By Catherine J. Frompovich

Time is running out to submit your comments to the CDC regarding the problematic MMR and MMRV vaccines given to infants and toddlers, which many think have an adverse impact on Autism.

I filed a 10-page comment, which is below, on December 14th. Guess how many comments were posted as of that date? A measly 236! The last time the CDC asked for comments, consumers posted over 15,000!

Earlier, I wrote an article about the CDC’s request for comments, which I heartily suggest you read and file your complaint. You can get some ideas from what I said in my filing, so please file your comment before midnight of Tuesday, December 19, 2016. Please don’t let an important opportunity slip by regarding vaccines that harm infants, toddlers and children.

Here’s the CDC website where you can file your complaint https://www.regulations.gov/docket?D=CDC-2016-0094, and thank you!

Proposed Revised Vaccine Information Materials for MMR (Measles, Mumps, and Rubella) and MMRV (Measles, Mumps, Rubella, and Varicella) Vaccines

>>Docket ID: CDC-2016-0094<<

Agency: Centers for Disease Control and Prevention (CDC)

Due Date: Dec. 19, 2016

Please accept the following information regarding MMR and MMRV vaccines, based upon published scientific research and studies, which I enumerate first, and follow with my comments that CDC requests regarding REVISED Vaccine Information Materials for MMR and MMRV Vaccines.

My comments are based upon studying published vaccine research since the 1980s and using the synopsis of 400 scientific papers in the 2016 book “Critical Vaccine Studies” by Neil Z. Miller.

Published Peer Review Studies

Med Sci Monit 2004 Mar; 10(3): P133-9.

A comparative evaluation of the effects of MMR immunization and mercury doses from thimerosal-containing childhood vaccines on the population prevalence of autism. Geier DA, Geier MR. “There is biological plausibility and epidemiological evidence showing a direct relationship between increasing doses of mercury from thimerosal-containing vaccines and neurodevelopmental disorders, and measles-containing vaccines and serious neurological disorders. It is recommended that thimerosal be removed from all vaccines, and additional research be undertaken to produce an MMR vaccine with an improved safety profile.”

Clin Infect Dis 2014 May; 58(9): 1205-10.

Outbreak of measles among persons with prior evidence of immunity, New York City, 2011. Rosen JB, Rota JS, et al. “This is the first report in which a person with a verified secondary vaccine failure despite receipt of two doses of MMR was demonstrated to be capable of transmitting disease to other individuals.”

J Infect Dis 2013 Mar 15; 207(6): 990-98.

Largest measles epidemic in North America in a decade—Quebec, Canada, 2011: contribution of susceptibility, serendipity, and superspreading events. DeSerres G, Markowski F, et al. “This outbreak raises important questions concerning the relative contributions of vaccine failure versus failure to vaccinate.”

J Biomed Sci 2002 Jul-Aug; 9(4): 359-64.

Abnormal measles-mumps-rubella antibodies and CNS autoimmunity in children with autism. Singh VK, Lin SX, et al. “Over 90% of MMR antibody-positive autistic sera were also positive for MBP autoantibodies, suggesting a strong association between MMR and central nervous system autoimmunity in autism. Stemming from this evidence, we suggest that an inappropriate antibody response to MMR, specifically the measles component thereof, might be related to pathogenesis of autism.”

J Public Health Epidemiol 2014 Sep; 6(9): 271-86.

Deisher TA, Doan NV, et al. “Rising autistic disorder prevalence is directly related to vaccines manufactured utilizing human fetal cells.” “The increasing number of vaccines made with human fetal cell lines is exposing infants and children to human DNA and retroviral contaminants that are associated with rising cases of autism.”[1]

Issues Law Med 2015 Spring; 30(1): 47-70.

Epidemiologic and molecular relationship between vaccine manufacture and autism spectrum disorder prevalence. Deisher TA, Doan NV, et al. “This study is one of the first laboratory and ecological studies conducted that has examined the relationship between human fetal cell line manufactured vaccines, cellular DNA damage, and the worldwide autism epidemic.” “Fetal DNA fragments in MMR and hepatitis A vaccines are significantly higher than the residual DNA limit established by FDA guidelines.” “Ecological data indicates a potential link between vaccines manufactured with human fetal DNA and the autism epidemic.”[2]

PLoS ONE 2011; 6(12): e27897.

