain.

The researchers behind today’s study say their findings highlight the importance of completing polio eradication. They also say that should wild-type poliovirus be eradicated, routine vaccination with oral polio vaccines will need to cease, in order to prevent further vaccine-derived strains of the virus from emerging.

The study was carried out by researchers from the Medical Research Council Centre for Outbreak Analysis and Modelling at Imperial College London, working with the Government of Nigeria and the World Health Organization (WHO) research teams.

Poliovirus is highly infectious and primarily affects children under five years of age. Around one in 200 of the people infected with polio develop permanent paralysis, which can be fatal.

Polio was virtually wiped out by the early 2000s following a major vaccination drive by the Global Polio Eradication Initiative, but since then the number of cases of paralysis reported has plateaued, remaining roughly constant at between one and two thousand each year from 2003 to 2009, dropping only recently in 2010.

The first reported polio outbreak resulting from a circulating vaccine-derived poliovirus, known as a cVDPV, occurred in Hispaniola in 2000. Prior to today’s study, there was little evidence available about the severity and potential impact of this kind of poliovirus.

Although billions of doses of oral vaccine have been distributed in the last decade, just 14 cVDPV outbreaks have been reported, affecting 15 countries. These outbreaks have usually been limited in size.

For the new study, researchers looked at the largest recorded outbreak of a cVDPV to date, which began to circulate in Nigeria in 2005. The authors examined data from 278 children paralyzed by this cVDPV, and compared them with children paralysed by wild-type poliovirus in the country. Their analysis showed that this serotype 2 cVDPV is as easily transmitted and likely to cause severe disease as wild-type poliovirus of the same serotype.

The study also shows that vaccination with trivalent OPV, one of the main types of vaccine currently used to combat polio, is highly effective in preventing paralysis by this serotype 2 cVDPV.

The research shows that it is even more effective against cVDPV than against the wild-type polioviruses that are currently circulating, which can also be targeted with a different vaccine.

The new findings mean that it is particularly vital that efforts to vaccinate children with trivalent OPV continue in Nigeria and neighbouring countries, to protect children against all strains of polio. The scientists hope their findings will help countries to devise the right vaccine strategies to eradicate polio.

Helen Jenkins, the lead author of the study from the Medical Research Council Centre for Outbreak Analysis and Modelling at Imperial College London, said: “Our research shows that vaccine-derived polioviruses must be taken seriously and that we have the right tools to tackle them. We’ve had a lot of success against polio in the past and we’re optimistic that ultimately we should be able to eradicate it completely.

“However, our study shows that we can’t be complacent about the virus. It’s still vital for us to protect children from this dangerous and debilitating disease and we have to make sure we continue to vaccinate as many children as possible in affected countries for as long as wild-type poliovirus continues to circulate,” added Ms Jenkins.

Senior study author Dr Nicholas Grassly, also from the Medical Research Council Centre for Outbreak Analysis and Modeling at Imperial College London, added: “There has been some debate about the significance of circulating vaccine-derived polioviruses for the eradication initiative. Our research shows these viruses can be as pathogenic and transmissible as wild-type polioviruses and outbreaks must be responded to with just as much vigour.”

Dr Bruce Aylward, Director of the Global Polio Eradication Initiative at WHO, added: “These new findings suggest that if cVDPVs are allowed to circulate for a long enough time, eventually they can regain a similar capacity to spread and paralyse as wild polioviruses. This means that they should be subject to the same outbreak response measures as wild polioviruses. These results also underscore the need to eventually stop all OPV use in routine immunization programmes after wild polioviruses have been eradicated, to ensure that all children are protected from all possible risks of polio in future.”

This study was funded by the Medical Research Council and the Royal Society.
http://www.sciencedaily.com/releases/2010/06/100623190726.htm

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Mercury in Vaccines Not IN SPITE of Devastating Toxicity, But BECAUSE Of It?

By Administrator on June 24, 2010 No Comments

Natural Solutions Foundation
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www.GlobalHealthFreedom.org

June 24, 2010

Donate to keep health freedom free!
http://drrimatruthreports.com/?page_id=189

Click here to tell Congress that it is high time for a meaningful Congressional Investigation into the causes and cures for autism and other environmentally caused diseases: http://salsa.democracyinaction.org/o/568/p/dia/action/public/?action_KEY=3688

Important Note: Please share this as widely as possible

Could mercury be included in vaccines not in spite of its devastating whole-body, all-systems toxicity, but BECAUSE it it? Read what Dr. Paul G. King, http://www.Mercury-freeDrugs.org, has to say on the topic.

Dr. King is one of my favorite health heroes. He is a human being who thinks like a scientist and a scientist who thinks like a human being. He also possesses one of the most important qualities which anyone can exhibit: he is fearless. Using his well-honed scientific logic, he asks questions that may seem to be inconvenient of impolite and then uses logic and research to find the answers.

Does, asks Dr. King, the use of mercury (Thimerosal) make any sense in vaccines as a preservative and antiseptic since it is not an antiseptic, not a preservative, nor is it safe? No, it does not. So why, Dr. King asks, is it used? What could possibly explain the available data? Perhaps that data is explained by the unthinkable: that Thimerasol is included in vaccines precisely because it is a systemic poison.

That is a horrific and close-to-unthinkable idea unless…. unless you look at that data. The questions of why anyone would poison our children “unto the seventh generation” is not one that Dr. King takes up. I do. I maintain that the sustainability of the globalists, which they do so love to talk about, is their reason for poisoning us with vaccines, Codex-degraded foods, pollution, deadly medicines and, yes, vaccines.

But before you accept this horrifying proposition, please read Dr. King’s editorial closely and consider it for yourself. Then, whatever you decide, join us in taking the Action Item at the head of the page in which we are demanding of Congress that they hold a Congressional Hearing on autism and other environmental diseases.

Yours in health and freedom,
Dr. Rima

Rima E. Laibow, MD
Medical Director

Natural Solutions Foundation
www.HealthFreedomUSA.org
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Donate to keep health freedom free!
http://drrimatruthreports.com/?page_id=189EDITORIAL – 23-06-2010
Thimerosal in Vaccines: A ‘Profitable’ Medical Maiming Agent?
Introduction to Thimerosal, a Highly Toxic Organic Mercury Compound

Paul G. King, PhD

Since the mid-1800s, we have been, and are being, exposed to increasing background levels of elemental,
inorganic, and naturally occurring organic mercury.

