Showing posts with label disease. Show all posts
Showing posts with label disease. Show all posts

Tuesday, February 10, 2015

CONNECTING THE DOTS

Did Vaccines Cause My Daughter’s Cancer?


I read with great interest the recent ‘measles epidemic’ articles that addressed the vaccine debate from the point of view of a cancer parent. My interest is the result of being a cancer parent myself – my little girl has been battling leukemia on and off for the past 10 years. I read these articles, and I became angry. Very, very angry. Once again, the government and drug companies are exploiting the plight of children stricken by cancer to achieve a profit-driven end without actually helping them. In fact, this profitable end could cause great harm, even increasing the rates of pediatric leukemia, if their obvious goal of a federally mandated vaccination protocol is achieved. I am a seasoned Momcologist, a term the research-driven cancer parents call themselves.  We are the cancer equivalent of  Thinking Moms, critical thinkers. I have done extensive reading on the etiology of leukemia, its connection to autoimmune disease, and how vaccines and natural disease may influence these sorts of childhood illnesses. Come connect the dots with me.

Clearly, I empathize with the raw fear the parents in these articles have that their children may contract an illness that could be devastating to their immunocompromised children. I have walked for years in their shoes. I get it. However, the parents in these articles are either grossly misinformed, or their comments have been edited with bias. Let’s get some facts straight about cancer treatment and infection. One of the first things we were warned about after my daughter’s diagnosis was live-virus vaccination. No one in the family was to receive a live-virus vaccine while my daughter was on treatment because these viruses can and do shed (1, 2, 3, 4), some for as much as four weeks (5), potentially infecting the immunocompromised patient with disastrous results. That includes the measles vaccine  (MMR II and ProQuad), the intranasal flu vaccine, and the chicken pox shot. In fact, my other children were able to get medical waivers not to receive vaccines because of my daughter’s illness. I know my child is much more likely to encounter a peer at school who has been recently vaccinated with a live-virus vaccine than she is to encounter natural disease from an unvaccinated child.

If my child were at a stage of treatment in which she was very immunocompromised, she would not be in school. My daughter missed most of fourth grade and a good portion of fifth, not because she was so sick, but because others were sick. Despite a nearly 100% vaccine compliance rate at our school, there were regular outbreaks of shingles, occurring after chicken pox vaccine boosters, influenza and other illnesses. Please note that, even in areas in which vaccine compliance is extremely high, there are still outbreaks of disease that are not caused by the unvaccinated (6).

The most deadly threats for a child during intensive cancer treatment lie right within his or her own body. Immunocompromised pediatric cancer patients are far more likely to die from opportunistic infections that originate from overgrowths of fungi, mold and bacteria(7) than they are from vaccine-related viral infections.  When I searched to find the last recorded incidence of a child dying of measles (because that is the hated disease du jour) while undergoing cancer treatment, well, I couldn’t find one.  I did, however, find at least one death in the immunocompromised from the measles vaccine (8), with no indication of when it or they occurred. There hasn’t been a recorded death in the U.S. from measles in the past 10 years. (9) In fact, measles infection may actually be curative of some blood cancers (10, 11), presumably by initiating normal immune system defenses.  The measles virus as an actual treatment has also been explored in other malignancies (12, 13).

N0009927 Photomicrograph; acute lymphocytic leukaemia
There is evidence that the “hygiene theory” of the immune system may have some relevance to to vaccines. It has been found that more “hygienic” populations, i.e. kids who have had fewer exposures to everyday germs, are at higher risk for some illnesses. The idea being that the immune system needs to “learn” how to respond appropriately by coming in contact with common bugs in order to develop properly.  Industrialized countries that have a decrease in infectious burden over less developed nations nevertheless show an increase in allergies and autoimmune disease.  “The leading idea is that some infectious agents — notably those that co-evolved with us — are able to protect us against a large spectrum of immune-related disorders.” (14) Are we trading benign, transient illnesses that were once considered normal childhood rites of passage, illnesses that appear to be protective for more serious disease, for a lifetime of chronic illness, even death?