Adverse events following 12 and 18 month vaccinations: a population-based, self-controlled case series analysis. Wilson K, Ducharme R, et al. “There are significantly elevated risks of primarily emergency-room visits approximately one to two weeks following 12 and 18-month vaccination.”

Vaccine 2014 Feb 26; 32(10): 1153-59.

Increased emergency room visits or hospital admissions in females after 12-month MMR vaccinations, but no difference after vaccinations given at a younger age. Wilson K, Hawken S, et al. “Our findings suggest that girls may have an increased reacto-genicity to the MMR vaccine.” This study analyzed 548,422 children’s health records. “For both males and females, the top reasons for ER visits and/or hospital admissions after their 12-month vaccinations were otitis media (ear infections/inflammation), acute upper respiratory tract infection, viral infection and non-infective gastroenteritis and colitis.”[3]

J Allergy Clin Immunol 2006 Jan; 1127(1): 59-66.

Allergic disease and sensitization in Steiner school children. Flὃistrup H, Swartz J, et al. “Children having received measles, mumps, and rubella vaccination showed an increased risk of rhinoconjunctivitis, whereas measles infection was associated with a lower risk of IgE-mediated eczema.”

JAMA 2004 Jul 21; 292(3): 351-57.

MMR vaccination and febrile seizures: evaluation of susceptible subgroups and long-term prognosis. Vestergaard M, Hviid A, et al. “The rate ratio of febrile seizures increased during the two weeks following MMR vaccination.” “Febrile seizures were nearly 3 times more likely to occur during the two weeks after MMR vaccination than at other times (incidence rate ratio, RR = 2.75).”[4]

Vaccine 2010 Jun 11; 28(26): 4308-11.

Use of the Australian Childhood Immunisation Register for vaccine safety data linkage. Gold M, Dougdale S, et al. “This study confirms the known association between MMR vaccination and febrile convulsions.”

Nat Genet 2014 Dec; 46(12): 1274-82.

Common variants associated with general and MMR vaccine-related febrile seizures. Feenstra B, Pasternak B, et al. “Febrile seizures represent a serious adverse event following measles, mumps and rubella (MMR) vaccination.”

Pediatrics 2010 Jul; 126(1): e1-8.

Measles-mumps-rubella-varicella combination vaccine and the risk of febrile seizures. Klein NP, Fireman B, et al. “Providers who recommended MMRV should communicate to parents that it increases the risk of fever and seizure over that already associated with measles-containing vaccines.” “More than 90% of the seizures were acute and 87% were febrile seizures.”[5]

Vaccine 2012 Nov 6; 30(48): 6731-33.

Febrile seizures and measles-mumps-rubella-varicella (MMRV) vaccine: what do primary care physicians think? O’Leary ST, Suh CA, et al. “After receiving data regarding febrile seizure risk after MMRV, few physicians report they would recommend MMRV to a healthy 12-15-month-old-child.”

CMAJ 2014 Aug 5; 186(11): 824-29.

Risk of febrile seizures after first dose of measles-mumps-rubella-varicella vaccine: a population-based cohort study. MacDonald SE, Dover DC, et al. “We observed a notable increase in seizure incidence in the 7-10 days after either vaccine combination, which fits with the biologically plausible period for febrile seizures after a measles-containing vaccine.” “This study compared the risk of seizures among 277,774 Canadian children 12-23 months of age who received the combination measles-mumps-rubella-varicella vaccine (MMRV) and those who received the MMR and varicella vaccines (MMR + V) separately on the same day.” [6]

Presentation at the 57th Annual Meeting of the German Society for Medical Computer Science, Biometry and Epidemiology (GMDS), September, 2012.

