Fluoride is a multi-system poison. The Natural Solutions Foundation strongly opposes compulsory drugging through its addtion to the water systems of communities. We believe that this is both medically reckless and unconstitutional.
The Natural Solutions Foundation’s strongly anti-fluoride position for infants and children is now echoed by the American Dental Association (ADA) which says that children under 1 year should not be exposed to fluoride.
Although the US supported fluoride in infant formula during the 2006 Codex Committee on Nutritiona and Foods for Special Dietary Uses meeting in Chiang Mai, Thailand which dealt with infant formula and other special purpose foods, using data provided by the Natural Solutions Foundation, South Africa pushed the restriction on fluoride in healthy infants’ formula through, despite strong US objection.
Long a proponent of fluoridation of children’s teeth, the ADA joins the Natural Solutions Foundation in pointing out the dangers of the now-debunked toxin in infant’s bodies.
Rather than deal with the expense of safe disposal, the mining industry created the false belief that fluoride should be added to water, toothpaste, supplements, etc. That way, mining companies make a profit instead of taking a loss on fluoride which is expensive to dispose of according to EPA regulations. Despite propaganda to the contrary, fluoride has no known place in human metabolism and increases disease in those exposed to it. It is toxic to the brain, kidneys, bones, teeth, causes bone and other cancers at levels far lower than those permitted in water and has no known positive impact on human health despite oft-repeated but deeply flawed research claims to the contrary. Recent re-evaluation of the original research and other data make it clear that fluoride in any amount is a cumulative biological poison.
Although the United States has sought to add Fluoride to infant formula in the US and internationally, the World Health Organization recommends that infant formula be prepared in water which has no fluoride. Fluoridating water supplies means that infants will necessarily be exposed to amounts of fluoride which are toxic to them. “Little is known of the particular susceptibility of infants to fluoride but what we do know makes it clear that infant formula should be mixed with fluoride free water because fluoride is so toxic to them. Since infants are generally more sensitive to toxins than adults, banning it from formula is the only sensitive alternative,” according to Rima E. Laibow, MD, Medical Director of the Natural Solutions Foundation (http://www.HealthFreedomUSA.org).
Despite its wide acceptance as a water and food additive, and even as a “nutritional supplement,” fluoride is actually a dangerous metabolic poison with permanent effects at levels much lower than 1 part per million (ppm). Exposure is cumulative since fluoride is a bio-accumulator which remains in the body and can cause cancer, kidney failure, bone disease, including bone cancers, structural damage to bone and teeth, thyroid poisoning, pineal gland calcification, reproductive failure, synergistic increases in lead poisoning when both are present, endocrine disruption leading to diabetes, other cancers and decreases in the availability of essential nutrients like magnesium.
In addition to water, the FDA allows sodium aluminum fluoride (cryolite) to be sprayed on more than 30 fruits and vegetables at up to 7 ppm. The USDA set a 1.2 ppm limit for arsenic and fluoride pesticides in 1933 since they are equally toxic. While arsenic sprays have been phased out, fluoride ones are increasingly popular and now can be used not only on food but on food storage areas as well. Current FDA water fluoridation standards allow up to 4 ppm and assure on-going fluoride contamination for most Americans.
Industry pressure is strong to increase the amount of fluoride we ingest: DOW Chemical uses extremely high fluoride tolerances on a wide number of common foods including 98 ppm for wheat germ, 40 ppm for wheat bran, 31 ppm for rice bran, 30 ppm for some nuts, 28 ppm for corn meal, 26 ppm for corn flour, 25 ppm for millet, wild rice, sorghum and wheat grains and 17 ppm for oat grain.
Leading scientists have called for a ban on all fluoride usage in light of its devastating impact on health and a recent evaluation of the data upon which fluoridation was initially approved by the FDA for municipal water supplies was deeply and fraudulently distorted when presented to the FDA and the public since toxic results were not revealed in the group receiving fluoridated water.
Vaccines often contain fluoride as an adjuvant or immune system irritant to provoke the immune system into producing more antibodies with fewer antigens since antigens are the expensive part of vaccines. Since vaccines also frequently contain aluminum hydroxide, the synergistic toxicity of the two toxins is significantly more than the toxicity of either toxic metal alone at the same dosage. This problem is repeated in municipal water supplies since fluoride is added for its alleged dental health benefits while aluminum salts are added to “polish” the water and give it an appealing gleaming appearance.
Fluoride as an additive has a dark past: it was first added to water in the Soviet Gulag (prison system) since it is a neurological poison and made political and other difficult prisoners complacent and therefore easier to manage. It was added to the water supplies of the Nazi death and slave labor camps for the same reason. Fluoride is widely used as an additive although the scientific evidence upon which its use rests is either fraudulent or flawed. Long a staple of water treatment, sodium fluoride has been replaced by other, even more toxic fluoride compounds like sulfuryl fluoride which has never been tested in water supplies nor approved for use in them.
The New York State Attorney General has expressed support for banning this dangerous but widely used pesticide. Fluoride contamination from either natural sources or its addition to liquids and products used by children results in dental fluorosis, a permanent mottling of teeth which is both cosmetic and structural, and similar structural damage to bone associated with increased fractures, osteoporosis (bone loss) and demineralization of bone. IQ loss and other neurological damage is due both to the fluoride itself and the dangerous interaction of fluoride with lead since fluoride renders lead even more toxic to the brain. Fluoride without lead leads to loss of higher cognitive functions including decision-making and IQ.
Yours in health and freedom,
Dr. Rima
Medical Director
Natural Solutions Foundation
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
www.NaturalSolutionsFoundation.org
www.Organics4U.org
www.NaturalSolutionsMarketPlace.org
www.NaturalSolutionsMedia.tv
DONATE NOW http://drrimatruthreports.com/index.php?page_id=189 All deductions are tax deductible if you pay taxes in the US.