A discussion of the peculiarities of leukemia is in order, its relationship to the immune system, and the and the idea that vaccines can act as a possible trigger for the cancer itself. Leukemia begins with the development of immature white blood cells in the bone marrow, when one of these baby white blood cells mutates into an abnormal, leukemic cell. The more actively the body produces white blood cells (which are infection-fighting cells), therefore, the higher the risk of mutation. This is the explanation given for  increases in the incidence of leukemia after a flu virus passes through an area (15), and why children who exhibit hyper-stimulated immune responses in the form of asthma and eczema also have increased risk for leukemia (16). It may seem contradictory to discuss infection as a preventative for leukemia when applying the hygiene hypothesis, while also pointing to infection as a cause.  It’s apparently all about the maturity and status of the immune system.  “Timing is critical, as early infections are likely to positively modulate the immune system thereby reducing risk of leukemia, whereas later infections in children whose immune system was less well modulated may increase such risk.” (17)

Time to stop and connect more dots.  What are American children exposed to that deliberately hyper-stimulate the immune system? Vaccines. Our children are subjected to an incredibly aggressive vaccine schedule, the likes of which no other country sees, from the day they are born (and we have the highest first-day infant death rate of any first-world country, by the way) (18). Could we actually be triggering leukemia, the most common form of childhood cancer, with these vaccines? Particularly when we give them to children who already show signs of abnormal immune response?

Vaccines are not calibrated by weight or age or health-risk factors; potency levels of vaccines are standardized (19), which may cause hyper-stimulation for a child with a highly sensitive immune system.  Isn’t it interesting that less industrial countries have lower rates of autoimmune disease,  yet when those kids come to industrialized countries, in one generation they match our rates? (20) Could this possibly be related to the fact that these immigrants are required to submit to more aggressive vaccine schedules?

Acute lymphocytic leukemia is also less common in third-world countries, despite their children’s otherwise more debilitated state.  Children in industrialized nations experience a sharp rise in leukemia between two and six years of the age, the vaccine years, which does not occur in less developed nations. (21)

It is so very obvious that this potential connection requires exploration, yet the only studies to be found merely compare leukemia in more vaccinated to less vaccinated kids. The data from children who are completely unvaccinated is critical in uncovering the true reality of overall pediatric health.  We may very well find many interesting discoveries. Read this study from Germany (22), for example, which shows less acute and serious chronic illness overall for unvaccinated children, though they did not include childhood cancer. Why are we merely chasing a cure when a likely cause is sitting right under our noses?
Jean's daughter
Jean’s daughter

One word: Profit. As of 1988, vaccine makers and the doctors who administer vaccines bear no liability for vaccine injury (23). They cannot be held accountable by law for adverse events from vaccination. In fact, the entire adverse event reporting system (VAERS) is voluntary! This means that the more aggressive our vaccine schedule, the more profitable it is for vaccine makers. But what about the Centers for Disease Control, don’t they direct the vaccines our children really need? Please note that the CDC uses worldwide disease data to formulate our policies, which makes no sense at all. How could one possibly compare a malnourished child living in unsanitary conditions and subsequently exposed to illness to a child exposed to that same illness in a first-world country? I invite parents to take a look at the resumes of some of the heads of pharmaceutical companies and members of the CDC like this one (24). One can very clearly see those in charge of vaccine policy have a dangerous conflict of interest with those who profit from that policy. Remember, pharmaceutical companies contributed $34 million dollars in campaign funds in 2014  (25). It would behoove anyone attempting office these days to err on the side of ‘big pharma.’

