Here is a 10 part video interview of Dr Andrew Wakefield by Dr Mercola. Dr Wakefield is the lead researcher who uncovered the link between vaccines and autism. He has published more that 100 research articles on the subject, but none the less has been attacked and vilified because the truth that he discovered threatens the profits of Big Pharma and the global diabolical elite. They are carrying out the evil plans of Sir Bertand Russell - using injections to produce brain injury in children as part of a down-breeding project that is well underway in most parts of the world.
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Showing posts with label contaminated vaccines. Show all posts
Showing posts with label contaminated vaccines. Show all posts
14 April 2010
07 April 2010
Seasonal Flu Vaccine Increased Swine Flu Risk by 68%!
Anybody who got the seasonal flu vaccine in 2009 increased their chances of getting the pandemic swine flu by a whopping 68% according to Canadian researchers! This, according to them, means next year you've got to double up and get both the seasonal flu shot and the pandemic swine flu.
This is how the data gets 'fudged' to increase income to the big drug and vaccine makers. Isn't it amazing how they never lose?
Oh, you know what?
They failed to mention that the seasonal flu vaccine doesn't work anyhow!
So, just in case you're confused here's what you have to do-
Get the seasonal flu vaccine even though it doesn't work, but since in will increase your chances of getting the swine flu by 68%, make sure you get that one too, that way the pharmaceuticals will earn maximum profits and their CEO's will get a bonus! Got it? Prove it by rolling up your sleeve.
Enjoy. Learn. Share.
Did 'Regular' Flu Shot Up Risks for H1N1 Flu?
Those who got seasonal vaccine were at higher risk, study found, but that shouldn't affect immunization next season
TUESDAY, April 6 (HealthDay News) The traditional seasonal flu vaccine may have increased the risk of infection with pandemic H1N1 swine flu, according to the results of four new studies by Canadian researchers.
dblclick('xxlA');
In one study, the researchers used an ongoing sentinel monitoring system to assess the frequency of prior vaccination with the seasonal flu vaccine in people diagnosed with H1N1 swine flu in 2009 compared to people without swine flu. The researchers found that seasonal flu vaccination was associated with a 68 percent increased risk of getting swine flu.
The other three studies included additional case-control investigations in Ontario and Quebec, as well as a transmission study in 47 Quebec households that were hit with swine flu. In these studies, the researchers found that seasonal flu vaccination was associated with a 1.4- to 5.0-times greater risk of having swine flu.
The studies, published April 6 in the online journal PLoS Medicine, don't show whether there is a true cause-and-effect relationship between seasonal flu vaccination and subsequent swine flu illness, or whether the association was possibly due to a common factor among the people in the study, said principal investigator Danuta Skowronski, of the British Columbia Center for Disease Control in Vancouver, and colleagues.
However, the findings may raise questions about the biological interactions between pre-existing and new pandemic influenza strains.
The researchers noted that the World Health Organization has recommended that protection against pandemic swine flu be included in future seasonal flu vaccines. This will provide direct protection against pandemic swine flu and eliminate any risk that may have been due to the 2009 seasonal vaccine, which did not include protection against swine flu.
Those who got seasonal vaccine were at higher risk, study found, but that shouldn't affect immunization next season
TUESDAY, April 6 (HealthDay News) The traditional seasonal flu vaccine may have increased the risk of infection with pandemic H1N1 swine flu, according to the results of four new studies by Canadian researchers.
dblclick('xxlA');
In one study, the researchers used an ongoing sentinel monitoring system to assess the frequency of prior vaccination with the seasonal flu vaccine in people diagnosed with H1N1 swine flu in 2009 compared to people without swine flu. The researchers found that seasonal flu vaccination was associated with a 68 percent increased risk of getting swine flu.
The other three studies included additional case-control investigations in Ontario and Quebec, as well as a transmission study in 47 Quebec households that were hit with swine flu. In these studies, the researchers found that seasonal flu vaccination was associated with a 1.4- to 5.0-times greater risk of having swine flu.
The studies, published April 6 in the online journal PLoS Medicine, don't show whether there is a true cause-and-effect relationship between seasonal flu vaccination and subsequent swine flu illness, or whether the association was possibly due to a common factor among the people in the study, said principal investigator Danuta Skowronski, of the British Columbia Center for Disease Control in Vancouver, and colleagues.
However, the findings may raise questions about the biological interactions between pre-existing and new pandemic influenza strains.
The researchers noted that the World Health Organization has recommended that protection against pandemic swine flu be included in future seasonal flu vaccines. This will provide direct protection against pandemic swine flu and eliminate any risk that may have been due to the 2009 seasonal vaccine, which did not include protection against swine flu.
16 March 2010
Vaccination Bribery
This story is from the UK, but you better believe the same thing could happen here at a mall near you. Teen age girls are the target for the dangerous yet ineffective vaccine Gardasil, the most expensive vaccine ever. How do you get them to roll up their sleeves to get the shot? You bribe them! You offer them the 'incentive' of a $70 gift certificate! This is immoral and unethical and it should be illegal. Forced Mass Medication is Wrong!!!
Enjoy. Learn. Share.
Government Bribes Teens to Get Vaccinated
Crooked campaign hits mall-loving teens Forget shady strangers and bags of candy... the biggest threat to our daughters and granddaughters comes from health officials armed with mall gift certificates. In one of the most irresponsible government programs I've ever heard of, clinics in Birmingham, England, are bribing teenage girls to get vaccinated. Believe it or not, they're offering girls up to $70 in "Love2Shop" mall vouchers in exchange for getting one of the most dangerous vaccines ever approved: Gardasil. They call this an incentive; I call it physical assault on a minor. They want a pat on the back; I want them pat down and tossed in jail. And if, as a parent, you don't like it... tough. In Jolly Old England, your daughter doesn't need your permission to get vaccinated... so you'll only find out when she comes home showing off her new earrings... or when you get a call from the emergency room after she suffers one of this dangerous drug's many side effects. I've been crusading against Gardasil from Day One. The media calls it a "cervical cancer vaccine," but don't be fooled by this fancy nickname. This vaccine doesn't protect against cervical cancer -- it protects against certain forms of HPV, an STD that can cause cervical cancer. It's far from 100 percent effective, and it's even farther from 100 percent safe. But do you expect these teenage girls to know that? Do you think they're going to go home and do the research before accepting their shopping bribe? Sadly, most of them have no clue that Gardasil has been linked to dozens of deaths and thousands of reactions ranging from anaphylactic shock and grand mal seizures to coma and paralysis. Some girls have come down with the incurable nerve disorder Guillian-Barre Syndrome after getting vaccinated, as I've warned before. And according to a stomach-turning report I found in the Daily Mail, officials in Britain are already talking about expanding the Birmingham mall scheme nationwide. If you think this won't happen here, you're only partly right. Health officials might not be bribing girls at shopping malls, but the approach they're taking could be far more devastating. Big Pharma is hard at work pressuring local officials across the country into making HPV vaccines a requirement for school. The worst part is that all of this hoopla is over something that's completely preventable. Vaccine or no vaccine, the only surefire 100 percent effective means of preventing HPV infection is abstinence. You can't spread a sexually transmitted virus without sex. It's as simple as that.
