A deadly experiment...

But seriously I'm not sure

Findings:

Between 11th–25th June 2021 (week 7–8 after dose 2), 69 healthcare workers were tested positive for SARS-CoV-2. 62 participated in the clinical study. were (pre)symptomatic with one requiring oxygen supplementation. All recovered uneventfully. 23 complete-genome sequences were obtained. They all belonged to the Delta variant, and were phylogenetically distinct from the contemporary Delta variant sequences obtained from community transmission cases, suggestive of ongoing transmission between the workers. Viral loads of breakthrough Delta variant infection cases were 251 times higher than those of cases infected with old strains detected between March-April 2020. Time from diagnosis to PCR negative was 8–33 days (median: 21). Neutralizing antibody levelsafter vaccination and at diagnosis of the cases were lower than those in the matched uninfected controls. There was no correlation between vaccine-induced neutralizing antibody levels and viral loads or the development of symptoms.

Interpretation:

Breakthrough Delta variant infections are associated with high viral loads, prolonged PCR positivity, and low levels of vaccine-induced neutralizing antibodies, explaining the transmission between the vaccinated people. Physical distancing measures remain critical to reduce SARS-CoV-2 Delta variant transmission.

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Data collection:

We collected demographics, vaccination history and clinical data alongside the results of SARS-CoV-2 PCR diagnosis from the study participants. For SARS-CoV-2 antibody measurement, we obtained 2ml of EDTA plasma from each study participants at diagnosis and at week 1, 2 and 3 after admission. Nasopharyngeal-throat swab collection, PCR testing and viral load conversion Nasopharyngeal swabs were collected and placed in 1mL of viral transport medium, and 200uL was used for viral RNA extraction using the MagNApure 96 platform (Roche Diagnostics, Germany), according to the manufacturer’s instructions. For SARS-CoV-2 RNA detection, we used real-time RT-PCR assay with primers and probe targeted at the envelope protein-coding gene (TIB MOLBIOL)7. PCR Ct values were converted to RNA loads using an in-house established formula (y = -0.3092x + 12.553, R² = 0.9963, where y is viral load and x is Ct value) based on 10-fold dilution series of in-vitro transcribed RNA.

Whole genome sequencing and sequence analysis:

Whole-genome sequences of SARS-CoV-2 were directly obtained from leftover RNA after PCR testing using ARTIC protocol and Illumina reagents on a MiSeq platform with the inclusion of a negative control in every sequencing run. The obtained reads from individual samples were mapped to a SARS-CoV-2 reference genome (GISIAD sequence ID: EPI_ISL_1942165) to generate the consensuses using Geneious software (Biomatter, New Zealand). SARS-CoV-2 variant assignment was carried out using Pangolin.9 Detection of amino acid changes as compared to the original Wuhan strain was done using COV-GLUE.10 Maximum likelihood phylogenetic tree was reconstructed using IQ-TREE.

ADE: Antibody Dependent Enhancement Also known as: Hyper Immune Response Virus Interference Pathogenic Priming Disease Enhancement

Antibody-dependent enhancement or pathogenic priming - another still-unproven yet undebunked threat. Does the "vaccine" create a greater threat to the immune system from contact with the wild virus? In the FDA documents, "vaccine enhanced disease" is listed as a possible outcome. (Fda possible side effects list Oct 2020: https://files.catbox.moe/v8j5u7.png). The skipped animal trials might have highlighted this issue.

https://pubmed.ncbi.nlm.nih.gov/12725690/ https://www.youtube.com/watch?v=TEdVZcp7Lbc https://archive.vn/epdWi

Nov 12 2020 "How Covid-19 vaccine can destroy your immune system" -- https://archive.vn/al2vh

Dec 10, 2020 “Pfizer Covid Vaccine Trial Shows Alarming Evidence of Pathogenic Priming in Older Adults” https://archive.vn/hdlys

Dec 11 2020 "Pfizer COVID vaccine trial shows alarming evidence of pathogenic priming in older adults" https://archive.vn/qVXC5

Dec 11 2020: Hiv side effect "Coronavirus Australia: UQ vaccine risk 'bigger than we thought" https://archive.vn/Ntzop

Jan 18, 2021 Wiki explaining “Antibody-dependent enhancement” https://archive.vn/36Fki

Jan 29 2021: "Dr. Lee Merritt: In Animal Studies, After Being Injected With mRNA Technology, All Animals Died Upon Reinfection" https://archive.vn/THkxd "after mRNA injections have been administered to cats, when the virus arrived once again into the body, it arrived like a Trojan Horse, undetected by the cats' own immune system" All animals die upon reinfection"

Feb 13, 2021 ‘Wiki’ explaining "Cytokine Storm" https://archive.vn/mbNqp

Feb 15, 2021 "Evidence Builds Against Bill Gates For Crimes Against Humanity" https://archive.vn/iGmKY From the article "As of Jan. 29, 501 possible vaccine-related deaths were officially recorded in the CDC Vaccine Adverse Event Reporting System (VAERS), 10,748 reported injuries, and 153 permanent disabilities. Thousands of the adverse reactions have rendered people “unable to work,” or perform “daily activities.” Horrific individual testimony continues to surface, as in the video compilation below.”

June 10 2021: “‘Urgent’ British report calls for complete cessation of COVID vaccines in humans” https://americasfrontlinedoctors.org/frontlinenews/urgent-british-report-calls-for-complete-cessation-of-covid-vaccines-in-humans/ “potential acute and long-term pathologies include: Pathogenic priming, multisystem inflammatory disease and autoimmunity Allergic reactions and anaphylaxis Antibody dependent enhancement Activation of latent viral infections Neurodegeneration and prion diseases Emergence of novel variants of SARSCoV2 Integration of the spike protein gene into the human DNA “It is now apparent that these products in the blood stream are toxic to humans. An immediate halt to the vaccination programme is required whilst a full and independent safety analysis is undertaken to investigate the full extent of the harms, which the UK Yellow Card data suggest include thromboembolism, multisystem inflammatory disease, immune suppression, autoimmunity and anaphylaxis, as well as Antibody Dependent Enhancement (ADE).”