Watch my good friend, @r_hirschman, share his testimony on how he’s finding rubber-like clots. These are not post-mortem clots and have never been seen before the roll-out of the experimental vaccine.

Prior to contemporary vaccination programs, 'Crib death' was so infrequent that it was not mentioned in infant mortality statistics. For the first time in history, most US infants were required to receive several doses of DPT, polio, measles, mumps, and rubella vaccines. Shortly thereafter, in 1969, medical certifiers presented a new medical term-sudden infant death syndrome. In 1973, the National Center for Health Statistics added a new cause-of-death category--for SIDS--to the ICD. SIDS is defined as the sudden and unexpected death of an infant which remains unexplained after a thorough investigation.

"The RT-PCR test being used for
COVID involves a cycling function.
The more you cycle the test material in the lab, the more people test positive for COVID. If you cycle the test material 60 times, every sample tests positive for COVID. If you cycle it 10 times, no one tests positive. If you cycle it 30 times, some test positive and some don't. This means all our corrupt goverments have full control of how many people test positive, depending on how many times they insist the test material be cycled. They've picked this test
purposely so they can
up-regulate or down-regulate the
pandemic at will..."
Jason Christoff

Give a Listen!

https://podcasts.apple.com/us/podcast/dr-tappers-podcast/id1756757592

Episode 5 is out!
https://podcasts.apple.com/us/podcast/dr-tappers-podcast/id1756757592

This Thursday, I will be interviewing David Daleiden, who was exposing Planned Parenthood on felony charges for selling aborted fetal parts. Kamala Harris dismissed the charges against Planned Parenthood and fined David millions of dollars for bringing the truth to the people. Ever ask yourself who’s buying???
Ever wonder why I’m so adamantly against vaccines? Because the abortion industry and the vaccine industry are one and the same.

“Today, more than 23 vaccines are contaminated by the use of aborted fetal cells. There is no law that requires that consumers be informed that some vaccines are made using aborted fetal cells and contain residual aborted fetal DNA. While newer vaccines produced using aborted fetal cells do inform consumers, in their package inserts, that the vaccines contain contaminating DNA from the cell used to produce the vaccines, they do not identify the cells as being derived from electively aborted human fetuses.”

Dr. Theresa Deisher, Ph.D.

CARMEN WHITE May 4, 2013 at 10:35 pm This is so AWESOME!!!! Thank you for taking the time to put this together. Hopefully with more people like you, we can continue to educate more parents about the harmful effects of vaccines. Reply

sandy fleming May 5, 2013 at 1:53 am I am really curious, how did you find these? I thought I was pretty good at googling, but never came across so much hard science when I did my research, instead I’d come across something on “Natural News” but never able to find these peer reviewed studies. If you don’t mind sharing, can you tell me how you found most of these? Reply
Pingback: my response to a friend who fears vaccination and is unsure what to do. | The Refurbished Rogue's Blog

myautisticmuslimchild June 1, 2013 at 1:24 am Thank you for this post. i will be posting this link on my blog. I researched a lot, bc my son’s problem started after his 13 months vaccine (rather 12 but i was late for 1 month). i always swear by that his autism has something to do with his vaccination since he got so sick after 4 combination shots. We are still struggling, but if I can help other families to make a better decision about vaccination ut will worth all the fight. Reply

the referbished rogue June 1, 2013 at 1:57 am thank you for the kind words. I don’t know how God decides which children will become autistic..but I do know that he chooses strong families who are not broken by this condition and he chooses parents like yourself who search to help others even through their own challenges. Thank you for allowing others to enter into your world and learn from your experiences. Keep fighting the good fight -briana Reply

Sheri Nakken, former RN, MA, Hahnemannian Homeopath November 17, 2013 at 7:03 pm I really don’t think God decides this…………….my God doesn’t cause injury or harm or pain. It is humans who do this.

the referbished rogue November 17, 2013 at 9:09 pm You are right..evil does not come from God but from sinful man. I do, however, believe that God allows bad things to happen at times for a higher purpose. For a purpose that only He knows. He allows bad things to happen only when the outcome from them will do good things. example: a Christian lady has cancer but while she is in the hospital, she witnesses to her roommate and her roommate becomes a follower of Jesus Christ. There could be two endings to this story..both good, one – the lady could receive healing and go on to live a long life. or two – the Lord could take her to spend an eternity with Him.