For donations in multiples of $25, we’ll say “Thanks†with a 1/2 lb bag of our full bodied Valley of the Moon(TM) Coffee: Shade Grown, GMO and Chemical Free Coffee from the Chiriqui Highlands of Panama, it’s Friendly Food Certified: Friendly to Your Health, Friendly to the Workers and Friendly to the Environment http://drrimatruthreports.com/?page_id=1130
Citing price as the reason, Alaska authorities backed off requiring – and providing – Gardasil shots to young girls and women.
While it is possible to see this announcement as just another cost-cutting measure, the liklihood is that the serious controversy around this unnecessary, dangerous and ineffective vaccine which actually increases cervical cancer incidence in women by as much as 44.7% is the real cause for this back-off.
Whatever the reason, girls in Alaska whose families cannot pay for this shot are a great deal better off than girls whose families can afford it and do make the much hyped, but dangerous decision to give their daughters Gardasil.
Vaccination is so dangerous, despite the hype and hoopla which supports this very profitable segment of the pharmaceutical industry, that it is a totally uninsurable risk. That means that no insurance company will provide a policy to the manufactures to protect them from the liability law suits that they could be exposed to when their products cause harm.
Who will pay if Gardasil causes death and damage? Surely not Merck, Gardasil’s manufacturer. The FDA, the supposed “regulatory agency” which keeps dangerous products off the market, bowed to pressure and conflict of interest and rushed Gardasil through without adequate trials to establish even short term safety. And it has done something else. It has removed any threat of liability from any drug or vaccine manufacturer who causes harm through their product IF that product has been approved for any thing at all by the FDA.
So who will pay for the death and damage to otherwise healthy girls and women who died or were crippled in the immediate post-vaccination period? Who will pay for the cancers and deaths yet to come in a poorly tested vaccine which was rushed to market to make, literally, a killing without proper evaluation? Who will compensate women who cannot bear children as a consequence of this vaccination for the grief of their infertility, should that be one of the long-term effects of Gardasil injection? Who will pay for the injury to children and husbands who loose their mothers and wives prematurely if Gardasil is a long-term killer?
No one.
Yours in health and freedom,
Dr. Rima
Medical Director
Natural Solutions Foundation
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
www.NaturalSolutionsFoundation.org
www.Organics4U.org
www.NaturalSolutionsMarketPlace.org
www.NaturalSolutionsMedia.tv
DONATE NOW http://drrimatruthreports.com/index.php?page_id=189 Tax deductible
For donations in multiples of $25, we’ll say “Thanks” with a 1/2 lb bag of our full bodied Valley of the Moon(TM) Coffee: Shade Grown, GMO and Chemical Free Coffee from the Chiriqui Highlands of Panama is Friendly Food Certified: Friendly to Your Health, Friendly to the Workers and Friendly to the Environment
http://drrimatruthreports.com/?page_id=1130
State limits access to 2 free vaccines
SCHOOL PROGRAM: 15 others will still be offered but these were too costly.
By GEORGE BRYSON
gbryson@adn.com
Published: November 7th, 2008 02:28 AM
Last Modified: November 7th, 2008 11:16 AM
For the first time in more than 30 years, the State of Alaska will no longer offer all vaccinations free to all Alaska schoolchildren, the state Division of Epidemiology reported this week.
When the new policy begins on Jan. 1, two of the newest and most expensive vaccines — immunizations for girls to prevent cervical cancer and for both boys and girls to prevent meningitis — will only be offered free to low-income, uninsured or Alaska Native and American Indian children.
Other Alaskans will have to rely on health insurance policies to cover the expense, or pay for the vaccines themselves.
Federal funding of the state’s universal immunization program has failed to keep pace with the increasing cost and rising number of recommended vaccines, said Laurel Wood, manager of the Alaska Immunization Program.
For that reason, the state will cut back on two of more than a dozen vaccines it currently distributes to Alaska health care providers at no cost, including:
• Gardasil, the human papillomavirus (HPV) vaccine for girls, and
• Menactra, the meningococcal vaccine for boys and girls.
Under provisions of the federally funded Vaccines for Children program, both immunizations will continue to be offered free to young Alaskans who are Medicaid-eligible.
They will also be offered at federally funded health clinics (including the Anchorage Neighborhood Health Center) to “under-insured” children whose family policies don’t cover the cost of vaccines.
Fifteen older vaccines — including immunizations to protect children against hepatitis, diphtheria, polio, tetanus, measles, mumps, chickenpox and influenza — will continue to be offered free to all Alaskans under 18 years of age, regardless of income or insurance.
ADVERTISEMENT
After the cutback, about 4,000 Alaska girls in need of the HPV vaccine and about 5,500 boys and girls in need of the meningococcal vaccine won’t be covered, Wood said.
The meningococcal vaccine costs the state $76 a dose, Wood said. The HPV vaccine — which requires three doses over a period of six months — costs about $300 per child for the complete series.
Trying to provide those vaccines at no cost to all Alaska school children would require an additional $1.6 million, Wood said.
The number of recommended vaccines has grown along with their costs, the Alaska Epidemiology Bulletin reported this week. In 2000 the entire battery of recommended vaccines cost $219 per child. Today the cost is $1,120 for boys and $1,429 for girls.
The cost of the HPV vaccine is the budget-buster.
Last year the state managed to cover that extra cost by tapping additional funds provided by the federal Centers for Disease Control and Prevention, Wood said. But that was a one-time fix.
“It was basically a disproportionate amount of money for the size of our population compared with other states,” Wood said.
Since the HPV vaccine was first made available in June 2007, the state has distributed 33,000 free doses to girls between 9 and 18 years of age, Wood said.
The vaccine is recommended for young women up to the age of 26, but it’s not mandatory to attend public schools.
The meningococcal vaccine was first made available in January, 2006. Since then the state has distributed about 36,000 free doses to boys and girls between 11 and 18 years of age,” Wood said.
