V.R.T.
Senior Member (Voting Rights)
I asked this question in the BTN2A1/2 thread but don't want to keep clogging that thread up. So ill quote some of the things I said there here:
Would such a study struggle to get funded now? If so, what would convince funders? Would pharma companies be on board? etc
Perhaps it is still a little early for this, perhaps not, but I thought it might be good to discuss if it is time and what these trials might look like. Even if it isn't, if and when more evidence comes from the genetics or elsewhere, we can have an idea of what well designed T cell drug trials would look like, what the pitfalls and dangers might be, and who we would want running them.
So what kind of experiments could get us from this point to a point where we understand more specifics about a potential gdT cell mechinism?
Also, if the issue is BTN2A1 mediated T cell pathology, could this kind of monoclonal antibody be a potential drug? I can only see it being used in lab experiments so I assume there isn't an approved drug form yet.
Again, the gdT conundrum and the broader T cell hypothesis all seems quite similar to the B cell/autoantibody situation, where there are a lot of theories and a lot of things that you'd expect to see that we don't, and a lot of possibilities that would be hard to prove through the basic science.
With the B cells there has been ritux, dara, cyclo and there will be isa and uplinza soon. It seems like there should be equivalent trials exploring T cell hypotheses...
Absolutely!
There does seem to be a lot of evidence and hypothesising possibly implicating various kinds of T cells and yet we've had no T cell clinical trials, and a good few B cell/antibody ones, and I'm not sure the evidence for B cells is any stronger than T cells.
In a manner analogous to ritux/dara for a general and specific approach to B cells and then LLPCs, perhaps there could be a pilot looking at something like Campath that is more general and another looking at the monoclonal that specifically targets gamma delta T cells.Are there any physician researchers who would have experience giving T cell drugs in the way Fluge and Mella have for B cell drugs?
Would such a study struggle to get funded now? If so, what would convince funders? Would pharma companies be on board? etc
Perhaps it is still a little early for this, perhaps not, but I thought it might be good to discuss if it is time and what these trials might look like. Even if it isn't, if and when more evidence comes from the genetics or elsewhere, we can have an idea of what well designed T cell drug trials would look like, what the pitfalls and dangers might be, and who we would want running them.
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