Posts Tagged flu

Child Diagnosed With Rare Disease After Flu Shot

By Chrissi Coile, KTBS 3 Health Reporter
Posted: Feb 10, 2010 8:28 PM
Updated: Feb 10, 2010 10:58 PM

A Shreveport girl is battling a rare disease.

In December 5 year old Hannah Pham started complaining her leg was numb. When her parents took her to the hospital doctors diagnosed her with Tranverse Myelitis. It’s a disease doctors say infects about 1 in a million people.

Experts say the disease is a neurological disorder which typically follows a virus.

Hannah got an swine flu shot in early December. The Pham family is worried that’s what caused the illness, but the CDC hasn’t reported any cases of Tranverse Myelitis following swine flu shots.
Hannah has been hospitalized for five weeks, meanwhile her family is praying for her recovery.

Employess at Spa Concepts where Hannah’s parents work are collecting donations and raffeling off spa treatments to help the family pay medical costs. They also set up an account at Capital One. If you would like to help out the account number is 573-240-4947.

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What To Do Before/After a Forced Vaccination

http://www.ktradionetwork.com/2009/11/17/what-to-do-beforeafter-a-forced-vaccination/

What To Do Before/After a Forced Vaccination

Here are just a few recommendations (sourced above) for what to do before and after a forced vaccination. These tips come directly from Dr. Leonard Coldwell, Fred Van Liew and Dr. Jeff McCombs.

Dr Leonard Coldwell

Listen to Dr Coldwell’s IBMS Stress Reduction and energizing CDs because healing and health can only happen in the state of relaxation and an abundance of energy. Remember the only cause of illness is lack of energy! Read the rest of this entry »

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“We Expect to Kill Some People With Every Mass Vaccination Campaign”

Read the Label.

Read the Label.

http://www.healthzone.ca/health/newsfeatures/swineflu/article/728601–batch-of-h1n1-vaccine-recalled-for-severe-reactions

A GSK spokesperson admitted, straight up, that they expect people to have severe reactions and some to die from every mass vaccination campaign. They expect it.

How does it feel to head to work every morning, fully knowing that what you do it going to kill someone, put people in wheel chairs and ruin lives? Does that make you feel good? It would make me physically sick. Read the rest of this entry »

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H1N1 Reaction: Product of Hype or Propaganda?

An H1N1 clinic in Ottawa gets the message across in this file photo from Nov. 13, 2009.

An H1N1 clinic in Ottawa gets the message across in this file photo from Nov. 13, 2009.

Link: http://www.healthzone.ca/health/newsfeatures/swineflu/article/728291–h1n1-reaction-product-of-hype-or-prudence

I’ve been pointing out for weeks now that the H1N1 mortality rates are far lower than the seasonal flu, yet everyone wanted to believe that they absolutely needed the vaccine. Congratulations – that attitude just lined the pockets of the pharma manufacturers while simultaneously toxifying your system without just cause.

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Public Health Reports 24 Cases of H1N1 Flu Shot Reaction

A Toronto Public Health Nurse loads syringes with H1N1 vaccine at Metro Hall, Nov. 18, 2009.

A Toronto Public Health Nurse loads syringes with H1N1 vaccine at Metro Hall, Nov. 18, 2009.

Link: http://www.healthzone.ca/health/newsfeatures/swineflu/article/730812–public-health-reports-24-cases-of-h1n1-flu-shot-reaction

Typical media – uses shocking headline to draw you into the article and then obfuscate the issue once you start reading. A man died after getting his flu shot and the only reason you’re hearing about it is because he was in his 80′s and they can wash it over by saying it’s not clear what killed him.

What about all the other stories about people who died after the flu? When it’s in the favor of the vaccine they say the flu killed them, straight up and no one asks the same question as above – what exactly killed them?

No, it’s just fear tactics to push the drug.