Persons with questions about the Alaska Immunization Program should contact the state Division of Public Health at 269-8000 or 1-888-430-4321.
http://www.adn.com/news/alaska/story/581569.html
Recently a reader wrote to me the following,
“Is it true that you charge $19.95 for your Codex eBook (http://drrimatruthreports.com/index.php? page_id=205)? I am on a limited income and want information that I do not have to pay for.” MK
Here is my response:
“Yes, there is a charge for our eBooks. But we make huge amounts of information available for free including our Health Freedom Blog (second button on the left on our home page, www.HealthFreedomUSA.org, and our Health Freedom eAlerts.
Every page on the website, and there are thousands of them, is free and if you go to www.NaturalSolutionsMedia.tv or www.Youtube.com/naturalsolutions.com you will find many, many resources.
We want all of our supporters, rich or poor, young or old, to be able to have information, share it with others and take action.
Real Advocates Have Real Expenses
We have real expenses, though, regardless how charitable our intentions are so donations (http://drrimatruthreports.com/index.php?page_id=189) are urgently needed.
Let’s fact it: we SHOULD have been at the vitally important meeting in South Africa this month when the Codex Committee on Nutrition and Foods for Special Dietary Uses (CCNFSDU) met earlier this month. We have worked for years to build a coalition of the unwilling, those countries which do not want GMOs in their food supply, especially unlabeled.
We could not attend because we did not have the money to buy the tickets, pay for the hotel rooms, for meals, etc.
So the world of people who want health (and food) freedom lost a great deal.
Small contributions mount up if there are a lot of them. Big contributions help, of course. But if you are able to give even a dollar a month, you should. Go to our home page and click on the “donate” tab and then either use credit cards, pay pal or send a check. But do it.
Most people (that’s 96% of 186,000+) people do not take this responsibility seriously. They they wonder why we cannot do everything they -and we – think needs to be done. Hmmm. Maybe it is because we are understaffed and severely underfunded while the other side has more money than God to accomplish its tasks.
Do you buy coffee? Buy it from Natural Solutions Foundation. Do you buy vitamins? Buy them from Natural Solutions Foundation. Do you buy magnets? Buy them from the Natural Solutions Foundation. Do you rent movies? Rent them from Natural Solutions Foundation on our Home Page. Do you have small balances left over on your gift cards? Donate those small amounts to the Natural Solutions Foundation.
There is a reason that we ask people to do these things – it is so we can fight the health freedom battle effectively.
Don’t give anything and there won’t be anything to protect your health and your health freedom.
And if you cannot donate or purchase, that’s fine, too, as long as you are organizing your email list and your community.
The information is out there. Each and every one of us has a role to play. Are you playing yours? If you are, congratulations, and thanks.
And if you are not, why not?
Yours in health and freedom,
Dr. Rima
Medical Director
Natural Solutions Foundation
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
www.NaturalSolutionsFoundation.org
www.Organics4U.org
www.NaturalSolutionsMarketPlace.org
www.NaturalSolutionsMedia.tv
DONATE NOW http://drrimatruthreports.com/index.php?page_id=189 All deductions are tax deductible if you pay taxes in the US.
For donations in multiples of $25, we’ll say “Thanks†with a 1/2 lb bag of our full bodied Valley of the Moon(TM) Coffee: Shade Grown, GMO and Chemical Free Coffee from the Chiriqui Highlands of Panama, it’s Friendly Food Certified: Friendly to Your Health, Friendly to the Workers and Friendly to the Environment http://drrimatruthreports.com/?page_id=1130
There is a great deal of misinformation about silver solutions. While there are several kinds (ionic, colloidal, nano technology, protein silver), the safety of silver is extraordinary, despite the fear of turning blue (argyria) which has been promulgated over the years.
The truth is that virtually no one has ever turned blue because of a deposition of silver particles in the skin. In the documented case where this has happened, the person drank huge and irrational amounts of silver daily for decades. In the recent well-publicized case of a politician who was supposed to have turned blue from drinking silver, it turned out to be a hoax perpetrated by his political opponents in the campaign for office he was participating in.
The smaller the particle size, the more effective the silver is at disrupting the biological function of disease causing bacteria, mycoplasma and viruses. The smaller the particle size, the more efficiently the body can get rid of the silver.
The silver we recommend, ASAP silver sol solution is exceedingly small in size, has never been shown to provide any medical or health problems and has been used for people from infancy to people in their 90s.
Here are the facts as I see them, after extensive experience using silver for infections of all types:
1. Silver in nano sized particles does not cause argyria because the particles are small enough to pass easily out of the urine, rather than being deposited in tissues. No case of argyria has ever been reported with nano particle silver
2. As you said, the amounts you would have to consume border on the insane.
3. Nano silver is effective, without any known side effects, against every pathogen it has been tested against
4. Through its applications in Africa, we know that pregnant women, tiny babies, fragile elderly, people with diabetes, cancer, auto immune disease, etc., do not develop side effects when they take silver as directed.
5. No ulcers have ever been reported with nano silver
6. The silver we recommend has been shown NOT to kill beneficial bacteria, thus protecting the integrity of the gut and the immune system.
ASAP silver sol solution has been tested against more than 650 pathogenic organisms and has been effective in vitro (in the lab) against every one. It has also been tested against the normal bacteria (which we refer to collectively as “pro biotics”) and found, rather amazingly, to spare these beneficial bacteria.
I personally never travel without ASAP silver sol solution. I have used it for common ailments like a cold and uncommon ones like malaria. It can be taken via sub lingual administration directly under the tongue to speed absorption and prevent it from reaching the GI tract or it can be mixed in a small amount of water and taken by mouth. It has no flavor or taste so even babies can take it without distress.
We have concluded a special arrangement with Nutronix.com to allow us to offer you this silver sol solution. Please do yourself a favor and lay in a good supply of this outstanding health aid.
Click here, http://www.Nutronix.com/naturalsolutions, to get your supply. Click on the “Products” tab, then go to the left hand column and click on “Silver Solutions”.