I must add additional comment about parental trust in the government as it concerns our cancer kids.  Once parents recover from a cancer diagnosis, they have a strong desire to  help their children – to participate in activism in some way.  It is then they discover a disturbing reality about the state of pediatric cancer research and funding: In a united front, the major cancer fundraising organizations, our government, and the pharmaceutical industry ignore pediatric cancer. Why? First, kids don’t vote.  Second, kids don’t get cancer in rates high enough to warrant good profit returns. There has not been a novel drug developed for the treatment of acute lymphocytic leukemia, the most common childhood cancer, in 20 years (26). Oncologists are forced to use the same horridly harmful chemotherapy and radiation; the only variability in protocols is in the combinations, dosages and timing of the same archaic drugs. And while ‘cure’ rates have increased, childhood cancer incidence is still on the rise (27).  Over and over again, however, these organizations will exploit the pitiful stories and pictures of our kids to tug heartstrings and solicit funding.  The National Cancer Institute directs a pittance (4%) at pediatric cancer research versus other, more common and profitable, cancers (28).  When  will health research be directed by the needs of the people rather than the greed of corporations?
If any parent wants their child to be safe from preventable illness, it is a cancer parent. Yet I also stand with scores of cancer parents who have seen their children become stricken with leukemia shortly after vaccination.  My little girl?  She was diagnosed with leukemia shortly after her pediatrician “caught her up” on her shots almost 10 years ago.  That “catch up” schedule matches the regular schedule for a toddler today.  Unfortunately, it is nearly impossible to untangle true childhood cancer statistics or ‘cure’ (as in survival) rates (29).  The SEER database includes only five states and ten cities in the U.S., and one cannot readily backtrack to the time before the mad rush of vaccines. (30)

It is time to ask the hard questions for the sake of our children.  Are we actually causing leukemia and other childhood illnesses with these vaccines?  Could we even prevent leukemia by allowing natural disease?  The current measles “scare” is clearly a push for a federally mandated vaccine program.  Measles is highly contagious, yes, but benign (even potentially helpful) for the vast majority in a first-world country. If the current vaccine schedule could be harming our children, what will happen when pharmaceutical companies are given carte blanche?  Do we really want to relinquish our parental rights to a government that has shown itself to be both corrupt and callous in their treatment of our cancer kids?  What data is critical to either prove, or disprove, the hypothesis that vaccines can lead to increased chronic disease, particularly those related to the immune system like leukemia?  An independent study of the overall health of vaccinated versus unvaccinated children must be undertaken.  It is past time to finish connecting the dots to reveal the true picture of vaccines and childhood cancer.   Though it is too late for my vaccine-injured daughter, this Momcologist stands against vaccine mandates, for the health of future children.