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Ingredients in Childhood Vaccines in Canada

http://vran.org/about-vaccines/vaccine-ingredients/active-ingredients/ingredients-childhood-vaccines-in-canada/

While health officials recommend an ever increasing quantity of vaccines for babies and young children, they are less than forthcoming with the ingredients list of vaccine additives and the potential for reactions. Today’s parents are concerned about the health impact of multiple vaccines & additives on their children’s health. Vaccine product monographs listing ingredients can be located in the CPS index (Compendium of Pharmaceuticals and Specialties) obtainable through any pharmacy in Canada. Some vaccine product monographs can be accessed on line at the manufacturers’ websites.

Starting at two months of age, most babies are injected with the following vaccines: Diphtheria, Tetanus, acellular Pertussis, Polio, Act-HIB (haemophilus influenza B), Hepatitis B, 7 valent Pneumococcal vaccine, Meningococcal C vaccine. Babies may be injected with as many as 8 vaccines concurrently. See the Canadian Immunization Guide (in English or French) for details of the vaccine schedule and number of doses given of each vaccine.

In the northern territories, babies are also routinely injected within hours of birth with BCG (tuberculosis vaccine) & hepatitis B vaccine. The province of New Brunswick vaccinates newborns with hepatitis B vaccine within hours of birth.

A two dose schedule of MMR (measles, mumps, rubella) vaccine is generally started at 12 months and given again at 18 months or 4-6 years. Varicella (chickenpox) vaccine is also injected at 12 months of age. Additionally, Influenza vaccine is now recommended for all children starting at 6 months of age. Babies and young children are injected with two doses of flu vaccine 30 days apart.

Health officials keep vaccine reaction reports under wraps. Unlike the U.S. where the VAERS (Vaccine Adverse Events Reporting System) is accessible on line and can be searched by anyone for vaccine reactions, Canadians do not have access to the vaccine reaction data base held by Health Canada. Only by filing an Access to Information request with the specific lot number of a vaccine, is it possible to obtain limited vaccine reaction information.

People should also know that the manufacturers do not disclose all the ingredients nor full details of the manufacturing process. Health Canada protects the “proprietary rights” of these companies and upholds their right to secrecy – something the greater Canadian public should be up in arms about. That parents are expected to submit their children for injection with multiple vaccines without first having full disclosure of all known ingredients is a disturbing statement on the control exerted by monopoly medicine and corporate and government allies.

Thimerosal (a preservative comprising 50% ethyl mercury) was phased out of early infant shots in Canada when polio vaccine was combined with DPT. Mercury is a potent neurotoxin. Apparently inactivated, injectable polio vaccine is degraded by thimerosal, hence vaccine combinations that contain polio vaccine do not contain thimerosal. Thimerosal may, however still be used in the manufacturing process, then filtered out. The question remains however, whether trace amounts of thimerosal still persist in the final product. Thimerosal was replaced by 2-phenoxyethanol, another toxic substance used in antifreeze and is contained in Pentacel, the DTPaP+Hib vaccine injected into most Canadian babies starting at 2 months of age.

Currently the two vaccines given to Canadian babies that may still contain thimerosal are influenza vaccine and hepatitis B. Both vaccines are available in single dose vials without thimerosal. Parents who choose to inject their babies with these vaccines should know they do have a choice to choose thimerosal free vaccines.

Your Baby’s First Shot – Five Vaccines in One:

Pentacel – combines Act-HIB and Quadracel vaccines(4 vaccines)

Produced by Sanofi Pasteur

Description:

Act-HIB ® Reconstituted with QUADRACEL ®Haemophilus b Conjugate Vaccine (Tetanus Protein – Conjugate) Reconstituted with Component Pertussis Vaccine and Diphtheria and Tetanus Toxoids Adsorbed Combined with Inactivated Poliomyelitis Vaccine.