It is not clear how long the FDA will allow this exceptional product to remain on the market. I suggest you stockpile it for pandemics, general disease use and immune system boosting.
Yours in health and freedom,
Dr. Rima
Medical Director
Natural Solutions Foundation
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
www.NaturalSolutionsFoundation.org
www.Organics4U.org
www.NaturalSolutionsMarketPlace.org
www.NaturalSolutionsMedia.tv
Effect of Prophylactic Treatment with ASAP-AGX-32 and ASAP Solutions on an Avian Influenza A (H5N1) Virus Infection in Mice
Gordon Pedersen,American Biotech Labs
Sidwell, Robert W., The Institute for Antiviral Research of Utah State University Animal, Dairy and Veterinary Sciences Dept
Alan Moloff, D.O., M.P.H., Colonel, MC, U.S. Army (RET)
Robert W. Saum Ph.D., IDHA, Medical Science and Technology, American Biotech Labs
Introduction
Avian Influenza (H5N1, or Bird Flu) can be a fatal disease in humans and a serious threat to become a pandemic event. Since there is no pharmaceutical remedy for the Bird Flu it is essential that preventive treatments be tested and developed in order to enhance survivor rates in the human population.
Since 1973, Silver has been shown to have topical activity against 22 bacterial species (643 isolates) including gram positive and gram negative bacteria1. As an antimicrobial agent, Silver has been shown to be beneficial in the treatment and prevention of burn infections, post surgical wound infections, and gynecological infections2, 3. In addition, Silver has been shown to be active against black mold4, Anthrax5, Bubonic plague6, Malaria7, and numerous viruses such as Hepatitis 8.
Recently it was reported that the American Biotech Labs product, Silver Sol, demonstrated additive and synergistic effects when combined in individual trials with 19 different antibiotics9. The Silver
from ABL was shown to improve the effectiveness of the antibiotics even against
antibiotic resistant infections 9.
The Merck Index identifies the following medicinal uses of silver: Antiseptic particularly for mucous membranes and infectious sinusitis10. The Merck Manual and Centers for Disease Control, recommend that Silver nitrate drops should be placed in each infant eye as soon as possible or at least in the first half hour of life to prevent gonorrheal ophthalmia 11.
The safe use of Silver as an orally consumed preventive agent has been demonstrated and supported by reports from the EPA and the United States Department of Health and Human Services in a 76 week long study12,13. Dogs that inhaled Silver showed activity in the lung in one hour with 90% of the silver carried to the liver by the blood within 6 hours14.
Due to the increased risk from methicillin resistant bacteria, black mold, plasmodium and especially bird flu, the need for orally consumed, safe, daily prophylactic prevention exists. In this study, Silver Sol from American Biotech Labs demonstrates safe beneficial and preventive activity against H5N1 Bird Flu, when taken orally in mice.
The American Biotech Labs product, ASAP- AGX-32, as well as their product designated ASAP, to be virucidal against the avian influenza A/Vietnam/1203/2004 (H5N1) x A/Ann Arbor/6/60 hybrid virus, with an up to 2 log10 virus titer reduction occurring after a 6 h incubation of the product and the virus
(USU report dated March 28, 2006). In that same report, similar incubation with the avian influenza A/Duck/MN/1525/81 (H5N1) virus reduced the virus titer by approximately one-half log10 in the same
time period. This material is reportedly very well tolerated in human subjects when ingested orally, Dr Gordon Pedersen of American Biotech Labs designed a study with the Centers for Antiviral Research to
evaluate the potential for ASAP-AGX-32 and ASAP, to inhibit an avian influenza A (H5N1) virus infection of mice when administered orally to the animals beginning 1 week prior to virus exposure. This report describes the results of this experiment.
Materials and Methods
Animals: Female specific pathogen-free 18- 21 g BALB/c mice were obtained from Charles River Laboratories (Wilmington, MA). They were quarantined 5 days prior to use. They were housed in polycarbonate cages with stainless steel tops and provided tap water and mouse chow ad libitum.
Virus: Influenza A/Duck/MN/1525/81 (H5N1) virus was originally provided by Dr Robert Webster of the St. Jude Hospital (Memphis, TN). The virus was adapted to mice by passage twice through weanling animals and a large pool prepared in MDCK cells for use in this study. The virus was titrated in young
adult mice prior to use in the present experiment.
Compounds: ASAP and ASAP-AGX-32 were provided by Dr Pedersen. They were in blue bottles, so all studies run with each were performed using the materials in injection bottles covered with aluminum foil to avoid light exposure. All were stored at room temperature until used. It is understood that the ASAP solution contained a colloidal silver at a concentration of 10 ppm, and the ASAP-AGX-32 contained the same colloidal silver at a concentration of 32 ppm. Ribavirin, included as a known positive
control, was provided by ICN Pharmaceuticals, Inc. (Costa Mesa, CA); it was dissolved in sterile saline and stored at 4o C until used.
Arterial Oxygen Saturation (SaO2) Determinations: SaO2 was determined using the Ohmeda Biox 3800 pulse oximeter (Ohmeda, Louisville, OH). The ear probe attachment was used, the probe paced on the thigh of the animal. Readings were made after a 30 sec stabilization time on each animal. Use of an earlier Ohmeda Model (3740) for measuring effects of influenza virus on SaO2 in mice has been previously described by Dr.s Sidwell and Pedersen15.
Lung Score Determinations: Each mouse lung removed and placed in a petri dish which, using a permanent black marker, had been divided into sections which were pre- numbered from 1 through 3 or, for placebo controls, 1 through 5. Each lung was assigned a score ranging from 0 (normal appearing lung) to 4 (maximal plum coloration in 100% of lung). These scores were assigned blindly, with the individual doing the scoring not being aware of what group was being examined. An arithmetic mean was determined for each group.
Lung Virus Titer Determinations: Each mouse lung was homogenized and varying dilutions assayed in triplicate for infectious virus in MDCK cells as described previously16. Each lung homogenate was
centrifuged at 2000 g for 5 min and the supernatents used in these assays.