~ Jean Ghantous
About the author:  Jean Ghantous is a wife and mother of three with a background in science, who formerly held a position with a pharmaceutical company as a research specialist. She has been a Momcologist for the past 10 years, since her daughter was diagnosed with high-risk pre-B cell acute lymphocytic leukemia as a toddler. After three years of treatment, the family enjoyed years of remission until her daughter was again diagnosed with a very late relapse at nine years old. She is currently in remission and doing well.
Jean’s penchant for research led to the important discovery that transfusional iron overload had been a long-overlooked high-risk factor for adverse late effects in cancer children. “Oncologists are so focused on treatment protocols that preventative care has been neglected, universally,” said Jean. “I realized within the first 10 minutes of researching iron overload that not only did my daughter have a very grave problem, but many kids, over many years, were at risk as well. I was horrified to read the list of side effects of iron toxicity; it was eerily similar to the late effects one is told to expect from chemotherapy.” Jean pushed for treatment and preventative care. She said “No one addressed iron overload because, well, no one had NOTICED it. For decades of cancer treatment.” This led to her hospital implementing a computerized tracking program for transfusional iron deposition and its involvement in a nationwide strategy for reducing risk from iron toxicity in children with cancer.
While Jean had always been suspicious that vaccines could play a role in the development of leukemia, she was told her daughter’s diagnosis after aggressive vaccination was “coincidence.” After her third child also sustained a vaccine injury, Jean took on the additional descriptor of Thinking Mom and became more actively involved in advocating for vaccine safety. “It is abundantly clear to any parent who takes the time to do the research that there is a very real causative connection between immune system disorders, chronic disease and vaccines,” warns Jean. “American kids are sick, really sick. EpiPens, inhalers, glucometers, special diets and special-needs teachers have become normalized in our schools. Four children in my neighborhood have been granted Make-A-Wish trips for life-threatening illness. One-third of my son’s class is in need of special-needs educational support. This is NOT normal. We MUST stop this insane, profit-driven push for federal vaccine mandates. Clearly, our families’ futures depend on it.”
References
1) “Detection of Measles Virus RNA in Urine Specimens from Vaccine Recipients,” http://www.ncbi.nlm.nih.gov/pmc/articles/PMC228449/
2) “ Vaccine Oka Varicella-Zoster Virus Genotypes Are Monomorphic in Single Vesicles and Polymorphic in Respiratory Tract Secretions,” http://jid.oxfordjournals.org/content/193/7/927.full
 3) MMR II vaccine insert:Excretion of small amounts of the live attenuated rubella virus from the nose or throat has occurred in the majority of susceptible individuals 7 to 28 days after vaccination.” http://www.merck.com/product/usa/pi_circulars/m/mmr_ii/mmr_ii_pi.pdf
4) “Chickenpox Attributable to a Vaccine Virus Contracted From a Vaccine With Zoster,” http://pediatrics.aappublications.org/content/106/2/e28.full
5) FluMist vaccine insert:FluMist contains live attenuated influenza viruses that must infect and replicate in cells lining the nasopharynx of the recipient to induce immunity. Vaccine viruses capable of infection and replication can be cultured from nasal secretions obtained from vaccine recipients (shedding).” Study showed shedding up to 28 days post vaccination: http://www.medimmune.com/docs/default-source/pdfs/flumist_pi.pdf
6) “Influenza Outbreak in a Vaccinated Population — USS Ardent, February 2014,” http://www.cdc.gov/mmwr/preview/mmwrhtml/mm6342a3.htm?mobile=nocontent
7) “Infections in the Neutropenic Patient— New Views of an Old Problem:,” http://asheducationbook.hematologylibrary.org/content/2001/1/113.full
8) MMR II vaccine insert: “Measles inclusion body encephalitis{44} (MIBE), pneumonitis{45} and death as a direct consequence of disseminated measles vaccine virus infection have been reported in immunocompromised individuals inadvertently vaccinated with measles-containing vaccine.” http://www.merck.com/product/usa/pi_circulars/m/mmr_ii/mmr_ii_pi.pdf
