Endonuclease fingerprint indicates a synthetic origin of SARS-CoV-2
Just as ACIP warms up to a vaccine with no benefit and all risk to children... this.
From Bruttel, Washburne and VanDongen (Germany & USA), uploaded today, 10/20/2022
Endonuclease fingerprint indicates a synthetic origin of SARS-CoV-2
Abstract
To prevent future pandemics, it is important that we understand whether SARS-CoV-2 spilled over directly from animals to people, or indirectly in a laboratory accident. The genome of SARSCOV-2 contains a peculiar pattern of unique restriction endonuclease recognition sites allowing efficient dis- and re-assembly of the viral genome characteristic of synthetic viruses. Here, we report the likelihood of observing such a pattern in coronaviruses with no history of bioengineering. We find that SARS-CoV-2 is an anomaly, more likely a product of synthetic genome assembly than natural evolution. The restriction map of SARS-CoV-2 is consistent with many previously reported synthetic coronavirus genomes, meets all the criteria required for an efficient reverse genetic system, differs from closest relatives by a significantly higher rate of synonymous mutations in these synthetic-looking recognitions sites, and has a synthetic fingerprint unlikely to have evolved from its close relatives. We report a high likelihood that SARSCoV-2 may have originated as an infectious clone assembled in vitro.
Quote
"The genome of SARSCOV-2 contains a peculiar pattern of unique restriction endonuclease recognition sites allowing efficient dis- and re-assembly of the viral genome characteristic of synthetic viruses. Here, we report the likelihood of observing such a pattern in coronaviruses with no history of bioengineering. We find that SARS-CoV-2 is an anomaly, more likely a product of synthetic genome assembly than natural evolution. The restriction map of SARS-CoV-2 is consistent with many previously reported synthetic coronavirus genomes, meets all the criteria required for an efficient reverse genetic system, differs from closest relatives by a significantly higher rate of synonymous mutations in these synthetic-looking recognitions sites, and has a synthetic fingerprint unlikely to have evolved from its close relatives. We report a high likelihood that SARSCoV-2 may have originated as an infectious clone assembled in vitro."
It is all graphene / nanotechnology poisoning
So, those CRIMINALS just added THIS to the "vaccine" "schedule": ALC-0315 and ALC-0159
Intended for research purposes. Not suitable for human or veterinary diagnostic or therapeutic use
https://outraged.substack.com/p/so-those-criminals-just-added-this
Occam’s Razor states Lab created.