Experimental Design: Groups of 19 mice were treated by oral gavage (p.o.) with either ASAP-AGX-32 or ASAP twice daily (every 12 h) for 7 days, then infected intranasally (i.n.) with an LD70 dose of
influenza virus, then treated an additional 10 days. A similar group of mice were treated p.o. with ribavirin at a dosage of 75 mg/kg/day twice daily for 5 days beginning 4h pre-virus exposure. The infection was achieved by anesthetizing the mice with an intraperitoneal injection of Ketamine at a dosage of 100 mg/kg and instilling 90 µl of suspended virus in minimum essential medium on the nares of the animals. As controls, 35 mice were treated with water using the identical schedule as used for the
ASAP materials and infected as above. Ten infected, test substance-treated mice and 20 water-treated controls were observed daily for deaths for 21 days after virus exposure, and SaO2 levels ascertained on days 3-11, which were the times when this parameter usually declines. From the remaining infected, treated animals, 3 test substance-treated and 5 water-treated control mice were killed on days 1, 3 and 6, and their lungs removed, assigned a consolidation score, weighed, and assayed for virus titer.
As toxicity controls, 3 uninfected mice were treated in parallel with each test material and observed for signs of adverse effects for 21 days. The weights of these mice as well as 5 normal controls were determined prior to initial treatment and again 18 h after final treatment to determine if the treatments
affected host weight gain. Three normal controls were also sacrificed on days 3 and 6 to provide background lung data.
Statistical Analysis
Increases in total survivors were evaluated by chi square analysis with Yates’ correction. Increases in
mean day to death, differences in mean SaO2 values, mean lung weight, and mean virus titers were analyzed by t-test. Only animals dying up to day 21 were considered for mean day to death calculations. The Wilcoxon ranked sum analysis was used for mean lung score comparisons. Each
statistical test was run using Excel software on a MacIntosh computer.
Results and Discussion
The results of this experiment are summarized in Table 1 and in Figures 1-4. As seen in Table 1, the virus challenge in this experiment was lethal to 14 of the 20 placebo-treated mice, with the mean day to
death being 8.4 days. Such a pattern of death is considered ideal for evaluation of potential antiviral agents. This optimal condition was verified by the observation that Ribavirin was fully protective to the
mice, preventing any deaths from occurring (Table 1), significantly lessening SaO2 declines (Figure 1), inhibiting lung score development (Figure 2), lung weight increase (Figure 3), and lung virus titer
increases (Figure 4).
Treatment with ASAP-AGX-32 appeared to not affect the numbers of animals dying of influenza, although a half-day delay in mean day to death was seen (Table 1). SaO2 declines in this group of treated mice were almost at the same rate as those in the placebo controls, although it was interesting
that on the first day this parameter was assayed, a highly significant (P<0.001) difference was seen (Figure 1). SaO2 declines are a manifestation of declining lung function, suggesting that the lung consolidation in the lungs did not progress as rapidly as seen in the placebo controls. The treatment appeared to moderately lessen lung consolidation as seen by lower lung scores on each time evaluated, the day 6 mean lung score being significantly (P<0.05) less than the placebo treated controls (Figure 2). Lung weights, another indication of fluid developing in the lungs to cause pneumonia in the animal, were also less at each time point than seen in the placebos (Figure 3). The mean lung virus titers in the
mice treated with ASAP-AGX-32 were lower than the placebo controls on days 3 and 6 of the infection (Figure 4).
Treatment with ASAP, which we understand is a less-concentrated version of ASAP-AGV- 32, also provided some intriguing results. Especially of interest was the observation that 60% of the infected mice treated with this compound survived compared to the 30% in the placebo-treated controls. Although not statistically significant because of the number which survived in the latter controls, this effect is strongly suggestive a disease-inhibitory effect may have occurred. At two time points during the SaO2 assays, days 3 and 6, the declines normally seen were significantly lessened (P<0.01), and
there was a general lessening of decline throughout the times of assay (Figure 1). Modest inhibition in lung scores were seen in this treated group as well, especially on day 6 (Figure 2); the lung weight data did not correlate too well with the lung scores, however (Figure 3). Again, slight inhibition of lung virus titers were seen in the ASAP- treated, infected mice (Figure 4).
Both the ASAP formulations were well tolerated by the toxicity control mice as seen by no deaths occurring in them and host weight increases observed during time of therapy. Ribavirin, while not lethal to the mice, did result in a 0.4 g host weight loss (Table 1); this was an expected effect for the latter material, since the maximum tolerated dose is approximately 100 mg/kg/day.
It is difficult to attribute the effects seen in this experiment wholly to viral inactivation, since both test materials were administered orally to animals infected by direct nasal inhalation, although the treatments began one week before virus exposure, so it is possible that a portion of the Silver Sol may
have been able to be in the vicinity of the virus-exposed lung tissue. It is also possible that this material is exerting a mild immunomodulatory effect in the animals, which would provide modest protection
against the infection. If such a mechanism is indeed associated with the potential activity seen, then a different treatment schedule, perhaps limiting the number of treatments to one per day or once every other day, may enhance any immune modulatory effects, since it is recognized that too-frequent dosing may overtax the immune system. The greater protection seen by the lower- dosed ASAP material could be explained by immunomodulation, since the greatest immunologic effect is not necessarily at the
highest dose used.
Another mechanism whereby the ASAP materials may have inhibited the influenza virus infection in these studies may simply be one of coating the virion with Silver Sol to prevent attachment and penetration. Again, the material would need to be in the vicinity of the exposed lung tissues at the time
infection was initiated. The Silver material could also play a role in limiting apoptosis of the epithelial lining of the lung induced during acute lung inflammation. Apoptosis plays a causative role in acute lung injury in part due to epithelial cell loss.
Further studies would have to be conducted to more fully delineate the actions of this material.