However, the history of mercury-containing poisons turned much more deadly when people began to make
synthetic organic mercury compounds specifically designed to be more toxic [1] to life than the common environmental inorganic mercury compounds.

[1] On a relative scale where metallic mercury has a relative toxicity of “1”, inorganic mercury compounds typically are “10 times more toxic as a group and organic mercury compounds are “100 to 1000” times more toxic on a weight basis than metallic mercury.

It is against this background that a chemist, M. S. Kharasch, synthesized a variety of “alkyl mercuric sulfur”
compounds, including sodium ethyl mercuric thiosalicylate [2], in the 1920s.

[2] Based on recent studies, this compound is on a molar basis at least 10 times more toxic to developing neurons and astrocytes than the methyl mercury compounds found in fish.

In 1928, the US Patent Office granted Kharasch a patent (“Alkyl Mercuric Sulfur Compound and Process for Producing it. US Patent 1,672,615”), relating to this alkylmercury sulfur-containing compound, which he had synthesized in the laboratory, and to the process for producing it.

He assigned this patent, along with two follow-on patents: “Kharasch, M. S. 1932. Stabilized Bactericide and Process of Stabilizing it. US Patent 1,862,896” and “Kharasch, M. S. 1935. Stabilized Organo-Mercuri-Sulphur Compounds. US Patent 2,012,820”, to the company for whom he worked, Eli Lilly and Company (Lilly) [3].

[3] These patents clearly established the instability of water- containing solutions of sodium ethyl mercuric thiosalicylate such as those in vaccine formulations.

The “safety” studies Lilly-affiliated personnel conducted on this compound were limited to some cursory animal toxicity studies that killed many of the test animals, and a specious test on some patients dying from bacterial
meningitis in the days before modern antibiotics.

In spite of the obviously highly toxic nature of this mercury compound and its instability in water-containing solutions, Lilly chose to manufacture and market this compound under the trade name “Merthiolate” [4] in the 1930s.

[4] “Mer” from mercury and “thiolate” from thiosalicylate”. The other trade names for this compound include: Merfamin, Merthiolate sodium, Mertorgan, Merzonin, Merzonin sodium, SET, Thimerosal, Thimerosalate, and, principally in Europe, Thiomersal and Thiomersalate.

Lilly sold Merthiolate as a 0.1% alcohol solution [5] (Tincture of Merthiolate), which it promoted as a “safe” and “effective” over-the- counter (O-T-C) topical antiseptic.

[5] As studies conducted in the 1930s and 1940s clearly established, the only effective antiseptic was the alcohol in the tincture – Merthiolate/Thimerosal, ateven levels of 0.1%, was neitheran effective antiseptic nor bactericidal.

Lilly marketed this O-T-C antiseptic without any valid toxicological proof of either Merthiolate’s “safety” (or its “effectiveness” as an antiseptic beyond that of the alcohol in which it was dissolved) from the early 1930s.

It also used this compound, also trade-named Thimerosal, as a preservative in the serum and vaccine products Lilly sold until the mid- 1970s [6].

[6] When it exited the vaccines business in the mid-1970s, Lilly licensed the use of its proprietary processes for the manufacture of Thimerosal- preserved vaccines to other vaccine makers and, until 1994, continued to make the Thimerosal powder used in their manufacture.

In 1998, after decades of procrastinating, the US Food and and Drug Administration (FDA) banned the use of Merthiolate/Thimerosal and related mercury compounds as ingredients in the manufacture of O-T- C topical antiseptics and vaginal contraceptives.

The FDA banned these uses of these mercury compounds on the grounds that they were neither safe to be administered to humans nor effective as a bactericidal agent in such applications.

However, though the FDA recognized Merthiolate’s/Thimerosal’s lack of safety to humans at antiseptic levels (nominally, 0.1 % by weight/volume) and its failure to be an effective antiseptic or spermicide, the FDA continued to ignore the realities of Thimerosal’s toxicity when it is used in the making of prescription medicines, where it is used as a preservative and its nominal levels range up to 0.01% by weight/volume.

As of June 2010, the FDA continues to permit the use of Thimerosal in prescription drugs, including vaccines and other biological drug products.

Thus, without the required toxicological proofs of safety, Thimerosal is still being used in the manufacture of several FDA-
approved vaccines and other drugs.

From the early 1930s until the mid- 1970s, Lilly manufactured and distributed Thimerosal-preserved serums and vaccines under licenses granted by the US National Institutes of Health (NIH), which regulated serums and vaccines.

In the late 1960s, because of the NIH’s mismanagement of vaccines, the oversight for serums and vaccines was transferred to the FDA.

Unfortunately, this transfer of oversight to the FDA included the transfer of key individuals from the NIH to the FDA’s then “Bureau of Biologics”.

Among the transfers was the then head of this FDA bureau, who continued to allow the use of Thimerosal as a preservative in biologics without the required toxicological proofs of safety.

Since 1973, all Thimerosal-containing serums and vaccines for use in humans have been regulated as biologics (biological drug products) under Title 21 of the United States Code of Federal Regulations (21 CFR) in 21 CFR §§ 600 – 680, in specific, and under all of the applicable parts of 21 CFR, in general.

As of June 2010, the manufacturers who use it have apparently not proven that the use of Thimerosal as a “preservative” in such biological products is “safe” in the manner required by law.

This is the case because 21 CFR §610.15(a), the applicable current good manufacturing practice (CGMP) drug producer’s minimum nondischargeable “shall” compliance obligation, specifically requires: “Any preservative used shall be sufficiently nontoxic so that the amount present in the recommended dose of the product will not be toxic to the recipient” [7].

[7] Note: Scientifically, the dose of a compound is “nontoxic” when the maximum level present is properly proven to be below the compound’s NOAEL (no observed adverse-effect level) when, in the intended manner (injected in the case of vaccines), the appropriate animal surrogates for the most sensitive group for which the use of the compound is intended (for vaccines, the most sensitive groups are the fetuses of pregnant women and developing children) receives the maximum amount permitted in a single dose at a frequency that appropriately matches the maximum in the most sensitive group.

