This is a sample guest message. Register a free account today to become a member! Once signed in, you'll be able to participate on this site by adding your own topics and posts, as well as connect with other members through your own private inbox!
![[icon]](/data/avatars/m/5/5167.jpg?1660313464){kind=avatar}
It is able to determine a prior infection independent of vaccination.
No, COVID was the first one to use mRNA technology. They're hopeful that its success will lead to other uses, including but not limited to flu vaccines. And I guess the answer to your last question will depend on the delivery mechanism. Meaning COVID uses the spike protein, but influenza might not be able to deliver via that same structure.
Great article that really sums up a lot of what I've been trying to articulate.
Moderna is working on a combo Covid/flu/RSV vaccine. I'm sure Pfizer/BioNtech is doing something similar.
Is there an antibody test that's not a blood draw? Didn't think they'd do those kinds of test at a chain drugstore.
Not that I'm aware of. It's not really a blood draw, its a simple p.rick of the finger tip. In and out in 15 mins and your finger will stop bleeding before you get your results
I hope the RSV vaccine works, and is able to be adjusted for kids sooner rather than later. Every winter our hospital got slammed with pediatric RSV patients. Even last summer RSV was raging.
I'll try answering this again: Variant testing isn't routinely done, takes time and money, and doesn't change clinical management. We're already having trouble keeping up with testing demands. We don't need to further overwhelm labs with unnecessary tests.
Unknown, but wouldn't be shocking, as there are individual differences in the structure, distribution and density of the receptors the virus uses for cell entry. Our immune systems also have subtle variation, and it's possible some people are much more resistant to infection related to their genetics.
Correct. There are commercial tests which distinguish immunity from infection vs. vaccination, but I have no idea about their availability.
Not exactly. IgG and IgM are different classes of immunoglobulins (antibodies), produced at different times in response to a foreign antigen (non-self proteins). That antigen can be derived from infection or vaccination.
In theory you could develop an mRNA vaccine for any protein whose structural sequence (amino acid composition) is known.
hasn't the issue been that, prior to the COVID vaccines, they were unable to find a delivery vehicle that would hold up and deliver the package to the intended target? and they found that in the spike protein for these vaccines
They needed a way to deliver mRNA, which encodes proteins. Once the mRNA makes it into cells, proteins are translated. While there may be a size limit for the amount of deliverable mRNA, there's nothing special about spike versus other viral structural proteins, SARS-CoV-2 or otherwise.
That's awesome. Thank you for explaining!