Each single dose (approximately 0.5 mL) after reconstitution contains:

  • purified polyribose ribitol phosphate capsular
  • polysaccharide (PRP) of Haemophilus influenzae type b
  • covalently bound to 20 µg of tetanus protein 10 µg
  • pertussis toxoid (PT) 20 µg
  • filamentous haemaglutinin (FHA) 20 µg
  • fimbrial agglutinogens 2 + 3 (FIM) 5 µg
  • pertactin (PRN) 3 µg
  • diphtheria toxoid 15 Lf
  • tetanus toxoid 5 Lf
  • poliovirus type 1 (Mahoney) 40 D-antigen units
  • poliovirus type 2 (MEF1) 8 D-antigen units
  • poliovirus type 3 (Saukett) 32 D-antigen units
  • aluminum phosphate 1.5 mg
  • 2-phenoxyethanol (not as a preservative) 0.6% v/v
  • polysorbate 80 10 ppm (by calculation)
  • bovine serum ≤50 ng
  • trace amounts of formaldehyde
  • trace amounts of polymyxin B and neomycin may be present from the cell growth medium

For information on precautions and adverse events, see the manufacturer’s monograph.

Hepatitis B vaccines marketed in Canada are produced by Merck Frosst & GlaxoSmithKline

Recombivax HB

Produced by Merck Frosst

Description:

RECOMBIVAX HB ® [hepatitis B vaccine (recombinant)] is a non-infectious subunit viral vaccine consisting of surface antigen (HBsAg or Australia antigen) of hepatitis B virus produced in yeast cells. A portion of the hepatitis B virus gene, coding for HBsAg, is cloned into yeast and the vaccine for hepatitis B is produced from cultures of this recombinant yeast strain according to methods developed in the Merck Research Laboratories.

Two formulations are available:

  • 10 µg/1.0 mL formulation: each 1.0 mL dose contains 10 µg of hepatitis B surface antigen adsorbed onto approximately 0.5 mg of amorphous aluminum hydroxyphosphate;
  • 40 µg/1.0 mL formulation: each 1.0 mL dose contains 40 µg of hepatitis B surface antigen adsorbed onto approximately 0.5 mg of amorphous aluminum hydroxyphosphate;

Thimerosal (mercury derivative) 1:20,000 (50 µg/mL) has been added only to the preservative-containing formulations. All preparations have been treated with formaldehyde prior to adsorption onto amorphous aluminum hydroxyphosphate. The vaccine is of the adw subtype.

For information on precautions and adverse events, go to: manufacturer’s monograph.

ENGERIX ® -B

Produced by GlaxoSmithKline

Hepatitis B Vaccine (Recombinant)

Composition:

The vaccine is a slightly opaque, white, sterile suspension. A slow settling of the white aluminum hydroxide may occur during storage leaving a clear colourless supernatant liquid. Each 1 mL adolescent/adult dose of vaccine contains 20 µg of hepatitis B surface antigen adsorbed onto 0.5 mg of Al +++ as aluminum hydroxide. Each 0.5 mL pediatric dose contains 10 µg of hepatitis B surface antigen adsorbed onto 0.25 mg of Al +++ as aluminum hydroxide. Multi-dose presentations contain 5.0 mg of 2-phenoxyethanol per mL as preservative.

The ENGERIX ® -B formulation contains a trace amount of thimerosal (‹0.5 µg mercury in the 0.5 mL pediatric dose and ‹1.0 µg mercury in the 1.0 mL adolescent/adult dose) from the manufacturing.

For information on precautions and adverse events see the manufacturer’s monograph.

Prevnar – 7-valent conjugate pneumococcal vaccine

Produced by Wyeth Lederle

The manufacturer’s website does not allow consumers to view a product monograph. Ingredients list is taken from CPS 2004 edition, product monograph page 1587:

Prevnar is a sterile solution of saccharides of the capsular antigen of S.pneumoniae serotypes 4, 6B, 9V, 14, 18C, 19F and 23F and diphtheria CRM197 protein. Individual polysaccharides are prepared from purification of the culture broth of each serotype. The saccharides are directly conjugated to the protein carrier CRM197 protein by reductive animation. CRM197 is a nontoxic variant of diphtheria toxin isolated from cultures of C. diphtheriae strain C7(B197) and/or C.diphtheriae strain C7 (B197) pPx350 grown in a casamino acids and yeast extract-based medium. CRM197 is purified through ultrafiltration, ammonium sulfate precipitation, and iron-exchange chromatography to high purity. Each serotype is conjugated as a monovalent preparation prior to compounding as a multivalent vaccine. Individual glycoconjugates are analyzed for saccharide to protein ratios, for molecular size, free saccharide and free protein.