To be “sufficiently nontoxic”, as required here, the level of the preservative dose must be appropriately below the NOAEL by
more than one order of magnitude (> a factor of 10).

For example, if the NOAEL for injected Thimerosal in a vaccine formulation is about 0.01 micrograms/kg of body weight/per
day, then a maximum level of about 0.0001 micrograms/kg/day (a
factor of 100 lower) might be an appropriate to ensure that the dose delivered were “sufficiently nontoxic”.

The need for a safety factor of 100, or more, arises because of the highly toxic, bioaccumulative nature of Thimerosal and its metabolites. In most current Thimerosal- preserved vaccines, the nominal level of Thimerosal is on the order of nominally 100 micrograms per milliliter. Moreover, the developing fetus typically weighs in the range from less than 1 gram to no more than 6 kg.

Thus, it is obvious that Thimerosal is much too toxic for 0.5-mL injections into the pregnant woman (delivering nominally up to 50 micrograms of Thimerosal to the fetus) to be safe since the maximum level could exceed 50,000 micrograms of Thimerosal per kilogram of fetal weight during the early weeks of pregnancy!

Today, Thimerosal, sodium ethyl-mercurithiosalicylate, is a recognized human teratogen, mutagen, carcinogen,
immune-system disruptor, and reproductive toxin at levels well below 1 part per million (ppm).

With the preceding background in mind, let us consider the “criteria” for a profitable medical population-maiming
agent and then assess how well Thimerosal used as a preservative in vaccines meets these criteria.

The “Criteria” for a Long-term ‘Profitable’ Medical Population-Maiming Agent

1. Hidden sub-acutely toxic doses of the poison must be given to each cohort of developing children before, or shortly after, birth and periodically afterward in some medicine.

Ideally, for a mass poison that is intended to “permanently” maim, but not kill, many of those who are given it, the poison needs to be given as soon as possible to as many of the target population as possible – in all parts of the target country at about the same time.

Thus, when the target is humans, the first characteristic must be that, before birth or as soon as possible after birth, almost every child must be covertly exposed to a suitably “toxic” dose of the poison.

This non-lethal, sub-acutely toxic dose must be sufficient to slowly poison some small percentage of those given it in a manner that, over time, renders them chronically ill.

In addition, to maximize the cumulative profit, almost every child must be given multiple sub-acute doses
of this poison as he or she develops.


This tactic helps to ensure:
o The percentage chronically harmed will increase over time, and
o The general population will be slow to connect the harm done to the concealed poison repeatedly administered to the developing children.

2. The doses of the poison must be portrayed as contributing to the “safety” of the product in which they are placed and the public must consider the products containing the doses of poison to be “vital” for developing children to receive

To permit the poisoning to proceed for a long time before anyone starts to notice it, the population as a whole, an especially those administering the poisoning doses, must not notice the poison or, if they do notice it, perceive that the dose being given is an insignificant dose.

In addition, the poison should be presented as a contributor to the “safety” of the medical product in which it is delivered.

Finally, the poison should be concealed in a medical product that the public perceives, or is led to believe, is necessary or vital for most all children to receive.


3. Each small dose of the poison must cause chronic disease in some who are given more of it

The third key for an exquisite mass-use poison is that only a single small dose is required to cause long-term toxic effects in some, with successive doses causing increasing effects in an increasing percentage of the population.


4. The poison’s effects must be time delayed and/or slow to develop

The fourth attribute for a near-ideal mass poison is that its observable poisoning effects must be delayed and/or slow to develop so that the resulting poisoning is not closely associated with the maiming doses’ delivery.

5. The poison must be a systemic Poison

The fifth characteristic for a “ideal” mass poison is that it must be a systemic poison that affects all of the biological systems of the targeted population to varying degrees.

This ensures that the agent’s harm is harder to recognize because the poison’s effects are not be limited to
one specific organ (e.g., heart) or system (e.g., immune system).

6. When recognized, the poison must be difficult to remove and/or to reverse its ill effects

The sixth attribute for a mass poison designed to provoke chronic disease must be that, once the poisoning is
finally recognized, the poison’s final metabolic products must be bioaccumulative persistent toxins that are difficult to remove from the body or hard to neutralize – making the chronic effects difficult and/or medically costly to reverse.

7. The poison and/or its metabolites must be soluble in aqueous and non-aqueous systems

The seventh design parameter for an effective mass poison must be that the poison and/or its immediate toxic
metabolites are soluble in both aqueous (hydrophilic) and non-aqueous (hydrophobic) regions of the body to ensure that as many organs and systems as possible are adversely affected in as many manners as achievable in the target population.

8. The poison must induce multi-generational adverse genetic and/or epigenetic effects in some of those who are dosed with it

The eighth key characteristic is that the poison must have some probability that some of its adverse health effects will be passed on to some of the offspring that those who are directly poisoned may subsequently bear or father so that, even when the poison’s use is finally stopped, it will continue to generate chronic illness in some children for generations to come.

9. The Establishment must claim that the poison is “safe” and block the requisite toxicity studies that would prove it is not “safe”

The ninth key, for our ideal mass poison, is that the medical establishment, drug makers, health officials, all the relevant government agencies and the mainstream media must not only claim that this poison is “safe” at the level used but also
refuse to conduct, and/or otherwise block, the appropriate toxicity studies that would reveal its true
toxicity.

Thimerosal at Preservative Levels in Vaccines: An Ideal Poison for Medical Mass Maiming?

From the history of its discovery, isolation and characterization, it is clear that Thimerosal is not stable when dissolved in aqueous environments.

Then, why would any firm knowingly choose Thimerosal for use as a preservative in water-based (aqueous) vaccine formulations when it is unstable in aqueous solutions?

Moreover, if one were looking for a preservative that was “safe” and “effective”, why would a firm choose to use Thimerosal, a compound that:
o Becomes more toxic over time when dissolved in isotonic pH-buffered physiological saline, and
o Rapidly losses its effectiveness as a “preservative” in serums
and vaccines, when exposed to common protein components present in such products?

Yet, Lilly used Thimerosal/Merthiolate as a preservative (nominally, at .01%) in its serum and vaccine products from the 1930s until the mid-1970s when it exited the vaccines business.

