RE:RE:RE:MTD and the FDA I think you are right safety and toxicity issues are becoming less tolerated by patients, docs and the fda so the bottom end of you're efficacy widow, the furthest from toxicity, is as important as the top end. Certainly looks like you can kill a drugs revenue potential by dosing too high.
scarlet1967 wrote: I think THTX needs to pay close attention to oncopeptid's situation, their PDC commercialization seems to be going nowhere due to the mortality issues. Now they haven't clarified what is the reason for the mortality but it seems to be an element of lack of safety reading between the lines! They seems to have included lower stages of cancers in their other trials now to expand the label for their drug, some are speculating that could be the reason for mortality.
Point is if the safety is due to wider therapeutic window for various stages of cancer then high dose high efficacy approach can backfire later on causing serious issues which can't be reversed during the trial and post potential approval of the drug. So all the speculations to less go higher thus better efficacy to me is a risky approach. Late stage cancer fragil patients shouldn't be exposed to drugs with safety issues, I believe if their PDC shows better safety and even equal efficacy compared to traditional chemotherapy there is an advantage right there.
Wino115 wrote: It could be why they added in a few months to the Phase2 timeline. I think you're right about the advantage of a known toxin. If you have safety all the way to your chosen MTD ( like Kuras Menin-inhibitor) and a wide therapeutic window as THTX has suggested, then maybe you explore high/low dose. The Menin-Inhibitors are new so that's valuable. Docetaxel in tumors is old and they probably know how to use it with low vs high dose like you say. But whatever the FDA works out for TH1902, it shouldn't be throwing a wrench in the works. Add a few more patients to each of the 4 tumors and do a low (or normal taxel equivalent) and MTD. On the other hand, since the normal therapeutic dose of taxel is below where they are, they know a lot about the low dose environment, although not delivered via SORT1.
qwerty22 wrote: Scarlett brought this news to the board about the fda seeking alternatives to MTD.
https://www.fiercebiotech.com/biotech/fda-s-renewed-focus-oncology-dosing-spooks-investors-but-companies-say-they-were-ready It got me thinking about how thtx might handle this (if they had to), I'm not suggesting they have to atm. Anyway it's pretty well known how normal docetaxel accumulates in tumours. You can use that concentration as your target concentration for dosing. So rather than rely on MTD to find the maximum dose based on safety you use a tumour accumulation number to get a dose based on efficacy. You can only do this because you have the long experience of using docetaxel in patients. I'm not saying this is what they'll do, to me it's just another example of how it might help the drug development process to be using an old, well-understood chemo.
Hopefully they get tumour material and are able to measure drug (and released docetaxel) in the tumour. It will be a good number to have for many reasons. If investors were truly spooked by the FDA's shift from MTD, it would be good for thtx to have a pre-prepared solution.