Sheri Nakken, former RN, MA, Hahnemannian Homeopath November 17, 2013 at 9:13 pm those outcomes could happen, but a perfect loving God could NOT cause these things, or even allow these things (if allowed them, is not the perfect God). I have a different view on this. If God allows or causes, then God is not a perfect loving being. Yes, those outcomse could happen, but not because God uses us in this way.

the referbished rogue November 17, 2013 at 10:06 pm The world that God intented for us to live was perfect..no pain..no sadness. But because God gave us freewill and is not a dictator..man chose to go against God and sin entered this world. From that point on..man has had to toil to eat..women scream out in pain during childbirth. But out of these hardships do you not still see love? Food to fill our bellies and children to love. The ultimate reason that I know that God is love through all the darkness..is that He sent his son Jesus Christ to die for our sins so that we may have life. Nothing that happens to us on this earth matters when you realize that heaven is ours because of what Jesus did on behalf of His Father. Just one example I would like for you look into if you like, is the book of Job. Regardless that we may see some things differently..let us keep our eyes on what really matters. Let us keep our eyes on Jesus. http://www.gotquestions.org/God-allow-Satan-attack.html

the referbished rogue November 17, 2013 at 10:36 pm I just thought about this post..i wrote this over a year ago but this touches on our discussion and this is from my heart. https://therefurbishedrogue.wordpress.com/2012/07/03/on-the-child-i-lost-the-child-who-waits-for-me/
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shanklandfamily September 13, 2013 at 6:11 pm What an amazing list! Thank you SO MUCH for putting this together!! I have been looking for more factual information like this and your list is just what I need to get started in my reading. Your hard work is much appreciated. Reply

the referbished rogue September 15, 2013 at 4:27 am So very glad to hear it. God bless! Reply

Kathleen E W Bailey September 15, 2013 at 4:14 pm Reblogged this on Soul Kitty and commented: Wow, a wealth of info! Reply

Sheri Nakken, former RN, MA, Hahnemannian Homeopath November 17, 2013 at 7:02 pm What an incredible list you have compiled! Wonderful and thank you. Will have to read further and see who you are! Reply

the referbished rogue November 17, 2013 at 9:03 pm thank you and your welcome! ohh Lord..im afraid of what you may find. Laugh, laugh. God bless you! Reply

puameliaclinic November 17, 2013 at 10:43 pm Reblogged this on The Pua Melia Clinic and commented: A page on getting some papers on Jab research Reply

notidlechatter November 18, 2013 at 1:45 pm I love all the titles to your blogs. It seems as if we have been on a similar journey. I also bask in God’s grace and seek to share the truths He teaches me with others. I have a particular interest in health, wellness and avoiding vaccines. I am learning about the technology I need to get the message out more effectively. I’ve started a blog at http://www.journeyboost.com I appreciate all the work you have put in and I wish all my friends and acquaintances who want to convince me that the science supports vaccines would read every article! Thank you. Reply

the referbished rogue November 18, 2013 at 4:58 pm Thank you for the encouragement! Seriously..that meant a lot to me. I can’t wait to.check out your blog 🙂 In Christ’s love and maranatha – briana Reply

Lou January 7, 2014 at 6:45 am Wonderful – many thanks. In my own years of research, it always bugged me why some children / people were effected and others not (I get this question sometimes). There are a few that I recall which explains why: 1. manufacture conditions can vary and ingredients/contamination occurs in “batches”. 2. temperature control 3. varying levels of toxic additives (e.g. mercury – can be more damaging if the vial is not shaken before injection) 4. the state of the immune system 5. autism is higher in boys because of the way mercury reacts with male hormones. Just to name a few….Certain groups are used more for “guinea pig” testing than other groups. Reply

the referbished rogue January 7, 2014 at 9:59 am Very good reasoning! I agree with you. It’s a shame that an industry that affects ( I really hope i used the right one there. . I always question myself ha) isn’t more aware and looking to fix these issues for the sake of the millions of children who, by blind faith, are subjected to these things. God bless you. – briana Reply

David September 2, 2015 at 10:58 am It’s about genetics. Some people have gene combinations that don’t allow them to methylate the toxins in Vaccines (along with other genes that contribute to adverse reactions in other ways). Meaning, their body doesn’t detect the toxins and therefore doesn’t get rid of them, so you have Aluminum, Mercury and other carcinogenics circulating in the system or burying into cells. There are therapies such as Chelation which flush these toxins, so there is hope. The problem is that NO ONE does genetic testing prior to Vaccination to determine if this is a problem. This is why some people have adverse reactions to Vaccines and some do not.