In addition, along with other firms, Lilly marketed Thimerosal as an O-T-C topical antiseptic (Merthiolate) until the late-1990s, when, on the grounds of a lack of safety and a lack of effectiveness unequivocally established in the 1970s, the FDA finally banned its use as an ingredient in such O-T-C antiseptics and vaginal contraceptives.

Further, the Thimerosal-preserved early childhood vaccines (like Lilly’s DT and DPT vaccines) appear to meet the first two criteria for a profitable population-maiming agent:
1. An early population-wide deployment that maximizes the profit potential, and
2. The concealment of an “inconspicuous” amount (1 part in 10,000) of the agent as a “helpful” substance (a “preservative”) in “life saving” vaccines given several times in early childhood.

Thus, besides Tincture of Merthiolate, touted as a “safe” and “effective” topical antiseptic but not universally used by pregnant women or on young developing children, the first Thimerosal-based mass-maiming agents deployed appear to be the injected Thimerosal-preserved DT and DTP Vaccines [8], which Lilly made for administration to babies several times before their first birthday.
[8] After Lilly exited the vaccine market, other vaccine makers, principally what is now Sanofi Pasteur and GlaxoSmithKline as well as other vendors have marketed Thimerosal-preserved vaccines including some that are still being manufactured to this very day and are approved for US use.

From the 1980s until the early 2000s, in addition to Thimerosal- preserved DT and DTP vaccines, Thimerosal-preserved Td, TT, Hib, Hep B, Meningococccal, Inactivated-influenza and other vaccines were approved for use in various population segments including, for the Hib and Hep B vaccines, children.

With the phasing out of the Thimerosal-preserved DTP, Hib and Hep B vaccines as well as the Thimerosal-preserved Rho(D) products given to Rh-negative women during pregnancy in the early 2000s, in 2002, the CDC moved to replace the lost Thimerosal-maiming doses with the mercury in inactivated-influenza shots to be given to pregnant women and children 6 months to 23 months of age. By steadily increasing the upper end of the age range for
the children until it was up to 18 years in 2009, recommending 2 shots the first time a child is vaccinated for influenza, and, in the 2009-2010 flu season, adding recommendations that included one Thimerosal-preserved inactivated- influenza 2009-A-H1N1 vaccine for pregnant women and two additional doses of what could be a Thimerosal-preserved 2009-A-H1N1 vaccine for children under 9 years of age and 1 dose for those over nine years of age, the CD has effectively more than replaced the mercury removed for most of the pregnant women and children because most doses of
the inactivated-influenza vaccines (nearly 100% in the 2002-2003 flu season, and at least 75% in the 2009-2010 flu season) were Thimerosal-preserved doses.

The CDC’s recommendation to give flu shots to pregnant women is particularly egregious because all flu vaccines are: a)
“Pregnancy Category C” drugs, whose fetal and reproductive safety and effects have never been properly established and b)
drugs that have also not been tested for mutagenicity and carcinogenicity.

These Lilly vaccines were touted as life saving drugs that “immunized” (bulletproofed) children from getting deadly diseases, diphtheria (D), tetanus (T), and pertussis (P; whooping cough), which were often fatal.

Moreover, each dose of these “preserved” vaccines directly delivered nominally 50 micrograms of Thimerosal (25 micrograms of organic mercury) – a level that is more than sufficient to cause a low-level of harm in susceptible babies [9].

[9] Based on the only FDA-recognized chronic rat study for injected Thimerosal, the “nontoxic” level for injected Thimerosal is somewhere below 0.0042 microgram of Thimerosal-derived mercury per kilogram per day [see:
http://mercury-freedrugs.org/docs/090812_fnldrft_TheTruthAboutTheToxicityOfThimerosalr5b.pdf,
“The ‘Truth’ About The Toxicity Of Thimerosal (12 August 2009; 6 pages)”].

Based on several independent retrospective statistical population records studies, an exposure increase of 200 micrograms of Thimerosal (100 micrograms of organic mercury) in children vaccinated during their first year of life has been proven to be a statistically significant, or nearly statistically significant, population risk factor for a variety of serious childhood medical conditions (e.g., autism, tics, and, most recently, premature puberty).

In some reported monkey studies, a single weight-proportional birth dose of a Thimerosal-preserved hepatitis B vaccine has been shown to cause subtle, but serious, adverse effects on their early development.

Thus, Thimerosal, at preservative levels in vaccines, appears to meet the third criterion.

Moreover, the principal persistent adverse effects, like loss of words, failure to thrive, tics, or premature puberty, that have been linked to Thimerosal exposure from the injection of Thimerosal-preserved vaccines, are delayed effects.

In most cases, the exposed infant in America appears to progress normally for some period after the initial or one of the subsequent poisonings (e.g., at 2, 4, and 6 months for the Thimerosal-preserved DTP vaccines up until 2004, or at before birth and 6 [and 7] months for the Thimerosal-preserved flu shots that the CDC started ‘encouraging’ healthcare professionals to give pregnant women and healthy babies in 2002) [10].

[10] Building on the DTP program, the Thimerosal exposures were increased to at birth, 2 and 4 to 6 months when the early hepatitis B program was introduced in the 1990s, in addition to 3 more doses (at 2, 4, and 6 months) from the Hib
vaccines introduced in the late 1980s.
Further, as the level of Thimerosal was being reduced in the early childhood vaccines, the CDC started making recommendations that pregnant women and healthy children at 6 to 23 months of age receive the Thimerosal-preserved inactivated-influenza vaccines in 2002.

Currently, the CDC recommends inactivated-influenza vaccination for pregnant women and children at 6 and 7 months and annually thereafter, where the majority (not less than 75%) of the available doses are Thimerosal-preserved. In addition, in 2009 the CDC recommended an additional 2009- A-H1N1 inactivated-influenza vaccine shot for pregnant women; two of these flu shots for children up to age 9; and one of these flu shots for those 9 and older – where most all of the available doses of the 2009-A-H1N1 flu shots were again Thimerosal-preserved inactivated-vaccine doses.

Then, the susceptible exposed infant begins to “regress” or “change” as the symptoms of the maiming become evident months (usually, at or after 1 year of age) or, in the case of premature puberty (and probably childhood MS), several years later.

Thus, Thimerosal clearly satisfies the fourth, “effects delayed and/or slow to develop”, criterion for an effective population-maiming agent.