Each dose (0.5ml) contains:

  • 2ug of each saccharide for serotypes 4, 9V, 14, 18C, 19F and 23F,
  • and 4 ug of serotype 6B (16 ug total saccharides);
  • and approximately

  • 20ug of CRM197 carrier protein.

Nonmedicinal ingredients:

  • aluminum phosphate adjuvant
  • sodium chloride
  • and water for injection

For information on precautions and adverse reactions, see the CPS Index available at any pharmacy or medical library in Canada.

MENJUGATE® – Meningococcal Group C–CRM197 Conjugate Vaccine

Produced by Merck Frosst

Description:

Menjugate ® (Meningococcal Group C–CRM197 Conjugate Vaccine) is intended for the prevention of meningitis and/or septicemia caused by Neisseria meningitidis group C in infants and older age groups. Menjugate ® is composed of meningococcal group C oligosaccharides conjugated to a protein carrier, a non-toxic mutant of diphtheria toxin, CRM197. In the final vaccine, aluminum hydroxide is used as an adjuvant.

Composition:

Menjugate ® (Meningococcal Group C–CRM197 Conjugate Vaccine) is formulated as a powder for suspension with each 0.5 mL dose containing 10 micrograms of meningococcal C oligosaccharide conjugated to Corynebacterium diphtheriae CRM197 protein (12.5 to 25.0 micrograms).13 Mannitol, sodium phosphate monobasic monohydrate, and sodium phosphate dibasic heptahydrate are present as excipients in the final lyophilized formulation. The lyophilized product is to be reconstituted with an adjuvant diluent containing aluminum hydroxide (1.0 mg per 0.5 mL dose) and sodium chloride in sterile water for injection. Menjugate ® contains no preservative.

For information about precautions and adverse effects, see the manufacturer’s monograph.

M-M-R ® II Measles, Mumps and Rubella Virus Vaccine, Live, Attenuated, MSD Std.

Produced by Merck Frosst

Composition:

M-M-R ® II (Measles, Mumps and Rubella virus vaccine, live, attenuated, MSD Std.) is a sterile lyophilized preparation of (1) ATTENUVAX ® (Measles virus vaccine, live, attenuated, MSD Std.), a more attenuated line of measles virus, derived from Enders’ attenuated Edmonston strain and propagated in chick embryo cell culture; (2) MUMPSVAX ® (Mumps virus vaccine, live, attenuated, MSD Std.), the Jeryl Lynn ® (B level) strain of mumps virus propagated in chick embryo cell cultures; and (3) MERUVAX ® II (Rubella virus vaccine, live, attenuated, MSD Std.), the Wistar RA 27/3 strain of live attenuated rubella virus propagated in human diploid lung fibroblasts.

The reconstituted vaccine is for subcutaneous administration. When reconstituted as directed, the dose for injection is 0.5 mL and contains not less than the equivalent of 1,000 CCID50 (50% cell culture infective dose) of measles virus 5,000 CCID50 of mumps virus; and 1,000 CCID50 of rubella virus. Each dose of the vaccine is calculated to contain sorbitol (14.5 mg), sodium phosphate, sucrose (1.9 mg), sodium chloride, hydrolyzed gelatin (14.5 mg), human albumin (0.3 mg), fetal bovine serum (‹1 ppm), other buffer and media ingredients and approximately 25 µg of neomycin. The product contains no preservative.

The growth medium for measles and mumps is Medium 199 (a buffered salt solution containing vitamins and amino acids and supplemented with fetal bovine serum) containing SPGA (sucrose, phosphate, glutamate, and human albumin) as stabilizer and neomycin.

The growth medium for rubella is Minimum Essential Medium (MEM) (a buffered salt solution containing vitamins and amino acids and supplemented with fetal bovine serum) containing human serum albumin and neomycin. Sorbitol and hydrolyzed gelatin stabilizer are added to the individual virus harvests.

The cells, virus pools, fetal bovine serum, and human albumin are all screened for the absence of adventitious agents. Human albumin is processed using the Cohn cold ethanol fractionation procedure.