18 January 2010
Vaccines Alter the Genetic Structure of Human Beings
The following article may be hard reading for some, but it is actually worth it to go through it. It is a little bit technical, but the main points are clear. Vaccines may alter the genetic structure of a human being!
We are human because we have the genetic makeup of a human being. This is called the human genome. If through vaccines the human genome is altered, then is it still the human genome?
If a 'person' has an alteration in its genome is that 'person', strictly speaking, still human?
In other words, have our children been made into hybrid human beings?
Mixtures of monkeys, pigs, chickens, cows, goats, viruses, bacteria, etc.
The article shows that these genetic changes are passed from parents to their children,
making them permanent.
This is the major reason vaccines are dangerous and should be outlawed:
They change the human genome!
We assert out right to remain human!
Enjoy. Learn. Think. Share.
(Note on my related blog, Original Dialogue, just today I posted an article about human mutation experiments going on at Plum Island, NY. Check it out.
It's all related.)
Are Current Childhood Vaccine programs compromising the genetics
of present and future generations?
by
Harold E. Buttram
Introduction
Previously published parts of this “Vaccine Overview” series reviewed the steadily increasing patterns of physical and mental health problems which have taken place since the relatively innocent times of the 1930s, largely involving the “4-A Disorders” (i.e., Autism, ADHD, Asthma, Allergies), now afflicting roughly one third of America’s children.(1) They also reviewed the U.S. Congressional Hearings on Vaccine Safety (1999-December, 2004) which revealed gross deficiencies in vaccine safety testing by federal health bureaucracies (FDA, CDC, NIH, etc.), as defined by Evidence-Based Medicine (EBM) and Quality of Evidence Ratings (QER).(2,3)
Because of surveillance and reporting deficiencies, we have no means of proving adverse vaccine reactions when they do occur. Since the growing patterns of adverse childhood health patterns have run parallel with increasing numbers of vaccines being administered (now up to 32 inoculations before school), common sense would have us suspect a causal relationship.
From a conceptual standpoint it is inconceivable that these adverse childhood health trends are not accompanied by corresponding genetic compromise and hybridization, the sources of which would be large-scale vaccine contamination with retroviruses and their reverse transcriptase enzymes, capable of imprinting viral DNA into the genetics of our children.
Although the human immune system is of almost inconceivable complexity in its detailed functions, the basic principles are quite simple, which might be compared with a medieval castle with an outer mote, an outer wall with parapets, and an inner defense wall, all of which serve to protect the king (brain and nervous system) and queen (genetic system).
Following this model, the human immune system is divided into two major classes: Cellular Immunity, located in the mucous membranes of the gastrointestinal and respiratory tracts and their respective lymph nodes (outer defenses), and Humoral Immunity, with production of antigen-specific antibodies by plasma cells in the bone marrow (inner defenses). For eons of time the mucous membranes of the gastrointestinal and respiratory tracts have been the primary sites of infectious microbe entry into the body so that, of necessity, mucosal immunity has evolved as the primary defense system, with humoral immunity serving a secondary or backup role. As reviewed earlier, vaccines are reversing these roles, (4) attempting to substitute vaccine-induced humoral immunity for the far more efficient mucosal immunity, the latter in turn undergoing a process of “atrophy of disuse” as a result of this role-switching.
The present article addresses some of the known pathways whereby some viral vaccines may be implanting their genetic material into the DNA of our children, and of the possible consequences.
Grossly Overlooked Mutational Risks
Viral vaccines, composed of mainly genetic material, may pose as much, or even greater, potential risk for causing genetic hybridization than other forms of vaccines (i.e., live viral or attenuated vaccines). This warning is supported by a study reported in Viral Research, in which a nuclear polyhedrosis virus was sent through 24 serial passages of culture media resulting in both “genetic insertions into and deletions from the virus,” (5) suggesting a propensity of viruses to accept, carry, and transfer genetic material from host to host.
This research and consideration takes on more gravity when we consider the extent of foreign genetic contamination in current vaccines:
“Among the 32 vaccines in current use, 7 contain chick embryo fluid or protein, 3 contain cells from monkeys, 1 contains sheep’s red blood cells, 1 contains mouse serum, 1 contains material from guinea-pig embryos, and 4 have cells from human aborted fetal tissue.”(6)
Additional research shows that vaccines containing aluminum, the mercury-based preservative (Thimerosal), and formaldehyde, pose additional risks for prompting genetic mutations following intoxications.(6a-d)
As reviewed by Roberts in “The Dangerous Impurities of Vaccines:”
“In 1998 and 1999 scientists representing the World Health Organization (WHO) met with the senior vaccine regulatory scientists from the USA and UK at the National Institutes of Health (NIH) in Washington D.C. to discuss the safety of the manufacturing methods employed to produce vaccines. No journalists were present, but official transcripts were kept. What they record is that all the many experts that spoke expressed grave concern over the safety of the manufacturing process currently employed to make the licensed vaccines, such as MMR, flu, yellow fever, and polio. It was reported by leading experts that the vaccines could not be purified, were “primitive,” made on “crude materials,” and the manufacturers could not meet lowered government standards. WHO specialists reported the widespread and continuing presence in the MMR vaccine of chicken leucosis virus. Others spoke about the presence of foamy virus, many other viruses, toxins, foreign proteins, enzymes and possibly prions and oncogenes, (which, being of equal or smaller size than the desired viral vaccines, cannot be filtered out). Grave concerns were expressed about the levels of foreign residual DNA and RNA contaminating the vaccines. It was feared that this (contamination) could be causing cancers and autoimmune diseases.” (7, 8)
Immune Suppression as a Co-Factor in Mutagenesis
In addition to the proneness of viral vaccines to exchange and transfer genetic material from host to host, another danger is that viral vaccines are inherently immunosuppressive, as reflected in the fact that viral infections tend to lower white blood cell (WBC) counts in contrast to bacterial infections, which raise WBC counts. Furthermore, in the field of chemical toxicology it is universally recognized that combinations of toxins may bring exponential increases of toxicity; that is a combination of two chemicals may bring a 10-fold increase in toxicity, three chemicals 100-fold increases. (9, 10) This same principle almost certainly applies to the immunosuppressive effects of viral vaccines when administered in combination, as with the MMR vaccine, among which the measles vaccine is exceptionally immunosuppresive. (11-13)
Returning to the medieval castle model of the human immune system, it is probable that the powerful, immune-suppressant effects of viral vaccines, when given in combination, may paralyze first-line cellular (mucosal) immune defenses sufficiently to allow viral DNA-grafting to take place into the genetics of many infants.