Epidemiological study on febrile convulsions after first dose MMRV vaccination compared to first dose MMR or MMR+V vaccination. Schink T, Holstiege J, Garbe E. “This study suggest a 2- to 4-fold increase in the risk of febrile convulsions in the interval 5 to 12 days after a first dose MMRV immunization compared to MMR immunization, and a 1.5 to 3.5-fold increase compared to MMR+V immunization.” “This study analyzed the health records of 270,824 German children to determine the risk of being hospitalized with a diagnosis of febrile convulsions after vaccination with MMRV compared to vaccination with MMR or MMR plus varicella given separately on the same day.” [7]

N Eng J Med 2001 Aug 30; 345(9): 656-61.

The risk of seizures after receipt of whole-cell pertussis or measles, mumps, and rubella vaccines. Barlow WF, Davis RL, et al. “There are significantly elevated risks of febrile seizures on the day of receipt of DTP vaccine and 8 to 14 days after the receipt of MMR vaccine.” “Data from the CDC-sponsored Vaccine Safety Datalink (VSD) was analyzed to determine the risk of seizures among 679,942 children after vaccinations with DTP and MMR.”[8]

J Pediatr Endocrinal Metab 2003 Apr-May; 16(4): 495-508.

Clustering of cases of type 1 diabetes mellitus occurring 2-4 years after vaccination is consistent with clustering after infections and progression to type 1 diabetes mellitus in autoantibody positive individuals. Classen JB, Classen DC. “The current findings indicate that there are clusters of cases of type 1 diabetes mellitus occurring 2-4 years post-immunization with the pertussis, MMR and BCG (tuberculosis) vaccines.”

Br J Clin Pharmacol 2003 Jan; 55(1): 107-11.

MMR vaccine and idiopathic thrombocytopaenic purpura. [A serious bleeding disorder] Black C, Kaye, JA, Jiek H.

“The risk of idiopathic thrombocytopaenic purpura (ITP) occurring within 6 weeks after vaccination with MMR is significantly increased.”

Arch Dis Child 2001 Mar; 84(3): 227-29.

Idiopathic thrombocytopenic purpura and MMR vaccine. Miller E, Waight P, et al. “Our study confirms a causal association between MMR vaccine and idiopathic thrombocytopenic purpura (ITP).”

Lupus 2014 May; 23(6): 554-67.

Immune thrombocytoppaenic purpura: an autoimmune cross-link between infections and vaccines. Rinaldi M, Perricone C, et al. “Vaccines such as MMR may prompt immune thrombocytopaenic purpura (ITP).” “ITP is 5 times more likely to occur after MMR vaccination (IRR = 5.48).”[9]

Hum Vaccin 2007 Mar-Apt; 3(2): 59-63.

Post-licensure safety of the meningococcal group C conjugate vaccine. Andrews N, Stowe J, et al. “There was evidence of an increased risk of convulsions and idiopathic thrombocytopenic purpura following MMR vaccination.”

Hum Vaccin Immunother 2013 May; 9(5): 1158-62.

Vaccine administration and the development of immune thrombocytopenic purpura in children. Cecinati V, Principi N, et al. “A number of reports have clearly demonstrated that all of the live, attenuated viruses in the MMR vaccine can cause ITP whether administered alone or in combination.”

Leukemia 1994 May; 8(5): 856-64.

Epidemiological characteristics of childhood acute lymphocytic leukemia. Analysis by immunophenotype. The Children’s Cancer Group. Buckley JD, Buckley CM. “Children who received MMR (measles, mumps, rubella) vaccination had a significantly elevated risk of acute lymphocytic leukemia (OR = 1.7).”[10]

Clin Microbiol Infect 2014 Jan; 20(1): 38-43.

Knowledge, attitudes, beliefs and practices of general practitioners towards measles and MMR vaccination in southern France in 2012. Pulcini C, Massin S, et al. “Many general practitioners shared the common misconception that measles is not a serious health threat, even though half of them had encountered measles.” “Eighty percent of GPs stated that most parents/patients consider measles a harmless disease.”[11]

PLoS One 2009 May 29; 4(5): e5738.