This is a hard science, called Epigenetics. Reply

Judy March 12, 2014 at 6:55 pm So many Newspapers are pushing provax messages – these journalists have not done any research. It is important to add to the comments whenever you can – not only do you educate the journalists but you may help inform the public and give another view. Love your Blog – great information, thank you so much. Reply

the referbished rogue March 15, 2014 at 1:56 am Your welcome so much, Judy 🙂 it makes me happy when I get a notification that this post has been viewed by someone referred to it from a comment on a pro vax, propaganda article. God bless 🙂 Reply

Chris March 14, 2014 at 2:28 am Keep up the good work!! The world is waking up. .. Reply

Gabriel March 19, 2014 at 8:15 pm Thanks for doing all this work. I do have one question. How do you know that the articles are “peer reviewed”? Thanks! Reply

the referbished rogue March 30, 2014 at 6:31 pm Your welcome Gabriel.. And thank you. All the links are to articles that have been published in journals that have a panel of medical / science professionals which must approve the data and the integrity of the article before it is allowed to be published. Reply

David Fenton December 20, 2015 at 6:13 pm Hi, I’m developing a web site called real-morality and would like to use you list of peer reviewed articles as is, with a credit to you and link. In time I might organise them into some logical groups. My website is still in parking mode. Thanks and appreciation

the referbished rogue January 16, 2016 at 9:20 pm Sure, that sounds fine. Thank you for wanting to include it. God bless, briana

David September 2, 2015 at 11:00 am Most of these are from NIH. I’ve found these myself as well. You can’t get more peer-reviewed than a government health and technology agency. Reply
Chris Robison March 30, 2014 at 6:04 pm bless you for doing this!! but I thought all anti-vaxxers are “anti-science”.. that’s what the science magazines all tell us.. 🙂 Reply

Tina "I" April 2, 2014 at 6:48 am Wow! This is wonderful! Thanks so much for the time you have put into this, and especially for “sharing”. Everyone needs to keep getting the word out, so those that blindly follow, might eventually get their wake-up call… Hopefully, before it’s too late. Thank you! Thank you! Thank you! So nice to have it all in one place, as a reference. Reply

the referbished rogue April 2, 2014 at 10:47 am Your welcome.. And thank you for commenting (every girl likes to feel special sometimes..ha) God bless! Reply

Merideth April 19, 2014 at 8:34 pm Can you add a Pinterest link, so I can pin it, and keep it forever! Thanks Reply

the referbished rogue April 21, 2014 at 6:06 pm Yes :)… Once I figure it out and am at my desktop..I will add it. Reply
Shane Thepeopleschemist Ellison April 28, 2014 at 6:49 pm Good parent! Reply

Lee June 14, 2014 at 5:21 pm Awesome job!!!!! Thanks Reply

Kim July 14, 2014 at 8:37 pm Thank you SO VERY MUCH for doing this! I have been helping members of my family research this issue (some of them for the very first time); this will help tremendously. Reply

Melinda Blondeaux July 27, 2014 at 12:09 pm You will probably want to add this one too: Abstract: “Background: The Shaken Baby Syndrome conceived by Guthkeltch to explain bruises, fractures, retinal and cerebral haemorrhage and encephalopathy in children, called the “triad”, can be explained by an autoimmune reaction to antigens in a genetically susceptible child. Method: Children diagnosed as suffering from Non-accidental injuries were investigated for evidence of immune response reactions following mandated vaccination and childhood illnesses.