For information about precautions and adverse events, see the manufacturer’s monograph.

VARIVAX® III varicella virus vaccine, live, attenuated (Oka/Merck) is a live, attenuated virus vaccine (a lyophilized preparation of the Oka/Merck strain of varicella).

COMPOSITION- Active Ingredients:

VARIVAX ® III [varicella virus vaccine, live, attenuated (Oka/Merck)], when reconstituted as directed, is a sterile preparation for subcutaneous administration. Each 0.5 mL dose contains a minimum of 1350 PFU (plaque forming units) of Oka/Merck varicella virus when reconstituted and stored at room temperature for 30 minutes.

Non-Medicinal Ingredients:

Each 0.5 mL dose contains approximately 18 mg of sucrose, 8.9 mg hydrolyzed gelatin, 3.6 mg of urea, 2.3 mg sodium chloride, 0.36 mg monosodium L glutamate, 0.33 mg of sodium phosphate dibasic, 57 µg of potassium phosphate monobasic, 57 µg of potassium chloride. The product also contains residual components of MRC-5 cells including DNA and protein; and trace quantities of neomycin, and fetal bovine serum from MRC-5 culture media. The product contains no preservative.

For information about precautions and adverse events, ese the manufacturer’s monograph.

Influenza Vaccines

In Canada, Vaxigrip and Fluviral are the two vaccines most widely used and are produced by pharmaceutical companies Sanofi Pasteur and ID Biomedical respectively. Product information for Vaxigrip is available on the Sanofi Pasteur website. Fluviral product details are not available on the ID Biomedical website but are copied below from the CPS index – 2004 edition.

A recent meta analysis conducted by international researchers at the Cochrane Vaccines Field, looked at the results of 64 international flu vaccine studies. They concluded that there is no scientific ground on which influenza vaccines should be recommended for babies. Despite this, the Canadian Paediatric Society promotes flu shots for all children 6 months and older, including those with immune dysfunction and other chronic diseases. Infants and young children are injected with two doses of the vaccine 30 days apart. See article by Dr. F. Edward Yazbak, “Nothing New about Lack of Effectiveness of Influenza Vaccination in Babies“ (5. Notes)

VAXIGRIP® – Produced by Sanofi Pasteur

Inactivated Influenza Vaccine Trivalent Types A and B (Split Virion)

DESCRIPTION: – from CPS index, 2004 edition, page 2149

VAXIGRIP ® [Inactivated Influenza Vaccine Trivalent Types A and B (Split Virion)] for intramuscular use, is a sterile suspension prepared from influenza viruses propagated in chicken embryos. The virus-containing fluids are harvested and the virus inactivated with formaldehyde and purified by zonal centrifugation. The virus is then chemically disrupted using polyethylene glycol p-isooctylphenyl ether (Triton ® X-100) producing a “split-antigen”. The split antigen is suspended in sodium phosphate-buffered, isotonic sodium chloride solution. The type and amount of viral antigens contained in VAXIGRIP® conform to the current requirements of the World Health Organization (WHO).

And from the VAXIGRIP ® web page: [Inactivated Influenza Vaccine Trivalent Types A and B (Split Virion)] also contains Triton ® X-100 and trace amounts of sucrose and neomycin. Thimerosal (added as a preservative in multidose presentation only).

For information on precautions and adverse events, see the manufacturer’s monograph.

Fluviral S/F – Produced by

(previously Shire Bilogics)

Split-Virion Influenza Virus Vaccine, Inactivated

DESCRIPTION: – from CPS index – 2004 edition page 793

Fluviral S/F for i.m. injection is a trivalent, split-virion influenza vaccine prepared from virus grown in the allantoic cavity of embryonated hens’ eggs. The virus is inactivated with formaldehyde, purified by centrifugation and disrupted with sodium deoxycholate and/or polyethylene glycol p-isooctylphenyl ether (TritonX-100).