How many scientists fabricate and falsify research? A systematic review and meta-analysis of survey data. Fanelli D. “This is the first meta-analysis of surveys asking scientists about their experiences of misconduct. It found that, on average, about 2% of scientists admitted to have fabricated, falsified or modified data or results at least once and up to one third admitted a variety of other questionable research practices.” “In one survey, 81% of research trainees in the biomedical sciences were ‘willing to select, omit or fabricate data to win a grant or publish a paper’.”[12]

Nature 2005 June 9; 435: 737-38.

Scientists behaving badly. Martinson BC, Anderson MS, deVries R. “Our findings reveal a range of questionable practices that are striking in their breadth and prevalence. U.S. scientists engage in a range of behaviors extending far beyond fabrication, falsification or plagiarism that can damage the integrity of science.” “Overall, 33% of scientists funded by the NIH admitted that they engaged in questionable scientific behavior during the previous 3 years.” [13]

Psychother Psychosom 2009; 78: 1-5.

Preserving intellectual freedom in clinical medicine. “For a pharmaceutical company, delaying or minimizing knowledge of a side effect of a medication has cash value. Similarly, not publishing negative studies may shift the balance of subsequent meta-analyses.” “Pharmaceutical companies use the public relations industry to manipulate the interpretation of clinical trials with propaganda and to stifle dissent.”[14]

PLoS Med 2005 May; 2(5): e138.

Medical journals are an extension of the marketing arm of pharmaceutical companies. Smith R. “Journals have devolved into information laundering operations for the pharmaceutical industry.” “About 70% of clinical trials published in major journals are funded by the drug industry. Studies funded by the industry are 4 times more likely than studies funded from other sources to have findings favorable to the company.”[15]

Monash Bioethics Review 2007 Jan-Apr; 26(1-2): 24-45.

Detecting bias in biomedical research: looking at study design and published findings is not enough. Noble JH. “Today’s biomedical researchers live in an organizational world within which lying and cheating are rife.” “More than 65,000 product liability lawsuits have been filed against pharmaceutical drug manufacturers, which suggests [sic] that they and the FDA consider patient safety a low priority.”[16]

Account Res 2012; 19(2): 65-88.

Conflicts of interest in vaccine safety research. DeLong G. “Vaccine manufacturers have financial motives and public health officials have bureaucratic reasons that might lead them to sponsor research that concludes vaccines are safe.” “This paper summarizes conflicts of interest that pervade the vaccine industry and offers suggestions on possible remedies.”[17]

J Gen Intern Med 2004 Jan; 19(1): 51-56.

Relationship between conflicts of interest and research results. Friedman LS, Richter ED. “Conflict of interest is widespread among the authors of published manuscripts and these authors are more likely to present positive findings.”

PLoS Med 2005 Aug; 2(8): e124.

Why most published research findings are false. Ioannidis JP. “For most study designs and settings, it is more likely for a research claim to be false than true. Moreover, for many current scientific fields, claimed research findings may often be simply accurate measures of the prevailing bias.” “This paper demonstrates that most published research findings are false.”[18]

Sci Eng Ethics 2015; 21(1): 143-57.

On the Suppression of Vaccination Dissent. Martin B. “According to the highest ideals of science, ideas should be judged on their merits, and addressed through mustering evidence and logic. Suppression of dissent is a violation of these ideals.” “Anyone who questions the dominant views about vaccines is subject to abuse, including threats, formal complaints, censorship, and loss of their livelihood.”[19]

The first 25 peer-reviewed, published scientific articles discuss MMR and MMRV vaccines and adverse health findings associated with those vaccines, which the medical profession currently ignores and consequently refuses to advise parents and intended vaccinees of those risks as part of standard accepted medical ethics, i.e., “informed consent.”

Items 26 to 34 discuss the unfortunate criminal state of “consensus science” in research, specifically regarding fraud and vested-interest-biases. Much fraud and biases apply to vaccines, which the CDC and FDA ignore to the mounting detriment of human health, especially the ever-escalating autism and other neurodevelopmental disabilities of younger generations since the 1990s.