Thimerosal clearly satisfies the fifth criterion because it is a proven systemic human poison at low levels (part-per million and lower).

For example, Thimerosal is a known human carcinogen, mutagen, teratogen, immune-system disruptor and reproductive toxin (by California Prop 65 criteria) at levels below 1 part- per-million (ppm) of Thimerosal in the body.

Further, Thimerosal’s end-product metabolites are tissue-bound inorganic mercury species that have human half- lives on the order of one to two decades, depending on the tissue.

Thus, it is clear that Thimerosal is a bioaccumulative persistent toxin.

Moreover, as studies in monkeys have established, the tissue-bound “inorganic mercury” species form faster when an ethyl mercury compound was administered than when a similar methyl mercury compound was administered.

In addition, even when aggressive “mercury chelating” agents, like DMSA and DMPS, are used, the level of mercury “bound” in the tissues can only be slowly reduced.

Typically, chelation takes years to significantly reduce the poisoned individuals’ body-burden of tissue- associated, “inorganic” mercury to the point that those reversible [11] symptoms induced by the mercury- poisoning events are minimized or, in some instances, are apparently eliminated.

[11] Unfortunately, unless tested for mercury toxicity and treated before the adverse effects produce persistent symptoms, some of the developmental harm done seems, at present, to be non-reversible in many
instances.

Thus, Thimerosal has the characteristics required for the sixth key attribute for a maiming poison because any exposure to it can slowly provoke a wide range of chronic adverse clinical conditions and its mercury containing end-point metabolites (tissue-bound “inorganic mercury”) are difficult to remove from the tissues in which they reside.

Further, when a Thimerosal-containing solution enters the human body, the Thimerosal present reacts with the body’s aqueous fluids to form the following organic compounds:
– Ethyl mercury chloride (EtHgCl), which is highly lipophilic (hydrophobic);
– Ethyl mercury hydroxide (EtHgOH), which is highly hydrophilic; and
– Sodium thiosalicylate, which is further metabolized in the body.

Since both of the initial ethyl-mercury-containing metabolites of Thimerosal are small neutral species, they:
– Are easily transported within the human body;
– Apparently cross or circumvent the blood-brain barrier and cross the placenta and enter the fetus; and
– Once inside a given tissue, are rapidly converted into tissue-associated “inorganic mercury” that tends to bioaccumulate in
that tissue.

Given the preceding realities, it is clear that Thimerosal and its mercury-containing metabolites directly and indirectly poison almost all human biological processes to some degree wherever a mercury species can interfere with the body’s fundamental systems.

Thus, Thimerosal’s rapid breakdown in the human body into small neutral mercury-poisoning metabolites (that are both hydrophilic and hydrophobic and which migrate into the tissues and are converted into tissue-resident “inorganic mercury”) satisfies the seventh criterion for an exquisite mass-maiming poison.

Further, based on multi-generational reproduction experiments done in the former Union of Soviet Socialist Republics (USSR) [12], sub-acute Thimerosal exposure is clearly capable of inducing epigenetic and/or genetic changes in the offspring who are exposed to Thimerosal in utero.

[12] Goncharuk GA. Experimental investigation of the effect of organomercury pesticides on generative functions and on progeny. Hyg Sanit. 1971; 36: 40-43.

The changes induced in utero were shown to be expressed in the non- Thimerosal-exposed second-generation offspring of the first-generation of indirectly exposed offspring.

Thus, Thimerosal, used as a preservative in vaccines, appears to be a multi-generational poison.

Moreover, these experimental findings help to explain why the then USSR, already experiencing a population decline, was the first European nation to ban the use of Thimerosal in vaccines (in the early 1980s) – more than 2 decades before the US finally began slowly reducing the level of Thimerosal in the previously Thimerosal preserved early childhood vaccines.

While, obviously driven by other imperatives, the FDA continued to approve additional Thimerosal- preserved vaccines (e.g., the vaccines for hepatitis B and Haemopholis influenza type B) and the Centers for Disease Control and Prevention (CDC) continued to add these additional FDA-approved Thimerosal-preserved vaccines to the recommendations for the national childhood vaccination program.

Thus, Thimerosal apparently meets the eighth key attribute for a near-ideal population-maiming toxin – its maiming effects can be transferred to the offspring of mothers who were themselves exposed during pregnancy as long as these in-utero-exposed ‘potential mothers’ are not so damaged that they are “miscarried” or they cannot bear children.

Finally, given:
-The official positions taken by the medical establishment, the vaccine makers, the health officials, academia, all relevant governmental agencies and the mainstream media that the use of Thimerosal as a preservative in vaccines is “safe” and
-The refusal of all to conduct (or report to the public) all of the applicable toxicity studies required to prove that this use of Thimerosal is “safe”,
Thimerosal clearly satisfies the ninth key factor for a near-ideal population-maiming poison that is touted a “beneficial” component (a preservative) and added to “life saving” vaccines that all American children are recommended to be repeatedly
given.

Thimerosal at Preservative Levels in Vaccines: A Near-ideal Medical Agent for ‘Profitable’ Mass Maiming

Thus, Thimerosal’s use as a “presser- vative” in medical vaccines seems to meet all nine (9) of the criteria for a ‘profitable’ medical mass-maiming poison.

Further, it seems clear that Lilly and the current vaccine manufacturers, which, without complying with 21 CFR § 610.15(a), continued to use Thimerosal as a preservative in vaccines and/or to
apparently profit from its on-going use, have been knowingly engaged in the apparent medical poisoning of
American children for decades in order to, at some point, profit over several decades from the Thimerosal-induced increase in the level of children in the USA who have life-long chroni health conditions (e.g., for ‘autism’, from less than 1 in 1000 children born in 1955 to more than 1 in 100 born in 2005; and, for asthma, from less than 1 in 1000 children in the 1950s to greater than 1 in 10 born in the 21st century).

Finally, these actions have apparently been, and are still being, undertaken with the tacit consent and/or assistance of all the Thimerosal-use-sup- porting facets of the Establishment.