The composition of Fluviral S/F is established in agreement with the recommendations of the Canadian National Advisory Committee on Immunization (NACI). The split-virion vaccine contains 0.01% thimerosal as a preservative, and trace residual amounts of egg proteins, sodium deoxycholate and/or polyethylene glycol p-isooctylphenyl ether (Triton X-100). Antibiotics are not used in the manufacture of this vaccine.

The product monograph also contains the specific antigens designated for the 2003-04 influenza season.

Notes & Sources for more information:

  1. VRAN publishes a comprehensive 32 page newsletter 3X a year with reports on vaccine awareness issues from around the world & alternatives to vaccination. Please contact VRAN.
  2. Numerous other vaccines may be offered your children that are not listed above. These may include DPT vaccines such as Adacel recommended for teens and young adults, Hepatitis A vaccines, 4-valent meningococcal vaccines, and DT (diphtheria & tetanus) as single tetanus vaccine is no longer available in Canada. Product monographs for these vaccines can be found at the Sanofi Pasteur website and VaccineShoppeCanada, and Merck Frosst.
  3. Critical Decisions Count: Medical and Articles on Immunizations.
  4. VRAN Links to associated vaccine awareness websites around the world.
  5. Vaccination Not Mandatory in Canada – Health Canada Statement
  6. F. Edward Yazbak, MD, Nothing New about Lack of Effectiveness of Influenza Vaccination in Babies
  7. Meningitis C vaccine: A Look at the Disease & The Jab, by Dr. Jayne Donegan
  8. Additional articles on Meningitis C
  9. Prevnar: Articles & critiques http://www.whale.to/v/prevnar.htm

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Letter from a Parent to the Regional Health Department

Screenshot of the letter being written

Screenshot of the letter being written

My children come home from school with letters telling me to get them the swine flu vaccine, and that I should too.

These letters do not provide any facts or figures that can be backed up. It is always simple propaganda style instructions on what I should do.

I want to know WHY I should do this. Don’t point to the TV or newspaper reports that say I should. A mass media campaign only proves that the talking heads are all reading from the same scripts. We have all had the flu in the past and we all got over it. The seasonal flu complications are contributors to more than 30,000 deaths per year in North America, but this swine flu does not have those kinds of numbers and at this rate it will not by the time the flu season has passed.

This has been blown out of proportion and you are failing in your duties as a public servant. Your job is not to tell us what to do. You’re supposed to know both the pro and con arguments and present the populous with that information, ideally with references, so that we can make our own choices. To ignore the fundamental right we have, through the Canadian Constitution, to freedom of conscience is to violate it. A violation of one person’s rights is a violation of every person’s rights.

Perhaps there is more time being spent with consideration to the income generated for the medical and pharmaceutical industries than there is for the actual health of the people.

Before passing me off as an oddball or some other derogatory expression it would only reflect on your intelligence if you considered the following:

Child Being Vaccinated

Child Being Vaccinated

Doctors say the swine flu is a threat and vaccination is needed.
Doctors say the swine flu is NOT a threat and vaccination is worse than getting sick.

With those two points in mind people are likely to immediately fall back onto their pre-conceived notions about which could possibly be right or wrong. That mentality would do well with a small paradigm shift. Both groups of Doctors are smart, skilled and reputable so you cannot easily discount one over the other but what you can do is analyze the science they’re basing their statements on, and then from there you can make an informed choice that is free from fear and pre-conceived opinion and propaganda.

When the mass media pushes only one side of the story it is clear that there is an agenda at work. The mass media does not give the same air-time to Dr. Ron Paul, Dr. Len Horowitz, Dr. Joseph Mercola, Dr. Russell Blaylock, Dr. Sherri Tenpenny ect., as anyone working for a government agency or pharmaceutical company. ALL of these doctors are credible, intelligent and successful in their fields, but there is a glaring difference between them and the government/corporate reps: None of them seek gains of any kind by way of vaccination and/or drug prescriptions. Their goals are clearly defined and the most basic: Keep the good health of the people. If something is dangerous, don’t do it. If something is unproven, prove it. If something is untested, test it. If someone is not informed, inform them.