9) “There has been no measles deaths reported in the U.S. since 2003,” Dr. Anne Schuchat, the director of CDC’s National Center for Immunization and Respiratory Diseases. (Apparently, the veracity of this statement is in question, as CDC data for 2009 and 2010 both list two measles deaths, leading one to wonder why does the director of CDC’s National Center for Immunization and Respiratory Diseases not seem to know about them?  Don’t you think given the current hoopla about an outbreak with no associated deaths that they would be screaming about them?  Could it be that they were in immunocompromised people who got the disease either from the vaccine or from recently vaccinated people?)  http://vaccineimpact.com/2015/zero-u-s-measles-deaths-in-10-years-but-over-100-measles-vaccine-deaths-reported/
10) Bluming A, Ziegler J. “Regression of Burkitt’s lymphoma in association with measles infection.” The Lancet. 1971 Jul 10;:105–106.
11) “Remission of Disseminated Cancer after Systemic Oncolytic Virotherapy,” http://www.mayoclinicproceedings.org/article/S0025-6196(14)00332-2/fulltext
12) “Measles Virus for Cancer Therapy,” http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3926122/
13) Liu TC, Galanis E, Kirn D. “Clinical Trial Results with Oncolytic Virotherapy: A Century of Promise, a Decade of Progress.” Nat Clin Pract Oncol. 2007;4(2):101–117. http://www.ncbi.nlm.nih.gov/pubmed/17259931
14) Hygiene hypothesis: “In countries where good health standards do not exist, people are chronically infected by those various pathogens. In those countries, the prevalence of allergic diseases remains low. Interestingly, several countries that have eradicated those common infections see the emergence of allergic and autoimmune diseases.”
“The ‘Hygiene Hypothesis’ for Autoimmune and Allergic Diseases: An Update,” http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2841828/
15) “Childhood Leukemia Incidence in Britain, 1974–2000: Time Trends and Possible Relation to Influenza Epidemics,” http://jnci.oxfordjournals.org/content/98/6/417.full.pdf+html?sid=b366f430-37bb-49a4-b9b0-794149a1d2da
16) “Allergic Conditions and Risk of Hematological Malignancies in Adults: A Cohort Study,” http://www.biomedcentral.com/1471-2458/4/51
17) “Timing is critical, as early infections are likely to positively modulate the immune system thereby reducing risk of leukemia, whereas later infections in children whose immune system was less well modulated may increase such risk.”
“Infection and Pediatric Acute Lymphoblastic Leukemia,” http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2834409/
18) U.S. highest first-day infant mortality of industrialized nations: “6 Articles You Should Read about Infant Mortality in the U.S” http://america.aljazeera.com/watch/shows/fault-lines/FaultLinesBlog/2013/9/19/america-s-infantmortalitycrisisbackgroundreading.html
19) “Potency Tests of Combination Vaccines,” http://cid.oxfordjournals.org/content/33/Supplement_4/S362.full
20) “The ‘Hygiene Hypothesis’ for Autoimmune and Allergic Diseases: An Update,” http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2841828/
21) “An Infectious Aetiology for Childhood Acute Leukaemia: A Review of the Evidence.” http://www.ncbi.nlm.nih.gov/pubmed/15491284. Sharp peak in ALL diagnoses in developed countries between 2 and 6 years; early infection could be protective.
22) German study on the health of vaccinated versus unvaccinated children: http://healthimpactnews.com/2011/new-study-vaccinated-children-have-2-to-5-times-more-diseases-and-disorders-than-unvaccinated-children/
23) Vaccine Liability removed: http://www.nvic.org/NVIC-Vaccine-News/March-2011/No-Pharma-Liability–No-Vaccine-Mandates-.aspx#a1
24) Julie Gerberding: “Merck Announces Appointment of Dr. Julie Gerberding as Executive Vice President for Strategic Communications, Global Public Policy and Population Health,” http://www.mercknewsroom.com/news-release/corporatenews/merck-announces-appointment-dr-julie-gerberding-executive-vice-president
25) Pharmaceutical campaign contributions 2014: “Pharmaceuticals/Health Products: Long-Term Contribution Trends,” http://www.opensecrets.org/industries/totals.php?cycle=2014&ind=H04
26) “Little Patients, Losing Patience: Pediatric Cancer Drug Development,” http://mct.aacrjournals.org/content/5/8/1905.full
27) Childhood and Adolescent Cancer Statistics, 2014: http://acco.org/LinkClick.aspx?fileticket=gAi0ji8IFPU%3d&tabid=670
28) National Cancer Institute gives 4% to pediatric cancer research: http://acco.org/Information/AboutChildhoodCancer/ChildhoodCancerStatistics.aspx
29) “Because Statistics Don’t Tell the Whole Story: A Call for Comprehensive Care for Children With Cancer,” http://acco.org/LinClick.aspx?fileticket=9egsDtJw3fw%3d&tabid=670
30) SEER database: http://seer.cancer.gov/csr/1975_2011/results_merged/sect_29_childhood_cancer_iccc.pdf