Considering that these vaccines will also be carrying elements of foreign bovine (from gelatin), chicken, monkey, and human proteins, which will also be transplanted into infant genetics, it might not be far amiss to consider viruses as nature’s ultimate polluters, all the more insidious because the process remains unrecognized.
Retroviruses and Reverse Transcriptase
“A retrovirus is a virus that does not enter host cells with a DNA genome, but an RNA genome. The most common way the RNA genome is replicated is via the enzyme reverse transcriptase to make DNA out if its RNA genome. The DNA is then incorporated into the host’s genome by an integrase enzyme. The virus thereafter replicates as part of the host cell’s DNA. Retroviruses are enveloped viruses that belong to the viral family, Retroviridae.” (14)
“Reverse transcriptase, also known as RNA-dependent DNA polymerase, is an enzyme that transcribes single-stranded RNA into double-stranded DNA…Normal transcription involves synthesis of RNA from DNA; hence,
reverse transcription is the reverse of this.” (15)
It is not necessary to understand these technical terms to know their underlying meanings. As outlined in Dr. Sherri Tenpenny’s scholarly text, Fowl! Bird Flu: It’s Not What You Think:
“Because of the way reverse transcriptase works in living cells, it is possible that genetic material from chicken viruses (and other retroviruses) is being woven into human DNA, especially that of our children.” (16)
Known sources of retrovirus/reverse transcriptase contaminations include the avian leukosis virus subgroup E and endogenous avian virus in measles and mumps vaccines (17) the influenza vaccine, (18) the sources being traced back to cultures in fertilized chicken eggs.
M.G. Montinari and Immunogenetics
Dr. Montinari and colleagues are best known for investigating the relationship between postvaccine central nervous system (CNS) diseases and mutation of human leukocyte antigens, (HLA) which essentially strip the body’s brain and nerve tissues of their outer coating of myelin. (19) The HLA system is one which aids an individual’s immune system to differentiate that which is “self” from that which is “nonself.” Although the mechanisms are complex, it is a system which, during embryonic life, learns to recognize healthy or normal cells of the body as “self” so that these cells will remain unmolested by the search and destroy mechanisms of the immune system, leaving the immune system free to eliminate foreign invaders. Of special concern is the fact that the HLA system also carries an increased proneness to mutations, which may result in an impairment of self-recognition. This process may be the fundamental cause underlying autoimmune disorders, in which the immune system attacks the cells of its own body.
Montinari found that certain alleles of HLA (A3 and DR7) were more frequent in patients with postvaccine-induced illness, which implicates an immunogenetic basis for such illnesses. What caused much concern was that Montinari and other researchers implicated vaccine adjuvants (additives), such as mercury-containing Thimerosal, as causing genetic mutations by modifying the amino acids in presenting antigen proteins. (20-22)
Herpes Virus Integration with DNA Transferred from Parents to Babies
Based on a public release of 2-Sept-2008 from the University of Rochester Medical Center, new research has shown that some parents pass on the human herpes virus 6 (HHV6) to their children because it is integrated into the parental chromosomes. This is the first time a virus has been shown to become a part of the human DNA and then get passed to subsequent generations.
This unique form of congenital infection may be occurring in as many as 1 in 116 newborns according to the report. The long-term consequences for a child’s development and immune system are unknown. (23)
Since it is known that viral DNA can be engrafted into parental DNA and then passed on to subsequent generations, should we not be investigating today’s live virus vaccines from this standpoint and looking into the possible consequences?
Summary and Conclusions
As outlined above, there are several factors indicating a possibility that the soaring incidence of physical and mental illnesses among today’s children are causally related to current childhood vaccine programs. Primary among these is the large-scale contamination of the measles, mumps, and influenza vaccines with retroviruses capable of engrafting their genetics into the DNA of childhood recipients. This is rendered more likely because of the cavalier regard with which combinations of viral vaccines are now being administered, primarily involving the MMR vaccines, but conceivably also in combination with chicken pox and influenza vaccines in today’s vaccine schedules, in spite of the toxicology principle that combinations of toxins may bring exponential (10-fold or 100-fold) increases in toxicity.
With some of today’s routine viral vaccines known to be contaminated with retroviruses and administered under conditions likely to bring varying degrees of immune paralysis in the recipient, these are conditions under which genetic hybridization would appear to be likely or inevitable.
Admittedly, this is indirect evidence which does not constitute proof, but consider this: The steadily increasing patterns of physical and/or mental illnesses among American children show no signs of abating. Unless this issue is definitively addressed, at some future time the process will pass a point of no return socially and economically from the sheer numbers of incapacitated children.
America unquestionably has the scientific technology to work out the proof that is needed to mandate a reduction and modification of current vaccine programs. The question is whether or not we have the necessary insights and determination to do so.
References
1.Bock K. Stauth C. Healing the New Childhood Epidemics, Autism, ADHD, Asthma, Allergies. New York: Ballantine Books, 2007.
2.Donohoe M. Evidence-based medicine and Shaken Baby Syndrome. Part I: Literature Review, 1966-1998. American Journal of Forensic Medicine and Pathology, 2003; 24:239-242.
3.Guyatt GH, Haynes RB, Jaesche RZ, Cook DJ, Green L, Naylor CD, User’s guides to the medical literature, XXV. Evidence-based medicine: principles for applying the users’ guides to patient care. JAMA, 2008; 284(10): 290-6.
4.Buttram H. Current childhood vaccine programs: An overview with emphasis on the Measles-Mumps-Rubella (MMR) vaccine and of its compromising of the mucosal immune system, Medical Veritas, 2008; 5:1820-1827.
5.Kumar S, Miller IK. Effects of serial passage of Autographa californica nuclear polyhedrosis virus to cell culture. Virus Research, 1987; 7:335-49.
6.Rense.com’s List of Vaccine Ingredients; Vaccination Liberation Index; Co-factors in mutagenesis, see: http://www.springerlink.com/content/reaqqy3re1wy9xdu/. For aluminum in mutagenesis in plants, see: http://www.springerlink.com/content/reaqqy3re1wy9xdu/ For formaldehyde mutagenesis, see: http://www.sciencedirect.com/science?_ob=ArticleURL&_udi=B6T2C-3YTCCB5-H&_user=10&_rdoc=1&_fmt=&_orig=search&_sort=d&_docanchor=&view=c&_searchStrId=1136849680&_rerunOrigin=google&_acct=C000050221&_version=1&_urlVersion=0&_userid=10&md5=7af93b19de77aaf45fa7365c2f074bc8. For mercury mutagenesis, see: http://www3.interscience.wiley.com/journal/111091091/abstract?CRETRY=1&SRETRY=0
7.Roberts J. The dangerous impurities of vaccines. Medical Veritas, 2008; 5:1897-1905.