I discovered a poster created by Dr. Joseph Mercola on one of his websites, http://swineflu.mercola.com, and I paid out of my pocket to have 500 copies printed. I took 100 of them to the grocery store and my children passed them out to the shoppers by saying to them, “Hi, this will keep you healthy!” It generated lots of great conversation, and do you know what most people were saying to us?

“Wow, this is a great thing you’re doing here.”
“People are confused by the media. They don’t know what to do because no one is telling them the truth.”
“You’re really teaching your kids a great lesson here.”
“Oh my goodness I didn’t know any of this!”

We handed out about 80 of them and one lady asked for some so she could pass them around her social circles so we gladly gave her about 20 copies. Every single person who took a copy said, “Thank you.” I think they honestly appreciated the effort on our part to help people, and that became evident when after numerous people asked me if I worked for the government or hospital. I told them all, “No, I am just a concerned citizen.” When they heard that they let their guard down because I wasn’t pushing something on them. The poster we were giving out was a fact sheet that, after reading, would allow them the chance to verify the information and make an intelligent, informed decision about getting the shot… or not.

Screenshot of the submitted letter

Screenshot of the submitted letter

There were only 3 people who refused a copy of the poster, and one offered the fact that she already had her shot. The mass media does not show that kind of real, grass-roots level numbers.

When we got home the kids were so excited about giving people the chance to be healthy that they wanted to go door-to-door and give them to even more people. So we did. Not one person refused to take a poster and everyone was appreciative – even those out for an evening stroll and those walking their dogs.

Before bed the kids asked if they could take some posters to school to give to their friends. You see what’s happening here? People feel good about helping people. People feel good when someone else cares enough to offer them the help, even if they didn’t know any was needed.

We were not running around telling people what to do. We simply handed out some information that they could then use to “stay healthy.”

I hope you stay healthy too. Look up those Dr. names I listed. Visit their websites. Search for their videos/documentaries on YouTube. Be informed.

Swine Flu Posters for you to Download, Print and Share

Swine Flu Posters for you to Download, Print and Share

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The Goal of Every H1N1 Swine Flu Vaccine: Immunotoxicity, Neurotoxicity and Sterility

Prevent Disease
October 30, 2009

featured stories   The Goal of Every H1N1 Swine Flu Vaccine: Immunotoxicity, Neurotoxicity and Sterility
featured stories   The Goal of Every H1N1 Swine Flu Vaccine: Immunotoxicity, Neurotoxicity and Sterility
Vaccine ingredients have been scientifically proven to cause immunotoxicity, neurotoxicity, sterility and cancer.

Science dictates that only a randomized double-blind, placebo-controlled study can generate unbiased results in any clinical trial. In the history of vaccine development, no such study has ever been performed. It is only unscientific opinions and pharmaceutical propaganda which have propelled the mythological validity, safety and effectiveness of vaccines. Dozens of controlled studies have scientifically verified the immunotoxicty, neurotoxicity and sterility of common vaccine ingredients which destroy human health, yet they are all ignored by conventional medicine.

There should be a public outcry and challenge to every public health official, medical specialist or scientist (from any country) who justifies the inoculation of their population without providing the evidence of safety and effectiveness of the respective H1N1 vaccine in their country.

The public should be demanding that their governments materialize at least one vaccine trial which is randomized, double-blind and placebo-controlled that can scientifically validate the assertions of public health officials.

Since the pharmacokinetic properties of vaccines are not studied, vaccine manufacturers cannot deny any of the toxic effects listed below. The reason they never analyze the absorption, distribution, metabolism or excretion of these ingredients is because it would eradicate the vaccine industry. However the individual effects of each ingredient and their toxic effects on cells are well documented.