SOURCE:  http://thinkingmomsrevolution.com/vaccines-cause-daughters-cancer/



Thursday, March 27, 2014

VACCINATED CHILDREN SPREAD DISEASE

"although individuals immunized with an acellular pertussis vaccine may be protected from disease, they may still become infected with the bacteria without always getting sick and are able to spread infection to others, including young infants who are susceptible to pertussis disease."

FDA study helps provide an understanding of rising rates of whooping cough and response to vaccination

FDA NEWS RELEASE 

For Immediate Release: Nov. 27, 2013
Media Inquiries: FDA- Jennifer Rodriguez, 301-796-8232, jennifer.rodriguez@fda.hhs.gov
NIH- Nalini Padmanabhan, 301-402-1663, padmanabhannm@niaid.nih.gov
Consumer Inquiries: 888-INFO-FDA,OCOD@fda.hhs.gov
FDA study helps provide an understanding of rising rates of whooping cough and response to vaccination
A new study is helping to provide a better understanding of vaccines for whooping cough, the common name for the disease pertussis. Based on an animal model, the study conducted by the U.S. Food and Drug Administration (FDA) and published November 25, 2013, in The Proceedings of the National Academy of Sciences, shows that acellular pertussis vaccines licensed by the FDA are effective in preventing the disease among those vaccinated, but suggests that they may not prevent infection from the bacteria that causes whooping cough in those vaccinated or its spread to other people, including those who may not be vaccinated.
Whooping cough rates in the United States have been increasing since the 1980s and reached a 50-year high in 2012. Whooping cough is a contagious respiratory disease caused by Bordetella pertussis bacteria. Initial symptoms include runny nose, sneezing, and a mild cough, which may seem like a typical cold. Usually, the cough slowly becomes more severe, and eventually the patient may experience bouts of rapid, violent coughing followed by the “whooping” sound that gives the disease its common name, when trying to take a breath. Whooping cough can cause serious and sometimes life-threatening complications, permanent disability, and even death, especially in infants and young children.
There are two types of pertussis vaccines, whole-cell and acellular. Whole-cell pertussis vaccines contain a whole-cell preparation, which means they contain killed, but complete, B. pertussis bacteria. The acellular pertussis vaccine is more purified and uses only selected portions of the pertussis bacteria to stimulate an immune response in an individual. In response to concerns about the side effects of the whole cell pertussis vaccine, acellular vaccines were developed and replaced the use of whole-cell pertussis vaccines in the U.S. and other countries in the 1990s; however, whole-cell pertussis vaccines are still used in many other countries.
“This study is critically important to understanding some of the reasons for the rising rates of pertussis and informing potential strategies to address this public health concern,” said Karen Midthun, M.D., director of the FDA’s Center for Biologics Evaluation and Research, where the study was conducted. “This research is a valuable contribution and brings us one step closer to understanding the problem. We are optimistic that more research on pertussis will lead to the identification of new and improved methods for preventing the disease.”
While the reasons for the increase in cases of whooping cough are not fully understood, multiple factors are likely involved, including diminished immunity from childhood pertussis vaccines, improved diagnostic testing, and increased reporting. With its own funds plus support from the National Institutes of Health (NIH), the FDA conducted the study to explore the possibility that acellular pertussis vaccines, while protecting against disease, might not prevent infection.
“There were 48,000 cases reported last year despite high rates of vaccination,” said Anthony S. Fauci, M.D., director of the NIH’s National Institute of Allergy and Infectious Diseases. “This resurgence suggests a need for research into the causes behind the increase in infections and improved ways to prevent the disease from spreading.”
The FDA conducted the study in baboons, an animal model that closely reproduces the way whooping cough affects people. The scientists vaccinated two groups of baboons – one group with a whole-cell pertussis vaccine and the other group with an acellular pertussis vaccine currently used in the U. S. The animals were vaccinated at ages two, four, and six months, simulating the infant immunization schedule. The results of the FDA study found that both types of vaccines generated robust antibody responses in the animals, and none of the vaccinated animals developed outward signs of pertussis disease after being exposed to B. pertussis. However, there were differences in other aspects of the immune response. Animals that received an acellular pertussis vaccine had the bacteria in their airways for up to six weeks and were able to spread the infection to unvaccinated animals. In contrast, animals that received whole-cell vaccine cleared the bacteria within three weeks.
This research suggests that although individuals immunized with an acellular pertussis vaccine may be protected from disease, they may still become infected with the bacteria without always getting sick and are able to spread infection to others, including young infants who are susceptible to pertussis disease.
For more information:

Pertussis infection in fully vaccinated children in day-care centers, Israel.

 http://www.ncbi.nlm.nih.gov/pubmed/10998384

 



Tuesday, January 29, 2013

TETANUS VACCINE

The vaccine junta is not only unconcerned with vaccine-induced diseases, it’s massively gearing up this vaccine arms race against the human race. It’s known that tetanus vaccine causes a new disease, antiphospholipid syndrome. New adjuvants are composed of phospholipids, a potential disaster.