Results: It was found in all the cases reported here the response to antigenic stimulation damaged the Beta cells in the Pancreas causing Hypoinsulinaemia which inhibited the cellular uptake of Vitamin C resulting in liver dysfunction, failure of carboxylation of the Vitamin K dependent proteins resulting in haemorrhages and fractures associated with the “triad”. Conclusion: Fractures, retinal and subdural haemorrhages and encephalopathy in children – is an autoimmune response to antigenic stimulation in a genetically susceptible individual. Common antigens are the mandated vaccines, viral bacterial and parasitic infections. ” Interpretation “In all four cases shown here there is evidence that hyperglycaemia followed vaccination and hyperglycaemia implies hypoinsulinism, an autoimmune disorder resulting from the destruction of the Beta cells of the pancreas. Since insulin is required for the transfer of vitamin C into the cells the intracellular vitamin C is reduced[12]. The resulting “tissue scurvy” compromises the function of the Liver by inhibiting carboxylation of the clotting and bone forming factors and is manifested as the signs and symptoms of the “triad”. Both Dr Kalokerinos and Professor Clemetson recommended giving the infant Vitamin C before vaccination but it would seem more appropriate to do an intradermal skin test to test for sensitivity in every case. Both were firmly of the view that a metabolic abnormality of Vitamin C was the essential cause of the signs and symptoms of the alleged “Non-accidental injuries”. ” Michael D Innis. Autoimmunity and Non-Accidental Injury in Children. Clinical Medicine Research. Vol. 2, No. 3, 2013, pp. 40-44. doi: 10.11648/j.cmr.20130203.15 Click to access 10.11648.j.cmr.20130203.15.pdf Reply

the referbished rogue August 28, 2014 at 9:43 pm Thank you 🙂 I will add this along with some others. Reply

Megan @LivingWhole.org September 6, 2014 at 8:37 pm Wow! You really did your research! I am very impressed and am glad I came across your blog. Keep it up. 🙂 Reply

the referbished rogue September 7, 2014 at 11:01 am If this is Megan from the living whole that recently published the article about God not liking vaccines.. wow!! I am honored!! Your website is awesome. Reply
Marcella Piper-Terry February 2, 2015 at 11:22 am Thank-you so much for this amazing resource! I would love to share it as a guest blog on VaxTruth.org. Reply

the referbished rogue February 2, 2015 at 5:27 pm Oh wow! Thank you thank you! Of course you may! I am tickled right now 🙂 and honored for you to have read my blog!!! I love TTMR! Reply

the referbished rogue February 2, 2015 at 5:31 pm I love vax truth as well.. I was so excited I don’t know what I wrote! God bless!!

punyahannawilbur February 3, 2015 at 4:55 am Reblogged this on Hanna Wilbur's. Reply

Lou July 22, 2015 at 11:08 pm Praise God for this site! Reply
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May 3, 2013
my list of peer reviewed vaccine research
• 57 Comments
This list is just a thrown together list and is pretty helter skelter..but, there are a lot of links to lead you down the research path if you are searching. There are are so many, many, many more out there that haven’t made it to this list. They sit and wait for me to find them..i better get to looking.. May our truth digging be successful!
Hypothesis: conjugate vaccines may predispose children to autism spectrum disorders.
the potential effects of conjugate vaccines on neural development merit close examination. Conjugate vaccines fundamentally change the manner in which the immune systems of infants and young children function by deviating their immune responses to the targeted carbohydrate antigens from a state of hypo-responsiveness to a robust B2 B cell mediated response. This period of hypo-responsiveness to carbohydrate antigens coincides with the intense myelination process in infants and young children, and conjugate vaccines may have disrupted evolutionary forces that favored early brain development over the need to protect infants and young children from capsular bacteria.
http://www.ncbi.nlm.nih.gov/pubmed/21993250
Serological association of measles virus and human herpesvirus-6 with brain autoantibodies in autism.
Considering an autoimmunity and autism connection, brain autoantibodies to myelin basic protein (anti-MBP) and neuron-axon filament protein (anti-NAFP) have been found in autistic children. In this current study, we examined associations between virus serology and autoantibody by simultaneous analysis of measles virus antibody (measles-IgG), human herpesvirus-6 antibody (HHV-6-IgG), anti-MBP, and anti-NAFP. We found that measles-IgG and HHV-6-IgG titers were moderately higher in autistic children but they did not significantly differ from normal controls. Moreover, we found that a vast majority of virus serology-positive autistic sera was also positive for brain autoantibody: (i) 90% of measles-IgG-positive autistic sera was also positive for anti-MBP; (ii) 73% of measles-IgG-positive autistic sera was also positive for anti-NAFP; (iii) 84% of HHV-6-IgG-positive autistic sera was also positive for anti-MBP; and (iv) 72% of HHV-6-IgG-positive autistic sera was also positive for anti-NAFP. This study is the first to report an association between virus serology and brain autoantibody in autism; it supports the hypothesis that a virus-induced autoimmune response may play a causal role in autism.
http://www.ncbi.nlm.nih.gov/pubmed/9756729
Effectiveness of pertussis vaccines for adolescents and adults: case-control study
The adjusted estimate of effectiveness of Tdap vaccination against pertussis was 53.0.
http://www.bmj.com/content/347/bmj.f4249
Neurologic Adverse Events Following Vaccination (Progress in Health Sciences Vol. 2(1) 2012•pp 129-141.)
“Conclusions: Despite the assurances of the necessity and safety of vaccinations, there are more and more questions and doubts, which both physicians and parents are waiting to be clarified… It seems that it would be worthwhile to apply the precautionary principle – the ethical principle (from 1988) according to which if there is a probable, although poorly known, risk of adverse effects of new technology, it is better not to implement it rather than risk uncertain but potentially very harmful consequences.”
http://progress.umb.edu.pl/sites/progress.umb.edu.pl/files/129-141.pdf
Abnormal measles-mumps-rubella antibodies and CNS autoimmunity in children with autism.