Every Physician, Nurse or medical personnel who administers the H1N1 vaccine (or any vaccine) should be asking themselves why they are injecting the following ingredients into patients that have been scientifically proven to cause immunotoxicity, neurotoxicity, sterility and cancer:

Novartis Focetria Adjuvanted H1N1

Influenza Vaccine Ingredients/Toxicity

Polysorbate 80: Sterilie Agent

Potassium Chloride: Neurotoxin

Squalene: Neurotoxin

Thimerosal: Neurotoxin

Novartis H1N1 Monovalent Influenza Vaccine Ingredients/Toxicity

Beta-Propiolactone: Carcinogen

Polymyxin: Neurotoxin

Neomycin: Immunotoxin

Thimerosal: Neurotoxin

GlaxoSmithKline Arepanrix Adjuvanted

H1N1 Influenza Vaccine Ingredients/Toxicity

Formaldehyde: Carcinogen

Polysorbate 80: Sterilie Agent

Sodium Deoxycholate: Immunotoxin

Squalene: Neurotoxin

Thimerosal: Neurotoxin

GlaxoSmithKline Pandemrix Adjuvanted

H1N1 Influenza Vaccine Ingredients/Toxicity

Octoxynol 10: Immunotoxin

Polysorbate 80: Sterilie Agent

Potassium Chloride: Neurotoxin

Sodium Deoxycholate: Immunotoxin

Squalene: Neurotoxin

Thimerosal: Neurotoxin

GlaxoSmithKline Fluarix 2009-2010

Formula Ingredients/Toxicity

Formaldehyde: Carcinogen

Octoxynol 10: Immunotoxin

Polysorbate 80: Sterilie Agent

Sodium Deoxycholate: Immunotoxin

Sanofi-Pasteur H1N1 Influenza Vaccine Ingredients/Toxicity

Formaldehyde: Carcinogen

Polyethylene Glycol: Systemic Toxin

Thimerosal: Neurotoxin

MedImmune H1N1 Vaccine Ingredients/Toxicity

Monosodium Glutamate: Neurotoxin

Gentamicin Sulfate: Nephrotoxin

Monobasic Potassium Phosphate: Immunotoxin

FLUARIX 2009 Latest Package Insert Ingredients/Toxicity

Formaldehyde: Carcinogen

Gentamicin Sulfate: Nephrotoxic

Polysorbate 80: Sterilie Agent

Sodium Deoxycholate: Immunotoxin

Thimerosal: Neurotoxin

CSL PANVAX H1N1 Vaccine Ingredients/Toxicity

Beta-Propiolactone: Carcinogen

Neomycin: Immunotoxin

Sodium Taurodeoxycholate: Carcinogen/Immunotoxin

Polymyxin: Neurotoxin

Thimerosal: Neurotoxin

CSL Afluria H1N1 Influenza Vaccine Ingredients/Toxicity

Beta-Propiolactone: Carcinogen

Neomycin Sulfate: Immunotoxin

Polymyxin B: Neurotoxin

Potassium Chloride: Neurotoxin

Sodium Taurodeoxycholate: Carcinogen/Immunotoxin

Thimerosal: Neurotoxin

Note: An additional CSL H1N1 Vaccine is Undergoing Trials with AS03 Adjuvant which contains Squalene.

Adverse Reactions of Vaccines

Serious adverse reactions are as follows:

* Pain

* Redness

* Swelling

* Fatigue

* Headaches

* Arthralgia (joint inflammation)

* Myalgia (muscle inflammation)

* Shivering

* Sweating

* Swollen lymph nodes

* Fever

* Vomiting

* Tingling or numbness of the hands or feet

* Shortness of breath

* Vasculitis (inflammation of the blood vessels)

Serious adverse reactions are as follows:

* Blood and lymphatic system disorders (lymphadenopathy)

* Psychiatric disorders (insomnia)

* Nervous system disorders (dizziness, paraesthesia, inflammation of the central nervous system, inflammation of nerves, autoimmune disorders affecting myelin sheaths of nerves such as Guillain-Barré Syndrome)

* Ear and labyrinth disorders (vertigo)

* Respiratory, thoracic and mediastinal disorders (dyspnoea)

* Gastrointestinal disorders (nausea, diarrhea, abdominal pain, vomiting, dyspepsia, stomach discomfort)

* Skin and subcutaneous tissue disorders (pruritus, rash)

* Musculoskeletal and connective tissue disorders (back pain, musculoskeletal stiffness, neck pain, muscle spasms, pain in extremity)

* General disorders and administration site conditions (bruising, asthenia, chest pain, malaise)

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