It is acknowledged that the effects seen in the present study, while of considerable interest, would need to be repeated to confirm that the observations were not due to mere chance. Consideration of combined use of oral administration of the ASAP materials and intranasal instillation at near
the time of virus exposure would determine
whether the effects seen were indeed
associated with virucidal effects of these
materials.
Summary
Mice infected with avian influenza A/Duck/MN/1525/81 (H5N1) virus were treated with the Silver Sol-containing formulations ASAP-AGX-32 and ASAP provided by American Biotech Labs. Oral gavage treatment began 7 days prior to virus exposure and continued twice daily for a total of 17 days. Treatments with both formulations provided a suggested inhibitory and preventive effect on this virus infection as seen by either less animals dying in the treated groups than in the placebo-treated
controls, delay in mean day to death, lessened SaO2 decline, modest inhibition of lung consolidation, and/or lessened virus titers in the lungs. Ribavirin was included as a positive control drug, used orally at a dose of 75 mg/kg/day twice daily for 5 days beginning 4 h pre-virus exposure, and this treatment was markedly inhibitory to the infection as expected.
References
1. Carr, H., Wlodowski, T., 1973. Department of Microbiology, College of Physicians and Surgeons, Columbia University, New York. Antimicrobial Agents and Chemotherapy. 10:585-587.
2. Fox, C. J. Jr., 1968. Silver sulfadiazine, a new topical therapy for Pseudomonas burns. Arch. Surg. 96:184-188.
3. Fox, C. J., 1969. Control of Pseudomonas infection in burns by Silver Sulfadiazine. Surg.Gynecol. Obstet. 128:1021-1026.
4. U.S. House International Relations Committee, 2005. Written testimony on Black Mold.
5. Illinois Institute of Technology. 2001. Anthrax.
6. Robinson, R., 2003. Bactericidal activity of ASAP Silver Solution on Yersinia Pestis, the etiological agent of plague. Department of Microbiology, Brigham Young University.
7. U.S. House Relations Committee. 2005. Written testimony on Malaria.
8. Hafkine, A., 2003. ASAP antiviral activity in Hepatitis B; DNA Polymerase Inhibition, Reverse Transcriptase Inhibition. Hafkine Institute for Training, Research and Testing.
9. DeSousa, A., Mehta, D., Leavitt, R. W., 2006. Bactericidal activity of combinations of silver-water dispersion with 19 antibiotics against seven microbial strains. Current Science. 91:7- 11.
10. Merck Index, 2006. Silver 1:645.
11. Merck Index, 2006. Silver 1:2082.
12. EPA Research and Development, 1988. Drinking water criteria document for Silver. Office of Health and Environmental Assessment.
13. U.S. Department of Health and Human Services, Public Health Service and Agency for Toxic Substances and Disease Registry, 1990. Toxicological profile on Silver.
14. Phalen, R.F. and Morrow P.E., 1973. Experimental Inhalation of Metallic Silver, Health Physics 24: 509-518.
15. Sidwell, R.W., Huffman, J. H., Gilbert, J., Moscon, B. Pederson, G., Burger, R. and Warren, R.W. 1992. Utilization of pulse oximetry for the study of the inhibitory effects of antiviral agents on influenza
virus in mice. Antimicro Agents Chemother 36:473-6.
16. Sidwell, R.W., Huffman, J. H., Call, E.W., Alaghamandan, H., Cook, P.D, and Robins, R.K. 1985. Effect of Selenazofurin on influenza A and B virus infections in mice. Antiviral Res. 6:343-353.
Another theoretical “impossibility†becomes real by experiment. Water burning? Yes, it can!
Materials Research Innovations, March 2008, Vol 12, 3-5.
Table 1. Expt. ABLA-1. Effect of Oral Gavage Prophylactic Treatment with ASAP-AGX-32 and ASAP on an Influenza A (H5N1) Virus Infection in Mice.
Animals: Female 18-21 g BALB/c mice Virus: Influenza A/Duck/MN/1525/81 (H5N1) Drug diluent: Company diluent Treatment schedule: bid x 17 beg -7 days (Ribavirin: bid x 5 beg -4 h) Treatment route: p.o. Experiment. duration: 28 days Tax Controls Infected, Treated Mice Tax Controls Dosage
Surv/Total Mean Host Weight Change (g) Surv/Total Mean Day to Death ± SD Mean Day 11
SaO2 (% =± SD) ASAP- AGX- 32 32ppm 3/3 1.8 2/10 8.9 ± 1.4 75.4 ± 1.0
ASAP 10ppm 3/3 1.4 6/10 7.3 ± 1.0 76.7 ± 2.1 Ribavirin 75 mg/kg /day 3/3 -0.4 10/10*** >21.0 ± 0.0*** 86.6 ± 2.5** * H2O — — — 6/20 8.4 ± 1.8 76.0 ± 1.9 Norma l Contro ls — 5/5 2.3 — — 88.8 ± 3.0
Difference between initial weight and weight 18 h after final treatment.
Difference between initial weight and weight 18 h after final treatment.
*P<0.05; **P<0.01; ***P<0.001 compared to H2O -treated controls.
As a physician I was trained to understand that there is a physicial underpinning to the function – or dis function- of any biological creature. It’s name? Biochemistry. Molecules support, or prevent, poison or allow all chemical reactions in the body. And there are lots of them. Every one of our trillions upon trillions of cells is carrying out about 35,000 enzymatic reactions at any moment and each of them is part of a chain of reactions that allow – or prevent – events “downstream” from that particular enzyme and its tasks.
Enzymes are robots. They are complexes of proteins (made up of chains of amino acids) and “nutritional metals” like magnesium, zinc, manganese, copper, and others). They have sulfur and other non metals and they are very, very precise.
After an enzyme does what it is there to day (for example, transferring a molecule from one side of a membrane to another) its shape has changed so it can no longer function, like a fork lift truck with its blades on backwards. Then another enzyme comes along and returns it to its origianl shape so that it can do the same job over again. The helper enzyme is now literally “bent out of shape” and ANOTHER enzymes comes along and fixes the fixer enzyme and then, you guessed it! Yet another enzyme fixes the fixer of the fixer. On and on it goes, one enzyme performing its job, then unable to perform again until another enzyme resets it, then needing to be reset itself.
