zlacker

but my friends who are tell me that's a lot of changes, and that experiments might change a few base pairs or proteins at a time. A lab leak theory doesn't explain how gain of function study resulted in so many mutations, unless they were blasting these viruses with radiation

Or explicitly creating chimeric coronaviruses, which has been the state of the are for some time. Here's https://pubmed.ncbi.nlm.nih.gov/26552008/ one of the sources of smoke on this, a 2015 paper co-authored by the Bat Woman (2nd to last author), the key sentence from the abstract:

Using the SARS-CoV reverse genetics system, we generated and characterized a chimeric virus expressing the spike of bat coronavirus SHC014 in a mouse-adapted SARS-CoV backbone.

Have you read the fine article? It cites more than a few papers.

>>Throwa+(OP)
I've read a few articles, skimmed a few papers and sent them to friends. The counterargument is that there still aren't enough similarities.

The mutations on covid 19 are Really Different compared to the known and studied viruses. If it was a lab leak of an engineered chimera, you'd be able to see that A proteins came from virus X and B proteins came from virus Y and Z, but that hasn't been shown to be the case. From what I understand there are a bunch of smaller mutations across a lot of proteins resulting in something that doesn't really line up with known and studied genomes.

This paper actually goes through and compares the DNA of covid 19 against several other studied viruses: https://www.nature.com/articles/s41579-020-00459-7

>>Jarwai+43
Of course that says little about SARS-CoV-2 relative to all the other viruses we don't know about, either sitting in a Chinese government lab, or in a bat cave somewhere.

I guess I don't find the argument "we can't figure out how to reconstruct SARS-COV-2 from known viruses" very convincing on either side.

>>teorem+9d
That's fair. I wouldn't say that it's "we can't figure it out" but rather that "doing so takes a lot of mutations and thus resources that may be difficult to do under the table"

Sitting in a cave somewhere implies not being studied, right? Which is more the "natural mutation" thing.

Sitting in some government lab is a different story and depends on belief in scientific institutions to do science and publish peer reviewed papers and all that jazz.

>>Jarwai+de
Another question is how you can make a virus evolve in the direction you want. 20 years of bat evolution would not necessarily bring a furin cleavage site, so how do you make sure it does?

>>Throwa+(OP)
What's the deal with you continuously referring to Zhengli-Li Shi as "Bat Woman" or "Bat Lady"? Is there some reason you can't or don't want to call her by her name?

>>Jarwai+43
My understanding is that this is what gain of function research is all about. Accelerated evolution within a lab towards infecting a specific species.

It doesn't have to be crispr introducing reach mutation.

>>igravi+nM
Because everyone knows whom I'm referring to when I use that title she earned through a lot of hard work, while I've seen multiple Romanized versions of her name.

>>Husafa+bS
RaTG13 is decades of evolution away from SARS-CoV-2, all over its genome.

You don't get there by splicing an ACE2 spike onto an RaTG13 backbone and passing it through a dozen mice. That gives you something that still looks similar to RaTG13 and infects mice.

The ACE2 spike also looks most similar to a previously unknown ACE2-binding spike protein found in malaysian pangolins.

So WIV would have had to have discovered that pangolin spike-protein, kept it secret, spliced it into an RaTG13 backbone, then not used mice but passed it through a species like that had a human-like ACE2 for a decade and millions of animals.

An alternative hypothesis is that Charles Darwin did that experiment.

>>Throwa+(OP)
The spike protein is the biggest difference between RaTG13 and SARS-CoV-2. To produce SARS-CoV-2 from it that would imply that WIV had unpublished sequences from the Pangolin-CoV spike protein that they used to combine with an RaTG13 backbone. You then do not get SARS-CoV-2 out of passing that through mice, you get a mouse virus. You'd need to pass it serially through something with a human-like ACE2 like minks. Then you need to do that enough to accumulate a thousand mutations which takes decades in nature and would take millions of animals.

That likely did happen, but Charles Darwin was the geneticist that executed the gain of function experiment via serial passage through that many animals.

> Have you read the fine article? It cites more than a few papers.

Yes, i read it. The ability to construct bibliographic references is also a fairly widely-held and unimpressive skill.

>>lamont+rT1
> To produce SARS-CoV-2 from it that would imply that WIV had unpublished sequences from the Pangolin-CoV spike protein

According to the article, the database of sequences for the WIV samples had been deleted before the pandemic became widespread, so there was no way to verify this, but also somewhat suspicious.

>you then do not get SARS-CoV-2 out of passing that through mice, you get a mouse virus. You'd need to pass it serially through something with a human-like ACE2 like minks.

From the article:

>Using the gene-editing technology known as CRISPR, the researchers had engineered mice with humanized lungs, then studied their susceptibility to SARS-CoV-2. As the NSC officials worked backward from the date of publication to establish a timeline for the study, it became clear that the mice had been engineered sometime in the summer of 2019, before the pandemic even started.

So, it's likely they had mice with humanized lung and ACE2 receptors, no?