Jonathan Weissman Profile picture
Mar 3, 2022 11 tweets 7 min read Read on X
[1/9] This is the untold and shocking story of Pfizer’s 12-to-15-year-old clinical trial. Just 2264 adolescents were randomised between October 2020 and January 2021. I will describe the various related, serious and life-threatening injuries sustained by these youngsters. Image
[2/9] 1180 of these youngsters received at least one 30μg dose before the data cutoff date, 13 March 2021, comprised of 1131 adolescents during the blinded study and 49 from the placebo group, who turned 16, were unblinded and chose to be treated under the FDA’s recent 16+ EUA. Image
[3/9] Although the study’s sample size was tiny and its statistical power weak, clinical trial data (however incomplete!) is as gold dust, as it represents a closed cohort. It can detect a crucial safety signal before treating every adolescent on the planet. Injuries included… Image
[4/9]
* 1 related life-threatening fever
* 1 related life-threatening anaphylaxis
* 1 related with “reasonable possibility” myopericarditis, hospitalised, “limited activity” advised at 2 months
* 3 on SSRI medication for depression, each hospitalised with symptom “exacerbation” ImageImageImageImage
[5/9] One more. Maddie de Garay suffered severe abdominal/chest pain and extreme numbness within a day of dose 2. She developed blood in her urine, mobility issues, is now paralysed and uses a nasogastric tube to eat. Mislabelled as “functional abdominal pain” and “neuralgia”. ImageImageImageImage
[6/9] Aside from those 7 youngsters, lymphadenopathy, swollen lymph nodes, occurred at a statistically significantly higher rate in the treatment group (9 vs. 2). Likewise for lymphadenopathy instances judged to be related to treatment (7 vs. 1). ImageImageImageImage
[7/9] The reactogenicity safety data is dramatic. These side effects were likely too obvious for the study blind to be maintained. The study’s administrators were unblinded anyway! Post dose 2, in the treatment group, 51% used antipyretic medication vs. 9% in the placebo group. Image
[8/9] There were no severe COVID-19 cases in either group. What was the efficacy “benefit” for all these injuries? The clinical endpoint was symptomatic infection confirmed by an NAAT test. We don’t know the positive PCR Cts, the symptoms, nor whether transmission was reduced. ImageImageImage
[9/9] To reiterate, the study’s data cutoff date was 13 March 2021. These injuries were all known by the time:
* Pfizer boasted their drug was “well-tolerated”
* the trial results were published in the NEJM
* the MHRA extended their TUA
* the JCVI advised the UK-wide rollout ImageImageImageImage
BONUS: There was an extra event in the open-label study:
* life-threatening serious adverse event hospitalised a 16-year-old with "depression"

This is aside from the 3 depression SAEs during the blinded study. No indication the youngster was taking an SSRI or depressed before. Image
I've now written up these related, serious and life-threatening adverse events from Pfizer's adolescent clinical trial in a table. Remember, these occurred amongst only 1180 subjects. All of these adverse events occurred prior to Pfizer's press briefing on 31 March 2021. Image

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More from @AllTheRisks

May 9, 2022
[1/19] Could Omicron be the calm before antibody dependent enhancement (ADE) induces a devastating mass cytokine storm? Dr Vanden Bossche’s (@GVDBossche) new white paper hypothesises a tragic evolutionary pathway the virus may now be forced into due to our “vaccine” foolishness. Image
[2/19] GVB characterises Omicron’s two defining characteristics:
i) high infectivity rate with the virus confined to the upper respiratory tract
ii) low virulence (mild symptoms) due to inefficient pulmonary infection

GVB then suggests how the next class of variants may emerge. Image
[3/19] We start with a few of GVB’s definitions. First up is trans fusion, the phenomenon whereby infected cells fuse with neighbouring cells in an ACE-2 independent fashion to form syncytia, multi-cell infected complexes. Image
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