Disclaimer

**************************************
* The information provided in this editorial is just that-information. *
* It is not medical advice and it does not require any specific action or actions. *
* While the statements made are thought to be accurate, no representations are made as to their accuracy other than that they are my best understanding of the facts on the date that this editorial was first published on the Internet. *
* All should verify the accuracy of the information provided for themselves before acting on it or reacting to it.
**************************************

Concluding Remarks

Should any reader find significant factual errors in this editorial, then please send the author (at drking@gti.net) your proposed changes along with e-mail attachments that contain copies of the published documents that provide the proofs needed to substantiate your claims.

Then, as has been the case in the past, after verifying the validity of your concerns, the confirmed factual errors will be corrected and an appropriately “revised editorial” posted.

If you find spelling, grammar or textual errors, please also send them in so that this document can be appropriately revised and posted as an “updated editorial”.

Categories : Activism, Autism, Avian Flu, Blog / Vlog, Compulsory Drugging, Disinformation, Genocide, Medical Hazards, Miscellaneous, Swine Flu, Vaccination
Tags : Autism, Big Pharma, Compulsory Drugging, Compulsory Vaccination, Disinformation, Dr. Rima, FDA, health freedom, Health Hazards, Mandatory Vaccination, medical hazards, mercury, Natural Solutions Foundation, NSF, Pandemic Swine Flu, Rima E. Laibow, Rima E. Laibow MD, Swine Flu, Vaccination, Vaccinations, Vaccine Dangers, vaccines, Valley of the Moon

Is Silver Under the Gun Because It IS the “Magic Bullet”?

By Administrator on May 11, 2010 No Comments

Natural Solutions Foundation
The Voice of Global Health Freedom™
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org

PROTECT YOUR RIGHTS TO MAKE YOUR OWN HEALTH CHOICES!
Make your tax deductible donation now to keep health freedom strong.
Click here: http://drrimatruthreports.com/?page_id=189. Dr. Rima discusses the new “pandemic” fungus and how to respond to this latest threat from an eco system under severe man-made stress. Yet another “weaponized” pathogen and Nano Silver…

Health Freedom Thought Experiment.

The article following this essay looks at an emerging danger, the newly virulent Cryptococcus gatti fungus. Apparently weaponized, this may be “The Next Big Thing” for the genocidalists at WHO and elsewhere. If so, we need to have a defensive strategy and an offensive one as well.

I believe that the defensive one is to have as much high quality Nano Silver on hand as you estimate you will need both for immediate use and for what comes next, and next, and next again after that. Because it appears that the plagues manufactured in laboratories will keep coming. Nano Silver, like the Silver Solution we recommend, www.Nutronix.com/naturalsolutions will keep you safe if you have it and if you use it.

The offensive strategy is two fold: protect our health options and expose the genocidal agenda at every turn, making it so widely understood that the secrecy which allows it to function is shattered. Make the myth of overpopulation a thing of the past, like the myth of necessary female circumcision or a flat earth.

Let’st hink this through. What happens if we protect Nano Silver? What happens if its use in animals and humans is so widespread that it eliminates antibiotics altogether?

Physicists use “thought experiments” to guide them to new approaches when the experiment is too hard, too expensive or too novel to actually conduct. By working through the experiment in their minds, they can make [very] educated guesses about what happens next if they were to conduct the experiment in the real world.

Health Freedom can use the same techniques to conduct an important Thought Experiment. First, the propositions and assumptions:

Antibiotics and Vaccines

1. Antibiotics, vaccines and other pharmaceuticals are astonishingly profitable

2. Antibiotics are widely understood to be overused, leading to drug resistant and multiply drug resistant pathogens.

3. Vaccines have never been tested in a placebo controlled, double blind study to show that they are effective in either preventing or treating any disease. Vaccine manufacturers and regulators hold the position that it would be “unethical” to deprive the test subjects of the benefits of vaccines even though such benefits have never been rigorously documented while vaccine dangers have been.

4. 90% of all antibiotics used world wide are used in factory farming.

Nano Silver

1. Nano Silver is the Universal Antibiotic because laboratory tests show that it is effective against every disease-causing organism against which it has been tested: bacteria, mycoplasma, fungus (i.e., mold), virus. In all, It has been tested against more than 630 disease organisms and the result is the same: Low concentrations of Nano Silver kills disease-causing organisms. In addition, Nano Silver:

a. Is non-toxic to the environment and to living organisms since it leaves coalesces into larger ionic units which have no biological impact once it leaves the body
b. Leaves the body rather than accumulating in it due to its ultra-small size making overdose impossible
c. Cannot lead to the generation of new super bugs even with wide spread use since its mechanism of action does not permit organisms to develop resistance
d. Is inexpensive and has an indefinite shelf life, requires no refrigeration or other special care
e. Is self sterilizing, automatically killing disease causing organisms if it is contaminated by them
f. Is safe and effective for use in people of every age and condition and animals of all types
g. Has no known side effects
h. Does not kill beneficial bacteria leaving both gut and skin pro-biotic organisms intact while killing pathogens
i. Boosts white blood cell function, providing enhanced immune response

The Experiment: If Nano Silver were widely available, what would the results be?

1. Drug resistant organisms would no longer emerge in human or animal reservoirs

2. Resistant organisms in humans and animals would be killed off by the use of Nano Silver when they created disease. Over time, their numbers would decrease and the impact of disease from them would be either greatly reduced or eliminated

3. No new drug resistant organisms would emerge through the use of Nano Silver since its mechanism of action makes the acquisition of resistance impossible except through horizontal gene transfer. Any such organisms would be killed if they caused disease in humans or animals since they would be treated by Nano Silver.

4. Animals consumed for food would be significantly less toxic since Nano Silver, unlike the metabolites (by products) of antibiotic metabolism, does not remain in the body of either humans or animals

5. The amount of antibiotic and vaccine residue in effluent water and soil would decrease dramatically with marked environmental and health benefits since metabolites of drugs from the urine and feces of antibiotic and vaccine treated animals and humans poses and increasing health and environmental danger

6. Finely divided silver (without biological effect) would increase in effluent water and soil. This poses no known health or environmental danger.