8.Available online at http://www.fda.gov/Cher/advisory/vrbp/vrbpmain.htm.
9.Schubert J, Riley EJ, Tyler SA. Combined effects in toxicology: A rapid systematic testing procedure: cadmium, mercury, and lead. Journal of Toxicology and Environmental Health, 1978; 4: 763-776.
10.Abou-Donia MB, Wilmarth KR, Ochme F, Jensen KF, and TI Kurt. Neurotoxicity resulting from coexposure to Pyridostigmine bromide, DEET, and Permithrin: Implications of Gulf War chemical exposures. Journal of Toxicology and Environmental Health, Part A, 1996; 48: 35-56.
11. Overfield T, Hammes IM, Depression of tuberculin reaction by viral (measles) vaccines. New England Journal of Medicine, 1964; 711:1294-1296.
12.Karp C, Wysocka M, Wakefield AJ, Mechanism of suppression of cell-mediated immunity by measles virus, Science, 1996; 273:228-231.
13.Kerdiles YM, Sellin Cl, Druelle J, Harvat B. Immunosuppression by measles virus: Role of viral proteins. Rev Medical Virology, 2006; 16:49-63.
14.Retrovirus – Wikipedia, the free encyclopedia, on the internet.
15.Reverse Transcriptase – the free encyclopedia, on the internet.
16.Tenpenny, Sherri J. Fowl! Bird Flu: It’s Not What You Think, NMA Media Press (Private Company) , 2006: 78.
17.Tsang SX, Switzer WM, Shanmugam V, Johnson JA, Goldsmith C, Wright A et al, Evidence of avian leucosis virus subgroup E and endogenous avian virus in measles and mumps vaccines derived from chicken cells: Investigation of transmission to vaccine recipients. Journal of Virology, 1999; 73: 5843-51.
18.Weiss R, RNA tumor viruses, RNA Tumor Viruses. New York: Cold Spring Harbor Laboratory Press, 1982. pp 1109 – 1203.
19.Montinari, M.G., Favoino, B., Roberto, A., Diagnostic role of immunogenetics in post-vaccine diseases of the CNS: preliminary results. Mediterranean Journal of Surgery and Medicine, 1996; 4(2):69-72.
20.Miglore, L., and Niere, M. Evaluation of twelve potential aneuploidogenic chemicals by the in vitro human lymphocyte micronucleus assay, Toxicity in Vitro, 1991; 5(4):325-336.
21.Miller, B.M. and Adler, I.D., Aneuploid induction on mouse spermatocyte mutogenesis, Mutogenesis, 1992; 7(1):69-76.
22.Shrana, I. Mitosis and numerical chromosome aberration analyses in human lymphocytes: 10 known or suspected spindle poisons. Mutation Research, 1993; 187:57-60.
23.Based on Public Internet release dated 2-Sept-2008, a report which was issued from the Rochester University Medical Center entitled, “Virus Weaves Itself into the DNA Transferred from Parents to Babies,” which can be accessed under this title.
of present and future generations?
by
Harold E. Buttram
Introduction
Previously published parts of this “Vaccine Overview” series reviewed the steadily increasing patterns of physical and mental health problems which have taken place since the relatively innocent times of the 1930s, largely involving the “4-A Disorders” (i.e., Autism, ADHD, Asthma, Allergies), now afflicting roughly one third of America’s children.(1) They also reviewed the U.S. Congressional Hearings on Vaccine Safety (1999-December, 2004) which revealed gross deficiencies in vaccine safety testing by federal health bureaucracies (FDA, CDC, NIH, etc.), as defined by Evidence-Based Medicine (EBM) and Quality of Evidence Ratings (QER).(2,3)
Because of surveillance and reporting deficiencies, we have no means of proving adverse vaccine reactions when they do occur. Since the growing patterns of adverse childhood health patterns have run parallel with increasing numbers of vaccines being administered (now up to 32 inoculations before school), common sense would have us suspect a causal relationship.
From a conceptual standpoint it is inconceivable that these adverse childhood health trends are not accompanied by corresponding genetic compromise and hybridization, the sources of which would be large-scale vaccine contamination with retroviruses and their reverse transcriptase enzymes, capable of imprinting viral DNA into the genetics of our children.
Although the human immune system is of almost inconceivable complexity in its detailed functions, the basic principles are quite simple, which might be compared with a medieval castle with an outer mote, an outer wall with parapets, and an inner defense wall, all of which serve to protect the king (brain and nervous system) and queen (genetic system).
Following this model, the human immune system is divided into two major classes: Cellular Immunity, located in the mucous membranes of the gastrointestinal and respiratory tracts and their respective lymph nodes (outer defenses), and Humoral Immunity, with production of antigen-specific antibodies by plasma cells in the bone marrow (inner defenses). For eons of time the mucous membranes of the gastrointestinal and respiratory tracts have been the primary sites of infectious microbe entry into the body so that, of necessity, mucosal immunity has evolved as the primary defense system, with humoral immunity serving a secondary or backup role. As reviewed earlier, vaccines are reversing these roles, (4) attempting to substitute vaccine-induced humoral immunity for the far more efficient mucosal immunity, the latter in turn undergoing a process of “atrophy of disuse” as a result of this role-switching.
The present article addresses some of the known pathways whereby some viral vaccines may be implanting their genetic material into the DNA of our children, and of the possible consequences.
Grossly Overlooked Mutational Risks
Viral vaccines, composed of mainly genetic material, may pose as much, or even greater, potential risk for causing genetic hybridization than other forms of vaccines (i.e., live viral or attenuated vaccines). This warning is supported by a study reported in Viral Research, in which a nuclear polyhedrosis virus was sent through 24 serial passages of culture media resulting in both “genetic insertions into and deletions from the virus,” (5) suggesting a propensity of viruses to accept, carry, and transfer genetic material from host to host.