“Thus the MMR antibody in autistic sera detected measles HA protein, which is unique to the measles subunit of the vaccine. Furthermore, over 90% of MMR antibody-positive autistic sera were also positive for MBP autoantibodies, suggesting a strong association between MMR and CNS 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.”
http://www.ncbi.nlm.nih.gov/pubmed/12145534
 Influenza: marketing vaccine by marketing disease
Closer examination of influenza vaccine policies shows that although proponents employ the rhetoric of science, the studies underlying the policy are often of low quality, and do not substantiate officials’ claims. The vaccine might be less beneficial and less safe than has been claimed, and the threat of influenza appears overstated.
http://www.bmj.com/content/346/bmj.f3037
An unmasking phenomenon in an observational post-licensure safety study of adolescent girls and young women.
Our recent experience in a post-licensure safety study of autoimmune conditions following the quadrivalent human papillomavirus vaccine in 189,629 girls and young women ages 9-26 years led us to question the adequacy of the exclusion of Day 0 events to prevent the erroneous association of prevalent conditions with vaccination. Of the 18 confirmed cases of Graves’ disease diagnosed in days 1-60 following vaccination, only 6 cases appeared to be truly new onset. Among the remaining 12 cases, 2 cases had abnormal thyroid stimulating hormone or thyroxine labs drawn prior to or on Day 0 but had no documented pre-existing symptoms. The other 10 cases had mention of symptoms of hyperthyroidism referencing a period prior to first HPV-4 dose. This ‘unmasking’ phenomenon, due to health care visits that include vaccination and new workups of preexisting symptoms, may not be adequately controlled through the exclusion of Day 0 events.
http://www.ncbi.nlm.nih.gov/m/pubmed/22580356/
 
How aluminum, an intracellular ROS generator promotes hepatic and neurological diseases: the metabolic tale
Metal pollutants are a global health risk due to their ability to contribute to a variety of diseases. Aluminum (Al), a ubiquitous environmental contaminant is implicated in anemia, osteomalacia, hepatic disorder, and neurological disorder. In this review, we outline how this intracellular generator of reactive oxygen species (ROS) triggers a metabolic shift towards lipogenesis in astrocytes and hepatocytes. This Al-evoked phenomenon is coupled to diminished mitochondrial activity, anerobiosis, and the channeling of α-ketoacids towards anti-oxidant defense. The resulting metabolic reconfiguration leads to fat accumulation and a reduction in ATP synthesis, characteristics that are common to numerous medical disorders. Hence, the ability of Al toxicity to create an oxidative environment promotes dysfunctional metabolic processes in astrocytes and hepatocytes. These molecular events triggered by Al-induced ROS production are the potential mediators of brain and liver disorders.”
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Waning of Maternal Antibodies Against Measles, Mumps, Rubella, and Varicella in Communities With Contrasting Vaccination Coverage
Conclusions: Children of mothers vaccinated against measles and, possibly, rubella have lower concentrations of maternal antibodies and lose protection by maternal antibodies at an earlier age than children of mothers in communities that oppose vaccination. This increases the risk of disease transmission in highly vaccinated populations.
http://jid.oxfordjournals.org/content/early/2013/04/29/infdis.jit143.full
“vaccine injury is so rare..don’t worry about it!” who has heard this?

