Wow, I hadn't realized how intensely they blind the studies involved!
This is the first trial I've ever encountered with quadruple blinding (participant, care provider, investigator, and even the outcomes assessor).
I've literally never encountered this in my time before, most trials stick to single or double blind (participant or participant + care provider).
This is extremely legit. They are really going all out to ensure no accusations of bias can occur nor will any bias actually mess with the trial.
Btw I forgot to add one even bigger factor that is incredible about this company's progress. We got hit by COVID-19 over the last 12 months and yet the company was only delayed 6 months on their day 90 readout (I think it was originally slated for September and it's now March).
I'm so glad to be a part of this movement and effort!
Here are my guesses for trial outcomes.
Primary Endpoints:
WR quiet: statistically significant improvement, 15-40% absolute improvement. Most obvious endpoint to succeed and with large magnitude in my opinion.
WR noise: potentially statistically significant, 10-15% absolute improvement. Second most likely endpoint to succeed in primary. However, I'm unsure if we will get low frequency penetration to resolve hair cell loss there or if synaptopathy issues are unaffected by drug. EHF should still benefit this endpoint but unsure statistical significance.
Standard audiometry: likely limited improvement here, depends how good drug penetration is especially with repeat dosing, likely 6-8 kHz improvement ranges at best since we did see in patent data that some patients saw improvement at 6 kHz-8 kHz on audiometry indicating drug penetration is possible here. However, if repeat dosing improves penetration deeper than I will be very excited to see the full potential.
Safety: No major adverse events, transient minor events.
Secondary Endpoints:
EHF audiometry: statistically significant improvements. 8 kHz-16 kHz.
TFI improvement: statistically significant dependent on how balanced populations are. Generally expecting improvement, unclear what magnitude or p value to expect.
QoL: statistically significant major improvements anticipated.
Generally unclear how repeat dosing changes things, like penetration of drug beyond 8 kHz-6 kHz and how it enhances WR/TFI/Audiometry.
This week will feel so slow til we have data in hand.
Yeah I meant to mention that to you in our chats. Carl LeBel has made a big point about blinding themselves at all levels for the exact reasons you have suggested. And yes, we were all gutted about COVID-19 pushing things back but all credit to them. Just to think that if this readout is good, had it not been for COVID-19, we would have gone from Phase 1 to Phase 3 in less than 5 years.
As for your predictions, I get the feeling you are edging on the conservative side of things. I know it was a small sample, but if you take the average WR scores of the responders' improvement over baseline, you get an average improvement of 62.5%! I'm not sure if your average was for all patients, but if it was for just responders I'd be inclined to say at least 50%. So anyway, here are mine:
Primary Endpoints:
WR: statistically significant improvement, 20-50% absolute improvement in "responders". Strongly agree with you that this is the most obvious primary endpoint to succeed.
WIN: There's obviously a bit of a question mark here as I think we all know this will largely come down to how much synaptic recovery there is in each patient. I'm also expecting minor WIN improvements in all categories along a similar percentage with statistically significant and clinically meaningful improvements at least in the x4 cohort, especially in the severe category which I suspect will have the most synaptic loss.
Standard Audiogram: given the highly selective criteria this time, I think we will definitely see statistically significant results at 8 kHz and possibly 6 kHz, at least in the higher dose cohorts, especially in the mild category if the "absorption" theory holds any weight. I don't think Frequency Therapeutics would be doing multiple doses unless this was informed from somewhere that this really could help. I suspect they may have done some further undisclosed preclinical work. If the drug does penetrate deeper, I would be pleasantly surprised if we got benefits all the way down to 4 kHz.
Safety: no major events, although
@FGG's point about links between VPA and dormant herpes viruses has me slightly on edge.
Secondary Endpoints:
EHF Audiometry: I think this will be the endpoint that knocks all others out the park, which is a shame, because it's only a secondary endpoint. I expect to see statistically significant improvements in all groups and a strong relationship between frequency and relative gain. I'm expecting exponential gains in the higher dose cohorts, with an average of 30-40 dB gain at 16 kHz in the x4 cohort for the moderate to severe categories.
TFI Improvement: I don't want to make any predictions here given the subjectivity of tinnitus, but I think this could be a real easter egg. Let's wait and see.
QoL: statistically significant major improvements anticipated as well.
Oh guys, by the way, today is 3/22...
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