7. The cost associated with antibiotic and vaccine therapy in humans and animals would be eliminated, to be replaced by a significantly lower cost

8. Pharmaceutical profits would drop dramatically since these two classes of drugs account for many billions of dollars of profit

9. Government and Union pension plans, as well as mutual funds, would loose value since they are heavily invested in major pharmaceutical stocks

10. Investing officers of pensions and mutual funds would seek other lucrative investments, including alternative energy and Advanced medicine options and companies, many of which have difficulty finding funding at this point because of the heavy investment in pharmaceutical and related, drug-based industries

11. Morbidity and mortality from nosicomial (hospital-acquired) infections would drop precipitously, eliminating a major health and health cost problem:

In the US in 1992, there were about 2 million nosicomial infections per year, =166,666 per month = 38,461 per week = 5,479 per day = 228 per hour =3 per minute. http://www.wrongdiagnosis.com/n/nosocomial_infections/stats.htm

Note: this equals approximately 10% of American hospital patients (CDC/NNIS 1992)

In 2004, 13% of all patients who acquired nosicomial infections died.

10. Nearly 100,000 people in the US alone would not die because nosocomial infections would be wiped out. “In the United States, the Centers for Disease Control and Prevention estimates that roughly 1.7 million hospital-associated infections, from all types of bacteria combined, cause or contribute to 99,000 deaths each year.” Pollack, Andrew. “Rising Threat of Infections Unfazed by Antibiotics” New York Times, Feb. 27, 2010

11. National, local and private health care costs would drop dramatically since the costs associated with antibiotics, vaccines and health care costs for infections would drop dramatically as well. In 2007, the direct costs of nosicomial infections Applying two different Consumer Price Index (CPI) adjustments to account for the rate of inflation in hospital resource prices, the overall annual direct medical costs of nosicomial infections to U.S. hospitals ranges from $28.4 to $33.8 billion (after adjusting to 2007 dollars using the CPI for all urban consumers) and $35.7 billion to $45 billion (after adjusting to 2007 dollars using the CPI for inpatient hospital services). (Costs of Hospital Acquired Infections in U.S. Hospitals Report,The Direct Medical Costs of Healthcare-Associated Infections in U.S. Hospitals and the Benefits of Prevention PDF 835 KB/16 pages, http://www.cdc.gov/ncidod/dhqp/)

12. Any pandemic, plague, or epidemic, whether intentional or unintentional, would be successfully halted by the universal application of Nano Silver orally.

13. Globalist plans for depopulation would be adversely impacted since communicable disease, including weaponized viruses, bacteria, etc., would be ineffective against a population supplied with Nano Silver.

14. Vaccine deniers would increase in number since epidemic diseases would be a thing of the past.

15. Globalists and their supporters would have to resort to means other than infectious agents, deadly drugs and dangerous, immune compromising vaccines to reduce the population. The 10-15% of the population which Bill Gates stated in a recent TED lecture could be eliminated through properly used vaccines would not die.

16. The myth of over population would suffer serious damage as the world population did not devour the available resources and the false mathematical and social engineering premises upon which it is based would be visibly flawed. See “Overpopulation, the Making of A Myth”, http://simranjeet.com/).

17. Local, clean and unadulterated food production could be instituted around the globe to enhance the health of people no longer dying from communicable diseases and parasites.

18. Chronic and deadly diseases like malaria, dengue fever, elephantiasis, tuberculosis, HIV and a host of others will become easily curable diseases.

19. Economic productivity and prosperity of poor and ill countries will rise as personal productivity increases due to decreased health care giver requirements and decreased time away from job and school.

20. Decreased overall health costs locally, nationally and internationally reversing some of the crushing burden of modern health costs through decreased hospital stays, increased infectious disease self care (fewer doctor and hospital visits and services), decreased drug and drug complication costs, less time away from job and school).

21. Increased Happiness Index, which is directly related to subjective (and, to a lesser degree, objective) measures of health.

21. Antibiotic and vaccine manufacturers will counter the loss of their market by political, propaganda and economic thrusts designed to eliminate Nano Silver. These will include
– Criminalizing and banning Nano Silver (already accomplished as of January 1, 2010 in the European Union and underway in the US)
– Deceptive science to “show” that the product is dangerous or ineffective
– Media campaigns to deride and/or demonize Nano Silver.

I think that covers most of the major impact of making Nano Silver widely and easily available. You have the good (health, autonomy, cost), the bad (pension and stock market impact) and the ugly (intentional, weaponized pandemics would be totally ineffective if they were based, as they have been to date, on infectious disease agents).

The net result? Stock up on Nano Silver, which we believe to have an indefinite shelf life.
We recommend the Silver Solution Nano Silver available at www.Nutronix.com/naturalsolutions because we believe that it is of exceptional quality and utility.

But whatever Nano Silver you choose to purchase, make sure that you have a good supply on hand. The apparently bioengineered Cryptococcus gatti fungi may be upon us as the next plague. MRSA may be the next plague. The next plague may be one that we have not heard of yet, but which has been in the works for years. Who know? Well, actually, it is very likely that WHO does know. But Nano Silver simply eliminates the threat of an infectious danger, IF you have it on hand and take it when the time is ripe.

I do. I hope that you do, too.

Yours in heath and freedom,
Dr. Rima
Rima E. Laibow, MD
Medical Director

Natural Solutions Foundation
The Dr. Rima Network: www.DrRima.net
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
Health Freedom Virtual Mall
www.Organics4U.org
www.NaturalSolutionsMarketplace.org
Valley of the Moon BeyondOrganic Coffee
www.ValleyoftheMoonCoffee.org
Valley of the Moon Eco Demonstration Project
www.NaturalSolutionsFoundation.org

TUESDAY 11 MAY 2010
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Mystery Disease Linked to Missing Israeli Scientist
Friday 07 May 2010
by: H.P. Albarelli Jr., t r u t h o u t | Report

(Photo: chickeninthewoods; Edited: Lance Page / t r u t h o u t)
Media outlets across the Northwest United States began reporting on April 24 that a strange, previously unknown strain of virulent airborne fungi that has already killed at least six people in Oregon, Washington and Idaho is spreading throughout the region. The fungus, according to expert microbiologists, who have expressed alarm about the emergence of the strain, is a new genotype of Cryptococcus gatti fungi. Cryptococcus gatti is normally found in tropical and subtropical locations in India, South America, Africa and Australia. Microbiologists in the United States are reporting that the strain found here, for reasons not yet fully understood, is far deadlier than any found overseas.