“The Health Resources and Services Administration (HRSA) is publishing this notice of petitions received under the National Vaccine Injury Compensation Program.. A pet…ition may be filed with respect to injuries, disabilities, illnesses, conditions, and deaths resulting from vaccines described in the Vaccine Injury Table… Set forth below is a list of petitions received by HRSA on * March 13, 2013, through April 30, 2013.*”
[take note of #7 and #17..]
1. Tory J. and Sarah E. Moody on behalf of Victorya E. Moody, Bedford, Indiana, Court of Federal Claims No: 13-0190V.
2. Pamela Jean Peguess, Memphis, Tennessee, Court of Federal Claims No: 13-0191V.
3. Eileen Goeschel, Sarasota, Florida, Court of Federal Claims No: 13-0199V.
4. Kearsten Demczuk, Park Ridge, Illinois, Court of Federal Claims No: 13-0205V. 5. Howard Reddy and Hanan Tarabay on behalf of Andrew Howard Reddy, Pensacola, Florida, Court of Federal Claims No: 13-0208V.
6. Mona Marie Troup, Everett, Washington, Court of Federal Claims No: 13-0209V.
7. Angel Blackstone on behalf of S.B., Deceased, Trenton, New Jersey, Court of Federal Claims No: 13-0213V.
8. Isidra Durwin, Sarasota, Florida, Court of Federal Claims No: 13-0214V.
9. Nancy and Sandro Giannetta on behalf of A.M.G., Sarasota, Florida, Court of Federal Claims No: 13-0215V.
10. Kimberly Pedersen, West Allis, Wisconsin, Court of Federal Claims No: 13-0216V.
11. Charles and Jeannie Maikish on behalf of S.M., Nyack, New York,Court of Federal Claims No: 13-0217V.
12. Ina Scanlon, Muncie, Indiana, Court of Federal Claims No: 13-0219V.
13. David Stachlewitz on behalf of H.G.S., Glendale, Arizona, Court of Federal Claims No: 13-0220V.
14. Mary E. Thompson, Brookport, Illinois, Court of Federal Claims No: 13-0222V.
15. Matthew Gorski, Wynnewood, Pennsylvania, Court of Federal Claims No: 13-0224V.
16. Woodrow Coffey, Jr., Irvine, California, Court of Federal Claims No: 13-0225V. 17. Stephen Warren on behalf of Taylor Warren, Deceased, New York, New York, Court of Federal Claims No: 13-0226V.
18. Robert Wiggins, Nashville, North Carolina, Court of Federal Claims No: 13-0228V.
19. Peggy Kalmeyer, Depew, New York, Court of Federal Claims No: 13-0230V.
20. Rosemary and Wayne Trezza on behalf of P.T., West Orange, New Jersey, Court of Federal Claims No: 13-0231V.
21. Jane Tomassetti, Woodbury, Minnesota, Court of Federal Claims No: 13-0234V.
22. Everett Johnson, Sr., Ashland, Kentucky, Court of Federal Claims No: 13-0235V.
23. Edwin W. Fockler, Sarasota, Florida, Court of Federal Claims No: 13-0237V. 24. James Cox, Las Cruces, New Mexico, Court of Federal Claims No: 13-0238V. 25. Chanel and Paul A. Monroe on behalf of Angelina Monroe, Las Vegas, Nevada, Court of Federal Claims No: 13-0239V.
26. Noteel Koss, Houston, Texas, Court of Federal Claims No: 13-0240V.
27. Tamika M. Kratzer on behalf of Ian M. Kratzer, Sacramento, California, Court of Federal Claims No: 13-0243V.
28. Rosalie Peck, Boston, Massachusetts, Court of Federal Claims No: 13-0249V. 29. Shannon Keller, Sacramento, California, Court of Federal Claims No: 13-0250V.
30. Edwina Bradshaw, North Myrtle Beach, North Carolina, Court of Federal Claims No: 13-0252V.
31. William and Brenda Lehann Rodriguez on behalf of C.R., Clayton, Georgia, Court of Federal Claims No: 13-0253V.
32. Corrine K. Ibana, Kamuela, Hawaii, Court of Federal Claims No: 13-0257V. 33. Lorel Cubano, San Juan, Puerto Rico, Court of Federal Claims No: 13-0259V. 34. Brittany and Davey Lambert on behalf of Noah Lambert, Memphis, Tennessee, Court of Federal Claims No: 13-0265V.
35. Scott and Caroline VanScoy on behalf of Alyssa VanScoy, Simi Valley, California, Court of Federal Claims No: 13-0266V.
36. Jane Sprecher, Reading, Pennsylvania, Court of Federal Claims No: 13-0271V.
37. Georgia Murdock, Silver Spring, Maryland, Court of Federal Claims No: 13-0273V.
38. Willie Andre Simmons, Augusta, Georgia, Court of Federal Claims No: 13-0274V.
39. Jung Park, M.D., New York, New York, Court of Federal Claims No: 13-0275V. 40.