This research and consideration takes on more gravity when we consider the extent of foreign genetic contamination in current vaccines:
“Among the 32 vaccines in current use, 7 contain chick embryo fluid or protein, 3 contain cells from monkeys, 1 contains sheep’s red blood cells, 1 contains mouse serum, 1 contains material from guinea-pig embryos, and 4 have cells from human aborted fetal tissue.”(6)
Additional research shows that vaccines containing aluminum, the mercury-based preservative (Thimerosal), and formaldehyde, pose additional risks for prompting genetic mutations following intoxications.(6a-d)
As reviewed by Roberts in “The Dangerous Impurities of Vaccines:”
“In 1998 and 1999 scientists representing the World Health Organization (WHO) met with the senior vaccine regulatory scientists from the USA and UK at the National Institutes of Health (NIH) in Washington D.C. to discuss the safety of the manufacturing methods employed to produce vaccines. No journalists were present, but official transcripts were kept. What they record is that all the many experts that spoke expressed grave concern over the safety of the manufacturing process currently employed to make the licensed vaccines, such as MMR, flu, yellow fever, and polio. It was reported by leading experts that the vaccines could not be purified, were “primitive,” made on “crude materials,” and the manufacturers could not meet lowered government standards. WHO specialists reported the widespread and continuing presence in the MMR vaccine of chicken leucosis virus. Others spoke about the presence of foamy virus, many other viruses, toxins, foreign proteins, enzymes and possibly prions and oncogenes, (which, being of equal or smaller size than the desired viral vaccines, cannot be filtered out). Grave concerns were expressed about the levels of foreign residual DNA and RNA contaminating the vaccines. It was feared that this (contamination) could be causing cancers and autoimmune diseases.” (7, 8)
Immune Suppression as a Co-Factor in Mutagenesis
In addition to the proneness of viral vaccines to exchange and transfer genetic material from host to host, another danger is that viral vaccines are inherently immunosuppressive, as reflected in the fact that viral infections tend to lower white blood cell (WBC) counts in contrast to bacterial infections, which raise WBC counts. Furthermore, in the field of chemical toxicology it is universally recognized that combinations of toxins may bring exponential increases of toxicity; that is a combination of two chemicals may bring a 10-fold increase in toxicity, three chemicals 100-fold increases. (9, 10) This same principle almost certainly applies to the immunosuppressive effects of viral vaccines when administered in combination, as with the MMR vaccine, among which the measles vaccine is exceptionally immunosuppresive. (11-13)
Returning to the medieval castle model of the human immune system, it is probable that the powerful, immune-suppressant effects of viral vaccines, when given in combination, may paralyze first-line cellular (mucosal) immune defenses sufficiently to allow viral DNA-grafting to take place into the genetics of many infants.
Considering that these vaccines will also be carrying elements of foreign bovine (from gelatin), chicken, monkey, and human proteins, which will also be transplanted into infant genetics, it might not be far amiss to consider viruses as nature’s ultimate polluters, all the more insidious because the process remains unrecognized.
Retroviruses and Reverse Transcriptase
“A retrovirus is a virus that does not enter host cells with a DNA genome, but an RNA genome. The most common way the RNA genome is replicated is via the enzyme reverse transcriptase to make DNA out if its RNA genome. The DNA is then incorporated into the host’s genome by an integrase enzyme. The virus thereafter replicates as part of the host cell’s DNA. Retroviruses are enveloped viruses that belong to the viral family, Retroviridae.” (14)
“Reverse transcriptase, also known as RNA-dependent DNA polymerase, is an enzyme that transcribes single-stranded RNA into double-stranded DNA…Normal transcription involves synthesis of RNA from DNA; hence,
reverse transcription is the reverse of this.” (15)
It is not necessary to understand these technical terms to know their underlying meanings. As outlined in Dr. Sherri Tenpenny’s scholarly text, Fowl! Bird Flu: It’s Not What You Think:
“Because of the way reverse transcriptase works in living cells, it is possible that genetic material from chicken viruses (and other retroviruses) is being woven into human DNA, especially that of our children.” (16)
Known sources of retrovirus/reverse transcriptase contaminations include the avian leukosis virus subgroup E and endogenous avian virus in measles and mumps vaccines (17) the influenza vaccine, (18) the sources being traced back to cultures in fertilized chicken eggs.
M.G. Montinari and Immunogenetics
Dr. Montinari and colleagues are best known for investigating the relationship between postvaccine central nervous system (CNS) diseases and mutation of human leukocyte antigens, (HLA) which essentially strip the body’s brain and nerve tissues of their outer coating of myelin. (19) The HLA system is one which aids an individual’s immune system to differentiate that which is “self” from that which is “nonself.” Although the mechanisms are complex, it is a system which, during embryonic life, learns to recognize healthy or normal cells of the body as “self” so that these cells will remain unmolested by the search and destroy mechanisms of the immune system, leaving the immune system free to eliminate foreign invaders. Of special concern is the fact that the HLA system also carries an increased proneness to mutations, which may result in an impairment of self-recognition. This process may be the fundamental cause underlying autoimmune disorders, in which the immune system attacks the cells of its own body.
Montinari found that certain alleles of HLA (A3 and DR7) were more frequent in patients with postvaccine-induced illness, which implicates an immunogenetic basis for such illnesses. What caused much concern was that Montinari and other researchers implicated vaccine adjuvants (additives), such as mercury-containing Thimerosal, as causing genetic mutations by modifying the amino acids in presenting antigen proteins. (20-22)
Herpes Virus Integration with DNA Transferred from Parents to Babies
Based on a public release of 2-Sept-2008 from the University of Rochester Medical Center, new research has shown that some parents pass on the human herpes virus 6 (HHV6) to their children because it is integrated into the parental chromosomes. This is the first time a virus has been shown to become a part of the human DNA and then get passed to subsequent generations.
This unique form of congenital infection may be occurring in as many as 1 in 116 newborns according to the report. The long-term consequences for a child’s development and immune system are unknown. (23)
Since it is known that viral DNA can be engrafted into parental DNA and then passed on to subsequent generations, should we not be investigating today’s live virus vaccines from this standpoint and looking into the possible consequences?
Summary and Conclusions
As outlined above, there are several factors indicating a possibility that the soaring incidence of physical and mental illnesses among today’s children are causally related to current childhood vaccine programs. Primary among these is the large-scale contamination of the measles, mumps, and influenza vaccines with retroviruses capable of engrafting their genetics into the DNA of childhood recipients. This is rendered more likely because of the cavalier regard with which combinations of viral vaccines are now being administered, primarily involving the MMR vaccines, but conceivably also in combination with chicken pox and influenza vaccines in today’s vaccine schedules, in spite of the toxicology principle that combinations of toxins may bring exponential (10-fold or 100-fold) increases in toxicity.
With some of today’s routine viral vaccines known to be contaminated with retroviruses and administered under conditions likely to bring varying degrees of immune paralysis in the recipient, these are conditions under which genetic hybridization would appear to be likely or inevitable.
Admittedly, this is indirect evidence which does not constitute proof, but consider this: The steadily increasing patterns of physical and/or mental illnesses among American children show no signs of abating. Unless this issue is definitively addressed, at some future time the process will pass a point of no return socially and economically from the sheer numbers of incapacitated children.
America unquestionably has the scientific technology to work out the proof that is needed to mandate a reduction and modification of current vaccine programs. The question is whether or not we have the necessary insights and determination to do so.
References
1.Bock K. Stauth C. Healing the New Childhood Epidemics, Autism, ADHD, Asthma, Allergies. New York: Ballantine Books, 2007.
2.Donohoe M. Evidence-based medicine and Shaken Baby Syndrome. Part I: Literature Review, 1966-1998. American Journal of Forensic Medicine and Pathology, 2003; 24:239-242.