Skull in Pupil, by Doug Wheller
Skull in Pupil, by Doug Wheller, Filter applied.
by Heidi Stevenson

The tetanus vaccine causes a new disease known both as Hughes syndrome and antiphospholipid syndrome (APS). It’s an autoimmune condition that can attack any part of the body, though is best noted for heart attacks and killing fetuses. It’s likely that APS will become more common with the new generation of vaccine adjuvants now being produced.

The sufferers of (APS) are mostly women, and its diagnosis is often made as a result of multiple pregnancy losses. As is typical of new diseases, research is focused on finding a genetic cause, in spite of the fact that the connection with vaccines is well known and documented.

As the name implies, APS is a condition in which phospholipids, natural and necessary substances required by every part of the body, is seen as an infectious agent by the immune system. So, this substance that exists in every cell becomes subject to attack. Symptoms include:
  • Blindness
  • Cardiovascular:
    • Deep vein thrombosis (clots in veins)
    • Phlebitis
    • Thrombocytopenia (deficiency of blood platelets, causing bleeding & bruising)
    • Atherosclerosis
    • Pulmonary embolus (clots in the lungs)
    • Heart valve abnormatilies
    • Stroke
  • Headaches & migraines
  • Miscarriages
  • Neurological disorders:
    • Epilepsy
    • Chorea (sudden uncontrollable jittery movements)
    • Transverse myelitis (inflammation of the spinal cord)
    • Multiple sclerosis
    • Cognitive dysfunction
  • Skin disorders, including mottling, ulcers, and necrosis
APS can also be diagnosed—more accurately, misdiagnosed—as lupus erythematosus, which is another vaccine-induced condition.

APS and Vaccines

One study calls Hughes syndrome the “classical antiphospholipid syndrome”[1]. That study refers to similarities between plasma protein beta-2-glycoprotein-I (β2GPI), which is attacked in APS, and the tetanus vaccine. That is, the tetanus antigen has parts that are virtually identical to β2GPI, which is found virtually everywhere in the body.

Another study documents how APS can be induced in laboratory animals with tetanus vaccination[2]. Many large number of other studies document and investigate the connection between vaccines and antiphospholipid syndrome[3,4,5,6,7,8].

These studies leave little doubt that APS is caused by vaccines. That should come as little surprise, since it was first identified as a disease during the 1980s. If this disease existed prior to vaccines, it was so rare that it was unknown. Now, it can take its place among a growing list of vaccine-induced conditions, including rheumatoid arthritis, macrophagic myofasciitis, multiple sclerosis, autism, and siliconosis. The list keeps growing and many believe that all these conditions should be included under a single name, autoimmune/inflammatory syndrome induced by adjuvants, or ASIA.

Why New Generation Vaccines Are Especially Worrisome

Phospholipids are a primary part of your body, forming part of the membrane of every cell, among other functions. They’re under attack in APS. As can be seen with regard to tetanus vaccine, APS can be induced by the antigen when the epitope—the part of the antigen forming the pattern that autobodies are designed to attack—is similar to a particular part of the body.

What’s frightening is that phospholipids are becoming a primary ingredient of vaccines in the form of a new generation of adjuvants made via recombinant DNA by diddling with a part of pathogenic bacteria called outer membrane vesicles (OMVs). You can read more about them in New Generation of Vaccine Adjuvants: Worst Ever?

OMVs allow for designer vaccine antigens and adjuvants. OMV adjuvants are, of course, being promoted as the safest ever developed. That safety claim is based on the fact that they’re so much like the body already. This is the same claim that’s been used to promote squalene, which, as we’ve recently seen with the tragic cases of narcolepsy in children after the squalene-laced flu vaccine, Pandemrix, was unleashed in Europe, can devastate lives. Gaia Health explained the issue in How the Flu Vaccine Causes Narcolepsy.