The vaccine industry’s consensus pseudoscience relative to human diploid cells (aborted fetal cell lines) and possible adverse homologous recombination; the use of recombinant and/or foreign DNA; plus numerous chemical ingredients being injected into infants and toddlers whose immune systems are not fully developed until around 2 years of age, truly is nothing short of “a flat earth theory” that was so prevalent in the Middle Ages, unless there’s a bio-diversifying agenda to restructure human physiology and promote transhumanism starting with infants, toddlers and teens.

MMR (MMR-II) Medium 199 (vitamins, amino acids, fetal bovine serum, sucrose, glutamate) , Minimum Essential Medium, phosphate, recombinant human albumin, neomycin, sorbitol, hydrolyzed gelatin, chick embryo cell culture, WI-38 human diploid lung fibroblasts MMRV (ProQuad) sucrose, hydrolyzed gelatin, sorbitol, monosodium L-glutamate, sodium phosphate dibasic, human albumin, sodium bicarbonate, potassium phosphate monobasic, potassium chloride, potassium phosphate dibasic, neomycin, bovine calf serum, chick embryo cell culture, WI-38 human diploid lung fibroblasts, MRC-5 cells

https://www.cdc.gov/VACCINEs/pubs/pinkbook/downloads/appendices/B/excipient-table-2.pdf

Comments for MMR and MMRV Vaccines Revised Information

First and foremost: CDC and FDA must restructure the childhood vaccination schedule for the MMR and MMRV vaccines to be administered only after 24 months or two years of age, based upon numerous studies documenting febrile seizures.

Also, the CDC and FDA should require all children to take an antibody titer test and a mitochondrial DNA test prior to receiving the MMR and MMRV vaccines in order to preclude brain and CNS adverse reactions to the problematic MMR and MMRV vaccines.

No. 1

All healthcare professionals who administer MMR and MMRV vaccines must verbally communicate, and also provide in writing, that MMR and MMRV vaccines are associated with a higher risk of seizures, both acute and febrile.

All printed, professional and media information must admit that for ten years the Mumps active efficacy rate in the MMR vaccine was fudged and falsified, as per a Merck & Company whistleblowers’ qui tam action lawsuit in Federal Court in Philadelphia, PA, which obviously skewed mumps demographics. Healthcare consumers have every right to know that important information as part of “informed consent,” which was denied consumers who took those vaccines thinking they were ‘protected’—but not—due to the deliberate Merck and Company fraud regarding the MMR vaccine.

Therefore, all printed, professional and media information must contain the following information:

Merck and Company “failed to disclose that its mumps vaccine was not as effective as Merck represented, (ii) used improper testing techniques, (iii) manipulated testing methodology, (iv) abandoned undesirable test results, (v) falsified test data, (vi) failed to adequately investigate and report the diminished efficacy of its mumps vaccine, (vii) falsely verified that each manufacturing lot of mumps vaccine would be as effective as identified in the labeling, (viii) falsely certified the accuracy of applications filed with the FDA, (ix) falsely certified compliance with the terms of the CDC purchase contract, (x) engaged in the fraud and concealment describe herein for the purpose of illegally monopolizing the U.S. market for mumps vaccine, (xi) mislabeled, misbranded, and falsely certified its mumps vaccine, and (xii) engaged in the other acts described herein to conceal the diminished efficacy of the vaccine the government was purchasing,” in order to meet the FDA’s 95% effective rate for the vaccine.”

http://philadelphia.legalexaminer.com/fda-prescription-drugs/massive-fraud-in-merck-mmr-vaccine-testing/

No. 2

All printed, professional and media information must admit that Merck and Company performed sham testing on the MMR vaccine in the 1990s in order to report a 95% or higher efficacy rate for that vaccine in order to maintain its FDA licensure and Merck and Company’s resulting monopoly market for its MMR vaccine.

No. 3

All printed, professional and media information must admit that Merck and Company added rabbit blood antibodies to the MMR vaccine, which increased the MMR vaccine efficacy rate to 100%, which was fraudulent and illegal.

No. 4

All printed, professional and media information must admit that the MMR vaccine in the 1990s had an efficacy rate of only 69% <https://www.ncbi.nlm.nih.gov/pubmed/15950329> and that the CDC/FDA misled the global medical profession and public health agencies regarding the MMR vaccine.

