lokibear0803• in reply toTall_Allen4 years ago

Thanks TA!

lokibear0803• in reply toGP244 years ago

Fantastic, thanks GP24.

OK, so Tall_Allen is suggesting the effect is to at first temporarily increase, but then decrease, PSMA expression/sensitivity.

The PSMAddition trial NCT04720157 allows up to 45 days of CYP17 or ARDT, by which I assume CYP17 = abiraterone and ARDT = either abiraterone or enzalutamide. This would be consistent with the presumed initial increase followed by a decrease in PSMA expression after some period of time…am I right so far?

Do we have a sense of just how long the enhancement would last before onset of PSMA expression decrease?

However the ASCO article from @GP24 excludes prior ENZ but not prior ABI. Then it must be that the trial referenced in the ASCO article has a different hypothesis: prior ABI will NOT reduce PSMA expression after time, while ENZ does (since they want no prior ENZ). Am I interpreting this part correctly?

Many thanks.

lokibear0803• in reply toGP244 years ago

Again, fantastic information, GP24 . I thank you very much.

Then the Emmett prospective comes close to what I’m trying to get to: the salivary glands showed no change from baseline regardless of androgen blockade (AB), while the PC lesions did show reduction in PSMA.

So, I (mistakenly?) generalize this from the salivary glands to other PSMA-expressing areas: although saliva glands, liver, kidney, brain, and etc. express PSMA, they do not show PSMA reduction with ADT…probably because they do not rely on androgens as do PC tumors.

If you believe I’m misreading, please let me know. Can’t thank you enough for those very useful links.