3.Guyatt GH, Haynes RB, Jaesche RZ, Cook DJ, Green L, Naylor CD, User’s guides to the medical literature, XXV. Evidence-based medicine: principles for applying the users’ guides to patient care. JAMA, 2008; 284(10): 290-6.
4.Buttram H. Current childhood vaccine programs: An overview with emphasis on the Measles-Mumps-Rubella (MMR) vaccine and of its compromising of the mucosal immune system, Medical Veritas, 2008; 5:1820-1827.
5.Kumar S, Miller IK. Effects of serial passage of Autographa californica nuclear polyhedrosis virus to cell culture. Virus Research, 1987; 7:335-49.
6.Rense.com’s List of Vaccine Ingredients; Vaccination Liberation Index; Co-factors in mutagenesis, see: http://www.springerlink.com/content/reaqqy3re1wy9xdu/. For aluminum in mutagenesis in plants, see: http://www.springerlink.com/content/reaqqy3re1wy9xdu/ For formaldehyde mutagenesis, see: http://www.sciencedirect.com/science?_ob=ArticleURL&_udi=B6T2C-3YTCCB5-H&_user=10&_rdoc=1&_fmt=&_orig=search&_sort=d&_docanchor=&view=c&_searchStrId=1136849680&_rerunOrigin=google&_acct=C000050221&_version=1&_urlVersion=0&_userid=10&md5=7af93b19de77aaf45fa7365c2f074bc8. For mercury mutagenesis, see: http://www3.interscience.wiley.com/journal/111091091/abstract?CRETRY=1&SRETRY=0
7.Roberts J. The dangerous impurities of vaccines. Medical Veritas, 2008; 5:1897-1905.
8.Available online at http://www.fda.gov/Cher/advisory/vrbp/vrbpmain.htm.
9.Schubert J, Riley EJ, Tyler SA. Combined effects in toxicology: A rapid systematic testing procedure: cadmium, mercury, and lead. Journal of Toxicology and Environmental Health, 1978; 4: 763-776.
10.Abou-Donia MB, Wilmarth KR, Ochme F, Jensen KF, and TI Kurt. Neurotoxicity resulting from coexposure to Pyridostigmine bromide, DEET, and Permithrin: Implications of Gulf War chemical exposures. Journal of Toxicology and Environmental Health, Part A, 1996; 48: 35-56.
11. Overfield T, Hammes IM, Depression of tuberculin reaction by viral (measles) vaccines. New England Journal of Medicine, 1964; 711:1294-1296.
12.Karp C, Wysocka M, Wakefield AJ, Mechanism of suppression of cell-mediated immunity by measles virus, Science, 1996; 273:228-231.
13.Kerdiles YM, Sellin Cl, Druelle J, Harvat B. Immunosuppression by measles virus: Role of viral proteins. Rev Medical Virology, 2006; 16:49-63.
14.Retrovirus – Wikipedia, the free encyclopedia, on the internet.
15.Reverse Transcriptase – the free encyclopedia, on the internet.
16.Tenpenny, Sherri J. Fowl! Bird Flu: It’s Not What You Think, NMA Media Press (Private Company) , 2006: 78.
17.Tsang SX, Switzer WM, Shanmugam V, Johnson JA, Goldsmith C, Wright A et al, Evidence of avian leucosis virus subgroup E and endogenous avian virus in measles and mumps vaccines derived from chicken cells: Investigation of transmission to vaccine recipients. Journal of Virology, 1999; 73: 5843-51.
18.Weiss R, RNA tumor viruses, RNA Tumor Viruses. New York: Cold Spring Harbor Laboratory Press, 1982. pp 1109 – 1203.
19.Montinari, M.G., Favoino, B., Roberto, A., Diagnostic role of immunogenetics in post-vaccine diseases of the CNS: preliminary results. Mediterranean Journal of Surgery and Medicine, 1996; 4(2):69-72.
20.Miglore, L., and Niere, M. Evaluation of twelve potential aneuploidogenic chemicals by the in vitro human lymphocyte micronucleus assay, Toxicity in Vitro, 1991; 5(4):325-336.
21.Miller, B.M. and Adler, I.D., Aneuploid induction on mouse spermatocyte mutogenesis, Mutogenesis, 1992; 7(1):69-76.
22.Shrana, I. Mitosis and numerical chromosome aberration analyses in human lymphocytes: 10 known or suspected spindle poisons. Mutation Research, 1993; 187:57-60.
23.Based on Public Internet release dated 2-Sept-2008, a report which was issued from the Rochester University Medical Center entitled, “Virus Weaves Itself into the DNA Transferred from Parents to Babies,” which can be accessed under this title.
25 December 2009
53 Vaccine Shots by Age Six
Here is the latest from our medical researcher, Bro Kevin Muhammad. Here he goes into the government mandated vaccination schedule for our children. This is the challenge we are up against. In total there are 53 mandated vaccine shots by the age of 6, with more on the way! This is an outrage and obvious genocide that we must resist with all the might we can muster. What follows here is an excerpted portion. You can find the entire article at Bro Kevin's web site below.© 2009 KEVIN A. MUHAMMAD ALL RIGHTS RESERVED
HTTP://WWW.KAMUHAMMAD.NET
DECEMBER 25, 2009
In the Name of Allah, The Beneficent, The Merciful
This paper was co-authored with my twin brother, Julian K. Muhammad
. . . . .
DIVINE GUIDANCE AND ITS VALIDATION
In a lecture delivered on October 28, 2007, titled Black Youth in Peril, Part 1, the Honorable Louis
Farrakhan stated:
...A man by the name of Bertrand Russell advocated the use of vaccines to induce partial chemical
lobotomies and create a servile, zombie population. This is why, in America, there are soaring rates of
autism, and increasing amounts of vaccines being mandated for babies and young children...
These words became the foundation of the national anti-vaccination campaign launched in early 2008. The
initial goal of the campaign was and is to educate the citizenry about the dangers of vaccination. The second
goal is to ratify our own health policies regarding vaccination, under the leadership of the Honorable Louis
Farrakhan—policies that are in accord with the Will of the Creator. We should care nothing about what the
CDC, FDA and other government health agencies have to say. We have already heard from them, and their
ploys have only meant unnecessary suffering, debilitation and premature death for us and our children.
ANALYZING THE CDC’S NATIONAL IMMUNIZATION SCHEDULE
Just how many vaccines are mandated for babies and young children? Let us examine the CDC’s official
document, Recommended Immunization Schedule for Persons Aged 0 through 6 Years—United States
2009. Again, this document is released annually by the ACIP, in collaboration with the American Academy of
Pediatrics and the American Academy of Family Physicians. Most children in the U.S. receive vaccines from
the time they are born and throughout the rest of their lives. However, the lion’s share of vaccines are
administered during their most critical developmental years, which are between 0 and 6 years of age.