Physicians in the Pacific Northwest are reporting that an undetermined number of people in the region are ill from the effects of the strange strain. Physicians also say that the virulent strain can infect domestic animals as well as humans, and symptoms do not appear until anywhere from two to four months after exposure. Symptoms in humans include a lingering cough, sharp chest pains, fever, night-sweats, weight-loss, headaches and shortness of breath. The strain can be treated successfully, if detected early enough, with oral doses of antifungal medication, but it cannot be prevented, and there is no preventative vaccine. Undiagnosed, the fungus works its way into the spinal fluid and central nervous system and causes fatal meningitis.

The estimated mortality rate is about 25 percent of 21 cases analyzed. Several newspapers and media outlets in the US and overseas quote a researcher at Duke University’s Department of Molecular Genetics and Microbiology, Edmond Byrnes, as stating: “This novel fungus is worrisome because it appears to be a threat to otherwise healthy people. Typically, we see this fungal disease associated with transplant recipients and HIV-infected patients, but that is not what we are seeing.”

Microbiologists and epidemiologists studying the strain say the mystery fungus came from an earlier fatal fungus that was first found on British Columbia’s Vancouver Island in the fall of 2001, and perhaps as early as 1999. There the fungus infected and killed dogs, cats, horses, sheep, porpoises and at least 26 people. The disease spreads through spores carried by breezes and wind and when people and animals encounter infected ground where the fungus is present. A number of microbiologists say that the disease has “the potential to essentially travel anywhere the wind or people can carry it.” Reads an alarming study authored in part by Duke University’s Edmond Byrnes: “The continued expansion of C. gatti in the United States is ongoing, and the diversity of hosts increasing.”

Several researchers in California also note that the Cryptococcus gatti fungus has been researched for decades, extending back to the 1950’s, at the US Army’s biological warfare center, Fort Detrick, in Frederick, Maryland. One microbiologist at the University of California at Los Angeles recounted that the fungus was first brought to the attention of Fort Detrick researchers by British scientists experimenting with the bark of eucalyptus trees from Australia. Army biological warfare reports obtained through the Freedom of Information Act reveal that beginning around 1952 the Army mounted a huge research program involving numerous plant and fungi products, and that well over 300 long-term contracts and sub-contracts were let with over 35 US colleges and universities to carry out this multifaceted research. Examples of this early research in California included experiments and projects at Camp Cooke; Port Huemene; Harpers Lake; Oceanside, and extensive experimentation with wheat stem rust and “various spores” including “several from tropical locations” and cereal rust spores and dyed Lycopodium spores. Several Army reports reveal that private-sector corporations that participated or assisted in these projects were the American Institute of Crop Ecology; the American Type Culture Collection Inc.; University of California; Bioferm Inc. and the Kulijian Corporation.

The same microbiologist, who declined to speak on the record and who recounted extensive fungus work at Fort Detrick, also stated that researchers at Israel’s Institute for Biological Research, located in Ness-Ziona about 20 km from Tel Aviv, have worked with the Cryptococcus gatti fungus. They also report that mysterious Israeli-American scientist Joseph Moshe, 56 years old, may have conducted covert studies with the fungus while he was recently living in California. This report concerning Moshe is especially interesting because Moshe was briefly in the international spotlight in 2009 when he was the subject of a spectacular chase and arrest by the LA police department and SWAT team, assisted by the FBI, Secret Service, CIA, US Army and several other unidentified federal officials. That highly unusual arrest has never been fully explained to the media, and the whereabouts of Moshe has remained unknown since its occurrence. Compounding the mystery surrounding the Moshe case is that there is another scientist named Moshe Bar-Joseph who works in Israel and who looks remarkably like Joseph Moshe, except that he is about 20 years older.

Why Moshe was pursued and apprehended by the police is a largely unanswered question. According to the Los Angeles media, which recorded the entire incident by helicopter and ground cameras, Moshe claimed to be “a former Mossad microbiologist” who had telephoned a police dispatch number before his pursuit and had made “threatening statements about the White House and the president.” Reportedly, Secret Service spokesman Ed Donovan confirmed this when he spoke with several Los Angeles reporters.

On August 14, 2009, several Los Angeles police cruisers and an unmarked armored vehicle pursued Joseph Moshe as he drove his red VW automobile several miles through downtown Los Angeles before his car’s engine was reportedly knocked out by an electromagnetic pulse. Moshe refused to exit his car when ordered several times by the police, and after the driver’s window of his VW was smashed out by a robotic arm and several rounds of tear gas and pepper gas were fired into the vehicle, he still remained behind the wheel, refusing to move. At the time, police officers on the scene were stunned that Moshe was able to withstand three tear gas shells and hosing with pepper spray without moving. Later that day, a Los Angeles law enforcement official said: “I can’t explain that; there’s no way to explain that.”

After his apprehension, Moshe was taken to the Patton State Mental Hospital and then to the Twin Towers Correctional Facility in Los Angeles. Sometime about 60 days later, Moshe was quietly released and his current whereabouts are unknown. Since his arrest became public, reports about Moshe’s activities in the US have spread like wildfire, especially across the Internet. Many of these reports are unconfirmed, but a few come from credible sources and have linked Moshe to the grossly under-reported outbreak of flu in the Ukraine.

Other reliable sources, including two former Fort Detrick biochemists, have also linked Moshe to a mysterious disease that is becoming alarmingly common in Vermont and other states, including California. The disease is known to have killed or incapacitated at least 10 to 20 rural dwellers and farmers. This disease is said to be Morgellons disease or “a rare, mutated form of Morgellons disease.” Former Fort Detrick scientists, speaking off the record, say that the disease is one that was “experimented with intensely” in the late 1960’s at several “test sites in New England.” Morgellons causes patients to suffer horrible skin problems as well as fatigue, confusion and serious memory problems, as well as joint pain and the strange sensation that pins and needles are piercing the body or that something is crawling beneath one’s flesh. Some researchers and physicians believe that Morgellons is actually a psychiatric condition called “delusional parasitosis.” Other physicians, who are familiar with treating the disease, say it may be caused by “an airborne, unidentified spore” and that it was developed in the laboratory from an affliction that was first identified in the 1700’s. Regardless of its origin, some researchers say that Morgellons is becoming “a very real medical problem in some parts of the country.”

This work by Truthout is licensed under a Creative Commons Attribution-Noncommercial 3.0 United States License.

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