Squalene is a lipid. That’s what makes it so dangerous. OMVs are even more precisely analogous to human tissue, because they are not only lipids, they are phospholipids—which are precisely what the body attacks in APS. Therefore, we can anticipate that there will be ever-more cases of APS as we see the approval of ever-more OMV-based vaccines, which are in the pipeline now.
Have no doubt: these vaccines will be approved. The first one, Cervarix, is already out there—and it’s been deemed safe, in spite of evidence to the contrary.

People with APS are suffering from phospholipid antibodies that are erroneously destroying parts of the eye, cardiovascular system, brain, nerves, skin, reproductive system—in short, any part of the body. This self-destruction is induced by vaccine technologies. These technologies are presumed safe without adequate, if any, testing. Just how many people must suffer before this travesty is ended? When will the clearly mad purveyors of these technologies step back and question what they’re doing?

The fact is that there are not just one, but several generations of people who don’t even know what good health is. Worse, each successive generation is growing sicker than the previous one. And worst of all, the vaccine junta is not only unconcerned, it’s massively gearing up this vaccine arms race against the human race.

Sources:

  1. When APS (Hughes syndrome) met the autoimmune/inflammatory syndrome induced by adjuvants (ASIA)”Lupus, M Blank, E Israeli, Y Shoenfeld, doi: 10.1177/0961203312438115.
  2. Vaccine model of antiphospholipid syndrome induced by tetanus vaccineLupus, L Dimitrijević, I Živković, M  Stojanović, V Petrušić, S Živančević-Simonović, doi: 10.1177/0961203311429816.
  3. β2 glycoprotein 1 (β2GPI), the major target in anti phospholipid syndrome (APS), is a special human complement regulatorBlood, Katharina Gropp, Nadia Weber, Michael Reuter, Sven Micklisch, Isabell Kopka, Teresia Hallström and Christine Skerka, doi:10.1182/blood-2011-02-339564.
  4. Anti-β2 glycoprotein I (β2GPI) autoantibodies recognize an epitope on the first domain of β2GPIPNAS, G. Michael Iverson, Edward J. Victoria, and David M. Marquis.
  5. Anti-phospholipid antibodies following vaccination with recombinant hepatitis B vaccineClinical and Experimental Immunology, J Martinuč Porobič, T Avčin, B Božič, M Kuhar, S Čučnik, M Zupančič, K Prosenc, T Kveder, and B Rozman, doi:  10.1111/j.1365-2249.2005.02923.x
  6. Immunomodulatory and physical effects of phospholipid composition in vaccine adjuvant emulsions.
  7. ‘ASIA’ – autoimmune/inflammatory syndrome induced by adjuvants.
  8. Infections and vaccines in the etiology of antiphospholipid syndrome.
  9. Hughes Syndrome Foundation
  10. Antiphospholipid syndrome
  11. Learning About Antiphospholipid Syndrome (APS)
  12. The antiphospholipid syndrome (Hughes’ syndrome)
  13. APS Foundation of America
Vaccines cause autoimmune disorders!

SOURCE: GAIA HEALTH

Friday, January 25, 2013

FDA-Adverse Drug Reactions

Why Learn about Adverse Drug Reactions (ADR)?

"This is why we stress the point of dangers in the chemical prescription drugs being so highly recommended by the health care establishment.  We learn to late many times that the drugs we are given and those given to our loved ones are actually detrimental to the body's own healing ability.  This information comes from the FDA on their own website and as a caution to all those in the health care profession" ~Vickie Barker


Institute of Medicine, National Academy Press, 2000
Lazarou J et al. JAMA 1998;279(15):1200–1205
Gurwitz JH et al. Am J Med 2000;109(2):87–94

  • Over 2 MILLION serious ADRs yearly
  • 100,000 DEATHS yearly
  • ADRs 4th leading cause of death ahead of pulmonary disease, diabetes, AIDS, pneumonia, accidents and automobile deaths
  • Ambulatory patients ADR rate—unknown