This is why this particular immunization schedule is extremely important, and should be an urgent matter
for all citizens. The following sections are divided according to the age of the child, detailing the kinds and
number of vaccines administered within each age category—according to the CDC’s immunization
schedule.
WHEN THE BABY IS 48 HOURS TO 1 MONTH OLD
The Hepatitis B vaccine is the first to be given, as previously stated. The vaccine is administered in a twodose
series. The first dose is given at birth, usually within 48 hours after the child is born. The second dose
is given when the baby is one month old. — number of vaccines administered: 2
What should a mother and father know about this vaccine? In addition to the “secretive” geneticallyengineered
microorganisms, the other ingredients in hepatitis B vaccines include: aluminium, mercury,
PAGE 8 FROM THE DESK
Part 1: Examining the CDC’s National Vaccination Schedule
formaldehyde, polysorbate 20, and MRC-5 cellular protein, a protein derived from the lung tissue of male
fetuses.
WHEN THE BABY IS 2 MONTHS OLD
At merely 2 months old, the infant begins a series of vaccinations, which consist of seven (7) different
vaccines. These vaccines are:
Rotavirus
Diphtheria, tetanus and acellular pertussis (DTaP)
Haemophilus influenzae type b (Hib)
Pneumococcal conjugate vaccine (PCV)
Inactivated poliovirus (IPV)
Three of these vaccines (diphtheria, tetanus and pertussis) are usually administered in the combination
shot, DTaP. The number of genetically-engineered microorganisms, metals, industrial chemicals and drugs
being injected into the infant at this tender and supple age of 2 months is enormous. — number of
vaccines administered: 7
WHEN THE BABY IS 4 MONTHS OLD
After being injected with seven different vaccines at 2 months old or 8 weeks old or 60 days old, the infant
returns two months later (4 months of age) to receive the second wave of toxic shots. Again, the vaccines
are:
Rotavirus vaccine
Diphtheria, tetanus and acellular pertussis (DTaP)
Haemophilus influenzae type b (Hib)
Pneumococcal conjugate vaccine (PCV)
Inactivated poliovirus (IPV)
— number of vaccines administered: 7
WARNING
Please be advised that every vaccine mentioned throughout this paper contains just as many
or more poisonous “secretive” genetically-engineered microorganisms and brain-damaging
chemicals.
WARNING
At this point, the 4-month old infant has received 16 vaccines, since its birth.
. . . . .
FROM THE DESK TOWARD OUR OWN HEALTH POLICY—CONCERNING VACCINATION - PAGE 9
WHEN THE BABY IS 6 MONTHS OLD
Two months later, at 6 months old, the infant receives another round of the same toxic vaccines that were
administered when she/he was 2 months and 4 months old, with the exception of the polio vaccine. The
third dose of polio vaccine is administered later in the immunization schedule. The vaccines administered
at the 6-month mark are:
Rotavirus vaccine
Diphtheria, tetanus and acellular pertussis (DTaP)
Haemophilus influenzae type b (Hib)
Pneumococcal conjugate vaccine (PCV)
— number of vaccines administered: 6
WHEN THE BABY IS 6 TO 18 MONTHS OLD
The infant receives the final dose of the Hepatitis B vaccine between ages 6 months and 18 months. The
pediatrician may recommend administering the Inactivated poliovirus (IPV) vaccine when the infant is 9
months old in order to reduce the number of shots given at age 6 months. — number of vaccines
administered: 2
WHEN THE BABY IS 6 TO 59 MONTHS OLD
The baby is given an annual influenza vaccine. In the initial administration of this vaccine, the baby usually
receives two (2) doses, spaced one month apart. In the following years, only one dose of the vaccine is
recommended. — number of vaccines: 2 +( 5 = 7)
WHEN THE BABY IS 12 TO 15 MONTHS OLD
The final doses of both the Hib and PCV vaccines are administered when the child is 12 months or older.
The first doses of measles, mumps, rubella and varicella (chickenpox) vaccines are also given at this time.
The measles, mumps, rubella are administered in one shot, called the MMR vaccine. To avoid giving all
four shots to the baby in one office visit, the pediatrician may give the MMR and varicella vaccines at 12
months, and the Hib and PCV vaccines at 15 months. The MMR and varicella vaccines may also be
combined into a single shot. Regardless how the injections are administered, the vaccines injected into the
baby are:
Haemophilus influenzae type b (Hib) - final dose of series
Pneumococcal conjugate vaccine (PCV) - final dose of series
WARNING
By the time the baby is a year old, it has received 24 vaccines.
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Part 1: Examining the CDC’s National Vaccination Schedule
Measles-mumps-rubella (MMR)
Chickenpox (varicella)
— number of vaccines administered: 6
WHEN THE BABY IS 12 TO 23 MONTHS OLD
The baby receives two doses of the Hepatitis A vaccine between ages 12 and 23 months. The shots are
administered, at least, six months apart. — number of vaccines administered: 2
Here, we must note that most diagnoses for neurological diseases, such as autism—the so-called mystery
disease—take place during this time. The physician or pediatrician fails to acknowledge that the 35
extremely toxic vaccines the child has, thus far, received is the cause of this life-long, neurological disease.
Many parents also fail to make the connection; therefore, they keep allowing their “autistic” child to be
vaccinated, adding insult to further injury. Again, the ignorance of parents and their fear to defy government
vaccination mandates are the greatest threats to their children.
WHEN THE BABY IS 15 TO 18 MONTHS OLD
Between the ages 15 and 18 months, the baby receives the fourth dose of diphtheria, tetanus and acellular
pertussis (DTaP) vaccine. In some cases, the fourth dose is given as early as age 12 months, but it must be
administered six months after the third dose. — number of vaccines administered: 3
WHEN THE BABY IS 2 TO 6 YEARS OLD
An additional dose of pneumococcal vaccine or hepatitis A vaccine or one dose of meningococcal vaccine is
recommended for children between the ages of 2 and 6 years, who are in so-called “high-risk groups.” This
basically means all children. Government health agencies push this vaccine on all children. — number of
vaccines administered: 3
WHEN THE BABY IS 4 TO 6 YEARS OLD
About the time the child starts kindergarten, he/she receives the final doses of the following vaccines:
Diphtheria, tetanus and acellular pertussis (DTaP)
Inactivated poliovirus (IPV)
Measles-mumps-rubella (MMR)
WARNING
By the time the baby is two years old, it has received 35 vaccines (includes 3 influenza
shots).
. . . . .
FROM THE DESK TOWARD OUR OWN HEALTH POLICY—CONCERNING VACCINATION - PAGE 11
Chickenpox (varicella)
The administration of these eight (8) vaccines, appears to be a major effort of drug companies and
government health agencies to ensure that the child has learning disabilities when entering school so that
he/she can begin receiving additional behavioral and neurological drugs—manufactured by the same drug
companies that make the vaccines.