If one step in this astonishing molecular dance is missed, there are consequences. If the cause of the mis-step is a drug, the consequences have a special name, “Side effects”. If the cause is the chronic lack of nutrients, only a few doctors understand that the disease which is identified is, in fact, chronic under nourishment. The treatment for most doctors trained in allopathic medicine is exactly wrong almost all of the time: they give drugs to poison more enzyme systems.
WHAT? That is, in a nut shell, the entire basis of pharmaceutical medicine. The only time I can see that it is justified, the ONLY time, is in the Emergency Room. Other than that, it has no place.
But for a few doctors, and many non-doctors, the treatment is obvious: if there is a deficiency not of a drug, but of a nutrient, or many, give the nutrient and its companion nutrients. Give it in a high enough dose that even starving cells and membranes can find the energy to absorb and begin to use the nutrients. And, Voila! people get better. Pretty much, in my experience, every single time.
This simple, intuitive and obvious fact is not at all obvious to those whose minds have been altered by drugs, either by the “education” shaped by the interests of the drugs (often referred to by its short hand name, “Medical School”) or drug regulators and others whose ability to think have been poisoned by the money involved in the drug system – more than all other industries when taken in the aggregate!
Science is often the last to know, like the girl whose boy friend is dating her best friend. Science has taken this long to notice that if you give children nutrients their brains function better. The article below, from the British Journal of Nutrition says that the paper published below is breaking new ground since this is the first time that the positive impact of nutrients on children’s capacity to carry out tasks has been shown to be impacted by supplements.
Or is it just that selective science is the last to know?
Consider:
Benton D; ILSI Europe a.i.s.b.l., The influence of children’s diet on their cognition and behavior., “… there is a growing body of evidence that diet can influence the development and functioning of the brain. Several lines of evidence support the view that the diet of the mother during pregnancy, and the diet of the infant in the perinatal period, have long-term consequences…”, Eur J Nutr. 2008 Aug;47 Suppl 3:25-37.
or
Gajre NS, Fernandez S, Balakrishna N, Vazir S., Breakfast Eating Habit and its Influence on Attention-concentration, Immediate Memory and School Achievement., “RESULTS: Comparison between groups indicated significant differences in the letter cancellation (LC) total scores with the regular breakfast group achieving the highest mean scores compared to the no breakfast group (P< 0.05). Marks scored by the regular breakfast group in subjects - Science, English and total Percentage were significantly higher compared to those scored by the children in the no breakfast group. Regular breakfast eating habit and weight for age percent were significantly (P< 0.001) associated with immediate recall memory score explaining 4.3 percent variation. CONCLUSIONS: Regular habit of eating breakfast as opposed to irregular consumption or skipping breakfast altogether had beneficial influence on attention-concentration, memory and school achievement.", Indian Pediatr. 2008 Oct;45(10):824-8.
or about a zillion other articles, books and studies showing the same thing. So why is this "news" rediscovered with wonder and astonishment over and over and over and over and over and....?
Because supplements are cheap and safe. And because doctors - and patients and parents - have been trained to discount this reality, provide garbage to their children and themselves which they mistakenly designate as "food" and then scurry to the nearest prescription pad when the "side effects" of malnourishment come piling up.
So while I am pleased to see this article, I am not pleased that the same findings continue to be "news" when the news is that real, appropriate, healthful, non GMO, chemical free food cures and lack of that kind of food creates illness, both behavioral and organ based illness.
Are there other causes of illness? Sure. But the major killers (and economic producers for the illness care industry, cancer, cardiovascular disease and stroke, diabetes, obesity and obesity, are specifically identified as the "non communicable epidemic diseases of under nutrition by the World Health organization, WHO.
Ah, yes! Killer disease of under nutrition creating a vast and wildly profitable market for dangerous drugs which kill people in greater numbers than the drugs themselves do! Can't make safe, cheap, effective nutrients available, now can we? Be serious. Instead, let's get Codex Alimentarius up and going and make sure that the food produced under its "Voluntary" Standards and Guidelines are as health hostile, chemical and industry friendly (including its beloved Biotech Industry) get as much support as possible.
Codex, you will recall, is the product of the mad -but very clever - mind of Fritz ter Meer, a Bayer Drug Company Executive who become the head of IG Farben, the civilian organization that made the German's participation in the Second World War a near-success. He was also a convicted criminal following his trial at the Nuremberg War Tribunals for his success and enthusiastic participation in creating the German Death Machine.
After he, and the 26 other IG Farben executives (many of them drug company executives) got out of jail a scant less-than-4-years after they entered, ter Meer was hard at work as the head of Bayer Pharmaceutical once again. His creativity was focused this time not on the slogan above the front gate of the Auswitz death camp ("Arbeit Macht Frei", or, in English, "work brings freedom") but to the creation of the concept of Codex Alimentarius. Subsequent events show that the idea of creating contaminated, poisoned food, full of chemicals, GMO adulteration, irradiation by products (like free radicals and dead bacteria and their spilled-out insides in "cold sterilization" processes), hormones, antibiotics, etc., etc. was a wonderful business decision for the pharmaceutical industry. Health people, after all, are generally eating healthy food. Take the healthy food, and the supplements that enhance nutrition, away and you have sick people who got that way from eating sick food. In short, you have the US "Food" Supply (more than 80% GMO, by the way) as the primary feeder (!) sending people into the illness care system - where they stay, literally until they die.
If that is NOT what you want for your food, then get even more active than you are in letting everyone on your list know that you are a Natural Solutions Foundation Health Freedom Advocate and that you need them to be a Health Freedom Advocate, too. Here's how"
1. Join the free Natural Solutions Health Freedom eAlert (http://drrimatruthreports.com/index.php?page_id=187) distribution list and take every action step in the Newsletter, each time it comes to your email box. Then send it along to your email list and other contacts asking them to do the same. If you voice is not raised loud and clear, speaking truth to power, how will we protect your health and health freedom?