No. 5

All printed, professional and media information must inform consumers that the CDC and FDA do not perform science-based testing upon any vaccines, but only promote the vaccine maker’s testing and efficacy results, which could be biased, inaccurate and not based on factual scientific data, since the CDC’s own records prove collusion to deceive healthcare consumers regarding vaccines transpired:

No. 6

All printed, professional and media information must report that the MMR-II vaccine contains 2.90 ppb glyphosate, the prime active in the herbicide Roundup®, as documented by independent laboratory tests and Samsel Environmental and Public Health Services in a letter to U.S. Senator Jeanne Shaheen (D-NH) dated August 29, 2016.

https://www.activistpost.com/2016/09/another-vaccine-bombshell-glyphosate-think-monsantos-roundup-confirmed-in-most-vaccines.html

That important chemical/pharmacological fact must be made public knowledge in all information about the MMR-II vaccine as a matter of patient informed consent plus truth in advertising which negatively impacts CDC/FDA’s and Merck’s ‘safety’ claims. Glyphosate is a Group 2A carcinogen per the World Health Organization’s International Agency for Research on Cancer[20].

No. 7

All printed, professional and media information must contain the fact that as of a 2015 EPA study, 15 percent of children between the ages of 3 to 17 in the USA have neurodevelopmental disorders.

The CDC and FDA refuse to investigate whether neurotoxins in vaccines have a causal effect or etiology with the relatively new syndrome of neurodevelopmental disorders, e.g., ADD, ADHD, ASD, etc., plus ever-increasing chronic diseases, e.g., diabetes and cancers, in children’s health.

Thank you for considering my comments.

Respectfully submitted by

Catherine J Frompovich

Consumer Health Researcher/Writer/Author since the late 1970s

The above graphic is courtesy of and copied from Cypher’s comment made to my ActivistPost.com article published December 9, 2016.

Notes:

[1] Miller, Neil Z. Critical Vaccine Studies, 2016; New Atlantean Press: Pg. 145

[2] Ibid. Pg. 146

[3] Ibid. Pg. 148

[4] Ibid. Pg. 187

[5] Ibid. Pg. 189

[6] Ibid. Pg. 190

[7] Ibid. Pg. 191

[8] Ibid. Pg. 192

[9] Ibid. Pg. 207

[10] Ibid. Pg. 245

[11] Ibid. Pg. 287

[12] Ibid. Pg. 304

[13] Ibid. Pg. 305

[14] Ibid. Pg. 307

[15] Ibid. Pg. 308

[16] Ibid. Pg. 309

[17] Ibid. Pg. 310

[18] Ibid. Pg. 315

[19] Ibid. Pg. 317

[20] http://www.iarc.fr/en/media-centre/iarcnews/pdf/MonographVolume112.pdf accessed 12-14-16

Catherine J Frompovich (website) is a retired natural nutritionist who earned advanced degrees in Nutrition and Holistic Health Sciences, Certification in Orthomolecular Theory and Practice plus Paralegal Studies. Her work has been published in national and airline magazines since the early 1980s. Catherine authored numerous books on health issues along with co-authoring papers and monographs with physicians, nurses, and holistic healthcare professionals. She has been a consumer healthcare researcher 35 years and counting.

Catherine’s latest book, published October 4, 2013, is Vaccination Voodoo, What YOU Don’t Know About Vaccines, available on Amazon.com.

Her 2012 book A Cancer Answer, Holistic BREAST Cancer Management, A Guide to Effective & Non-Toxic Treatments, is available on Amazon.com and as a Kindle eBook.

Two of Catherine’s more recent books on Amazon.com are Our Chemical Lives And The Hijacking Of Our DNA, A Probe Into What’s Probably Making Us Sick (2009) and Lord, How Can I Make It Through Grieving My Loss, An Inspirational Guide Through the Grieving Process (2008)

Catherine’s NEW book: Eat To Beat Disease, Foods Medicinal Qualities ©2016 Catherine J Frompovich is now available