Many state governments require proof that the child has received these vaccinations before allowing the
him/her to enter school. At this point, the parents whose children do not have their “shots” up-to-date for
reasons other than defiance against vaccination, rush to pediatricians to overload their children with the
missed vaccines. This is a sad state of affairs. — number of vaccines administered: 8
UNFATHOMABLE AMOUNT OF POISONS
Here, we must first note that few people have seen a person who has not been poisoned by vaccines.
Therefore, we can only assess the dangers of vaccines in the context of a world where most people succumb
to disease, mental degeneration, and death between the ages of 40 and 70 years, or 4 to 7 decades of life,
respectively. No one can deny that this is a very short lifespan. Unfortunately, it is the only frame of
reference we have. This makes it easy for parents to accept the extreme vaccination of their children.
Given this fact, it is in our best interest to examine the extreme toxicity of vaccines. The 53 vaccines that
children receive by the time they reach the age of 6 years saturate their bodies with “secretive” geneticallyengineered
microorganisms that come from different species of animals and insects; industrial chemicals;
other types of chemicals; various kinds of drugs; and neurotoxic metals.
For a list of the “ingredients” contained in the vaccines named in this document, please visit my website at
http://www.kamuhammad.net or obtain a copy of my book, The Case Against Hepatitis B Vaccination.
THE PATH OF OVERCOMING MEDICAL TYRANNY
The United States Declaration of Independence is the official document which delineated the justification of
the thirteen colonies that comprised the United States of America to break from the aristocratic oligarchy,
the King of Great Britain, in 1776. This document is more often cited by name than actually read by the
citizens of America. If it were read, we would discover that the conditions that led to this nation’s separation
from tyrannical dictatorship persist today. This document opens with the following statement:
When in the Course of human events, it becomes necessary for one people to dissolve the political
bands which have connected them with another, and to assume among the powers of the earth, the
WARNING
By the time the child is six years old, it has received 53 vaccines (includes 4 annual influenza
shots).
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Part 1: Examining the CDC’s National Vaccination Schedule
separate and equal station to which the Laws of Nature and of Nature's God entitle them, a decent
respect to the opinions of mankind requires that they should declare the causes which impel them to
the separation.
We hold these truths to be self-evident, that all men are created equal, that they are endowed by their
Creator with certain unalienable Rights, that among these are Life, Liberty and the pursuit of
Happiness. That to secure these rights, Governments are instituted among Men, deriving their just
Powers from the consent of the governed, — That whenever any Form of Government becomes
destructive of these ends, it is the Right of the People to alter or to abolish it, and to institute new
Government, laying its foundation on such principles and organizing its powers in such form, as to
them shall seem most likely to effect their Safety and Happiness...
A few statements later, it reads:
The history of the present King of Great Britain is a history of repeated injuries and usurpations, all
having in direct object the establishment of an absolute Tyranny over these States. To prove this, let
facts be submitted to a candid world.
These “facts” are often referred to as “The Crimes of the King.” It is a long and detailed list of abuses so
disrespectful of human life that one wonders if the King’s rule could have ever been called a government.
The first crime listed is as follows:
He has refused his Assent to Laws, the most wholesome and necessary for the public good.
Let us consider this in the context of all that we have learned regarding the mass drugging and vaccination
of our children, specifically the aim of those who use the power of “government” to do this.
LONG TRAIN OF ABUSES AND USURPATIONS
The following is a continuation from the second paragraph in the 1776 United States Declaration of
Independence:
...Prudence, indeed, will dictate that Governments long established should not be changed for light
and transient causes; and accordingly all experience hath shewn that mankind are more disposed to
suffer, while evils are sufferable than to right themselves by abolishing the forms to which they are
accustomed.
But when a long train of abuses and usurpations, pursuing invariably the same Object evinces a
design to reduce them under absolute Despotism, it is their right, it is their duty, to throw off such
Government, and to provide new Guards for their future security. — Such has been the patient
sufferance of these Colonies; and such is now the necessity which constrains them to alter their former
Systems of Government.
According to the above, it was quite known at that time that human beings are more apt to suffer under
evils that are “tolerable” than to stand up, on the basis of “right,” to abolish the systems through which
. . . . .
FROM THE DESK TOWARD OUR OWN HEALTH POLICY—CONCERNING VACCINATION - PAGE 13
such evils are borne and enacted. This has much to do with our awesome ability to adapt, which can work
for us or against us. These “sufferable evils” are those that are short of flagrant abuses and blatant murder,
yet the result is the same—the society becomes one of injustice, inequality, misery, and enslavement.
Today, these abuses are shrouded as “good” government, and they are gradually heaped on us, which
makes them tolerable. However, to endure these evils is worst than being outright slaughtered.
In the Holy Quran 2:191, it states:
...for tumult and oppression are worse than slaughter.
For a mother to endure the pain of carrying a child for nine months, only to witness the destruction of her
baby’s physical and mental capabilities and potential, under medical tyranny and for the benefit of the
aristocratic families who regard us as mere “cattle,” may be worse than slaughtering the child. To live with
fear and grief, having your human rights persistently violated, with no apparent recourse or redress, is like
not living at all. At some point, we must make a stand.
How long is the train of abuses and usurpations of federal and state governments? What is usurpation? It is
“the act of taking by force and as though with justification.” When it comes to governments, abuses are
usually justified through the enactment of laws. Is this not how vaccinations are pushed on the citizenry—
being justified by government officials, who frame laws that work for the benefit of the drug companies they
serve?
Indeed, the mass drugging of our children facilitated by federal and state governments is indicative of a
“long train of abuses and usurpations” by these governments. This has placed the citizenry “under
absolute Despotism”— tyranny and terrorism. The precedence for thwarting the gross and inhumane
tyranny is already established in the Holy Quran and Bible, and in the United States Declaration of
Independence.
We will continue with this subject in Part II of this series.
12 November 2009
04 November 2009
HIV Brought to US in Contaminated Vaccine
Merck Vaccine Chief Admits Guilt!
So, you see, there really is no mystery of how HIV was introduced into certain populations in the USA. Well, it's no different today. The hypodermic syringe is a bio-weapon delivery system to make sure the weapon reaches the intended target. In this case, it is always necessary to first do an 'artillary bombardment' of fear, disinflrmation, hysteria and government coersion to induce in the population an artificial 'demand' for the vaccine. You have to be psychologically manipulated into rolling up your sleeve.
So, pay attention to what is taking place in Ukraine. But do not expect that the whole picture will come into focus until it is too late. By looking at what happened in the past, we may have a chance to avoid the trap that is set for us today, by the enemy to us all.
Remember, Congress has 'vaccinated' Big Pharma by passing laws that make the pharmaceutical companies 'immune' to criminal responsibility. You can not sue them, no matter what they do. They are above the law and have a license to commit mass murder.
Apply the lessons of history to right now and act accordingly.
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