Allison and Steven Council on behalf of Adam Council, Plainfield, Illinois, Court of Federal Claims No: 13-0276V.
41. Maryann Giordano, Lindenhurst, New York, Court of Federal Claims No: 13-0277V.
42. Laura A. Jones, Greensboro, North Carolina, Court of Federal Claims No: 13-0279V.
43. David D. Griffin, Afghanistan, Court of Federal Claims No: 13-0280V.
44. James Demoski, Endicott, New York, Court of Federal Claims No: 13-0286V. 45. Christina N. Steinat, Seattle, Washington, Court of Federal Claims No: 13-0287V.
46. Jessica L. Stone, Baraboo, Wisconsin, Court of Federal Claims No: 13-0289V. 47. Holly Rhew, Wichita, Kansas, Court of Federal Claims No: 13-0293V.
48. Janet DeYear, Dallas, Texas, Court of Federal Claims No: 13-0299V.
49. Cynthia Adkins, Sarasota, Florida, Court of Federal Claims No: 13-0295V.
50. Saurabh V. and Archana Amin on behalf of Sheaa Amin, Linwood, New Jersey, Court of Federal Claims No: 13-0300V.
51. Juliet and Mohamed Edoo on behalf of Justin Edoo, Miami, Florida, Court of Federal Claims No: 13-0302V.
52. James Boyer, Boston, Massachusetts, Court of Federal Claims No: 13-0303V.
*these are from March 13, 2013 – April 30, 2013. 48 days. what is the true number that these 52 petitions represent? how many don’t file claims? think about it..its scary. I wish we could see more about these petitions..more about the injury caused.It is impossible for a parent to make a solid risk/benefit analysis when it comes to vaccinations.. I don’t care what anyone may say.. vaccine injury is downplayed and pushed aside, disease rates and risks are over exaggerated and blasted throughout the media via mass scare campaigns (remember those 8 measly cases of the measles in Wales during the month of march 2013?) ..and natural and safe preventative measures and treatments are suppressed. How are we supposed to make an informed medical decision when it comes to our children being injected with almost 50 doses of 16 vaccines before the age of 6?
https://www.federalregister.gov/articles/2013/05/24/2013-12347/national-vaccine-injury-compensation-program-list-of-petitions-received?utm_content=next&utm_medium=PrevNext&utm_source=Article
“In 1990, infants received a total of 15 vaccine doses prior to their first year of life: 3 DPT injections (9 vaccine doses), 3 polio, and 3 Hib vaccines—5 vaccine doses at 2, 4, and 6 months of age. By 2007, the CDC recommended 26 vaccine doses for infants: 3 DTaP, 3 polio, 3 Hib, 3 hepatitis B, 3 pneumococcal, 3 rotavirus, and 2 influenza vaccines. While each childhood vaccine has individually undergone clinical trials to assess safety, studies have not been conducted to determine the safety (or efficacy) of combining vaccines during a single physician visit as recommended by CDC guidelines. For example, 2-, 4-, and 6-month-old infants are expected to receive vaccines for polio, hepatitis B, diphtheria, tetanus, pertussis, rotavirus, Haemophilus influenzae type B, and pneumococcal, all during a single well-baby visit—even though this combination of 8 vaccine doses was never tested in clinical trials.
An article written by Guess, representing a vaccine manufacturer, claimed that it is “impractical to conduct preapproval studies of all combinations [of vaccines] in clinical practice.”1 However, a recent study by Miller and Goldman found that among the developed nations, infant mortality increased with an increase in the number of vaccine doses.2 Similar associations have also been found with respect to other serious adverse outcomes. Delong reported that the higher the proportion of children receiving recommended vaccinations, the higher the prevalence of autism or speech and language impairment.3 A CDC report on mixed exposures to chemical substances and other stressors, including prescribed pharmaceuticals, found that they may produce “increased or unexpected deleterious health effects.” In addition, “exposures to mixed stressors can produce health consequences that are additive, synergistic, antagonistic, or can potentiate the response expected from individual component exposures.