2. Donate to the Natural Solutions Foundation (http://drrimatruthreports.com/index.php?page_id=189). Your 100% tax deductible donations make it possible for the largest, most active and most effective health freedom organization in the world to protect your interests.
3. Change your buying habits so that you are ONLY purchasing GMO free foods. Look for labels that say “GMO-Free” or “Contains No GMOs” or “Organic”. Even though the outlay appears higher, how expensive is cancer? diabetes? heart disease? stroke? For organic supplements (not sourced from genetically modified plants, viruses and animals, free of pesticides and other dangerous contaminants, visit www.Organics4U.org. And for helpful guides click here (http://docs.google.com/fileview?id=F.40991bfe-ae98-4e5b-b5d6-25e09b923db9) for a short version and here (http://docs.google.com/fileview?id=F.a9a511b9-bfd2-4199-80ad-44f8818c8831) for a more detailed one.
4. If you are a lucky enough to be a coffee drinker (or detox person), or know people who are, we have a wonderful way to combine health freedom donation and the purchase of wholesome food! Coffee is the second most heavily chemically sprayed substance consumed by humans, running a close second to tobacco. So brewing coffee makes a water extract of God-Alone-Knows-What. Toxins too dangerous for use in US agriculture are made by US companies and sold in high volume in the coffee producing regions of the world where workers, often illiterate, spray huge quantities of deadly poisons on the theory that “more is better”. And you drink it.
Not any more! The Natural Solutions Foundation is now producing delicious, smooth and flavorful chemical free, Shade Grown, 100% Hard Bean Specialty Valley of the Moon(TM) Coffee (http://drrimatruthreports.com/?page_id=1130) as part of its Valley of the Moon Eco Demonstration Project (http://www.NaturalSolutionsFoundation.org) in the highlands of Panama. In appreciation of your $25 dollar donation, we’ll send you a bag of the best coffee you have ever had. Remember to give some to your friends, (http://drrimatruthreports.com/?page_id=1130) and you will see why we say Valley of the Moon(TM) Coffee is “A Little Bit of Heaven in a Cup(C)” What a delicious way to donate to the Natural Solutions Foundation!
Yours in health and freedom,
Dr. Rima
Rima E. Laibow, MD
Medical Director
Natural Solutions Foundation
www.HealthFreedomUSA.org
www.GlobalHealthFreedom.org
www.NaturalSolutionsFoundation.org
www.Organics4U.org
www.NaturalSolutionsMarketPlace.org
www.NaturalSolutionsMedia.tv
Nutritional and dietary influences on attention deficit hyperactivity disorder.
Sinn N.
Nutritional Physiology Research Centre, School of Health Sciences, University of South Australia, Adelaide, South Australia 5001, Australia. natalie.sinn@unisa.edu.au
The influence of children’s diet on their cognition and behavior.
Multivitamins and minerals help children’s brain function: study
By Stephen Daniells, 05-Nov-2008
Daily supplements of multivitamins and minerals may improve the brain function of children, says a new study from British and Australian researchers.
Twelve weeks of supplementation with vitamins and minerals was found to boost the attention scores of children, according to results published in the British Journal of Nutrition.
“This represents the first observation of acute behavioural effects of vitamins/minerals in human subjects,†wrote the researchers, led by Professor David Kennedy from Northumbria University in Newcastle.
“Naturally, these observations require replication in larger cohorts, but they do suggest that this matter should be given some priority,†cautioned the researchers.
Study details
The Newcastle-based researchers, in collaboration with scientists from Swinburne University in Australia, and the University of Westminster in London, recruited 81 children (average age 11) to participate in the randomised, double-blind, placebo-controlled, parallel groups investigation.
The children were reportedly all healthy and free from food allergy. In addition, none of the children used other dietary supplements during the three months prior to the study. Participants were randomly assigned to daily multivitamin and mineral supplements or placebo for 12 weeks. The study used Pharmaton SA’s Pharmaton Kiddi blend of multivitamins and minerals. The Swiss company also provided funding for the study.
Cognitive performance was measured using a battery of laboratory assessments. Measures were taken before the study, after one and three hours after the first dose, and after 12 weeks.
Kennedy and his co-workers report that the children in the vitamin/mineral group performed more accurately on two tests of attention. Indeed, the researchers noted the first signs of improvement only three hours after the first dose on the first day.
“The most surprising facet of the improvement in attention task performance seen here is that it became evident by three hours post-dose on the first day,†they wrote.
“To the best of our knowledge, the possibility that vitamins or minerals could exert behavioural effects after a single dose has not been explored,†they added.
However, no effects were observed on measures of the children’s mood, they added.
Science behind the claims?
The researchers noted that the study was aimed at testing the claims of the manufacturer that the multivitamin and mineral could improve the physical development and neural performance of the children.
“The combination of vitamins, minerals and amino acids present… in the present study does not allow the results presented to be attributed to any one component,†wrote the researchers.
“Further work in this area could examine the constituent parts of this treatment in more detail, perhaps focusing on attentional measures and including acute, as well as chronic, assessment,†they added.
Source: British Journal of Nutrition
November 2008, Volume 100, Pages 1086-1096, doi:10.1017/S0007114508959213
“Cognitive and mood effects in healthy children during 12 weeks’ supplementation with multi-vitamin/mineralsâ€
Authors: C.F. Haskell, A.B. Scholey, P.A. Jackson, J.M. Elliott, M.A. Defeyter, J. Greer, B.C. Robertson, T. Buchanan, B. Tiplady, D.O. Kennedy
http://www.nutraingredients-usa.com/Publications/Food-Beverage-Nutrition/NutraIngredients/Research/Multivitamins-and-minerals-help-children-s-brain-function-study