Thank you for the clarification. I mixed up University of Michigan with University of Minnesota.No, Dr. Shore helped @linearb.
The University of Minnesota device helped @kelpiemsp but their lead (Hubert Lim) bailed on the device for Neuromod. Epic-level sellout.
Whoever they are, I hope they burn in hell because of their involvement.So someone faked their audiogram results to get into the trial? Then they were given placebo and showed improvement which was just their real results?
Why on earth? And which hearing aid manufacturer was behind this?
I feel you for sure. The whole day I had the uncomfortably familiar, bed-binding, skyrocketing anxiety and existential emptiness that I felt during the earliest stages of tinnitus. I really don't feel that bad anymore. They just have to smash their severe category and then they could angle for compassionate use. This is a unique challenge that may not go as swimmingly as their Phase 1 results had, but at least there is some consistency with the dosing.We keep praying and praying but today I came to the conclusion that God has hearing loss himself.
Hi Lucifer,I really don't see this happening. Single dose has been more effective with FX-322. It's just how to get FX-322 deeper in the round window whether that is by reformulating or additional doses monthly.
Neuromod is the Irish company behind Lenire, which is the device.Which device is "Neuromod"? Is that the device that became available in Ireland recently that had a disappointing performance? If Neuromod isn't that device, might it be as good as (or identical to) that University of Minnesota device?
No problem. It's 5 am right now so I'm about to go to bed but if I recall correctly, Neuromod's Lenire and Minnesota's respective devices are very dissimilar. Early on there was some hope that Lim's promising research in signal timings could optimize Neuromod's (Ireland) approach, but that didn't come to fruition. Honestly can't remember how Minnesota's device distinguished itself from Shore's, but I remember the two US devices having more commonalities than Neuromod's. Neuromod stimulates the tongue (vagus nerve?) while Shore's stimulated nerves in the neck/jaw.Thank you for the clarification. I mixed up University of Michigan with University of Minnesota.
Which device is "Neuromod"? Is that the device that became available in Ireland recently that had a disappointing performance? If Neuromod isn't that device, might it be as good as (or identical to) that University of Minnesota device?
I have never paid close attention to research on tinnitus cures, as I figured that once something that works becomes available, I will know. So please forgive my lack of knowledge as far as those devices are concerned. It would help a lot to learn the answers to my questions above...
Phase 1/2 showed [statistically significant] signs of functional hearing improvement.Hi Lucifer,
Would you be so kind to tell me how single dose was proven to be effective? I keep reading this on this thread and I feel I must have missed something from the release and the Q&A afterwards. They mentioned they only had positive results from the WR, and that was flawed due to recruiting problems.
My conclusion was that the drug is not effective at all.
I would be really happy if someone would shed some light on this statement of single dose being effective for me.
Right? The placebo improved their hearing. How dumb does that sound to you? It's another clear indication the FDA process has failed.So someone faked their audiogram results to get into the trial? Then they were given placebo and showed improvement which was just their real results?
Why on earth? And which hearing aid manufacturer was behind this?
@Pharz, this is your answer. I like to also add that the reason the multiple dosing of FX-322 might have failed as they quoted about seeding of the lawn and that with successive doses of FX-322 weekly it has affected the regrowing process and it may have been better to try a monthly doses instead.Phase 1/2 showed [statistically significant] signs of functional hearing improvement.
Thank you.The answer is no: not one person in their Phase 2a improved on the audiogram, including extended high frequencies. Furthermore, they apparently ran a parallel new Phase 1/2 trial. Again, not one patient improved on the audiogram, including extended high frequencies. Listen to their webcast from yesterday, last few minutes.
Better yet — just run a tinnitus trial, separate from the others.I say this half jokingly, but they should offer Compassionate Use as a preventative measure from further gaming of future trials. If anything, doesn't this show just how far people are willing to go for some sort of relief?
Agree, unfortunately, it's far away from a robust regenerative effect. It is hard to accept after years of hope.As much as it saddens me the fact is FREQ does not work! The WR and WIN is always going to be a subjective measurement which is why seeing results on the audiogram is so important. We haven't seen any of this even on the EHF. You can argue as much as you want that the audiogram is outdated etc but it is the only accurate measure!
How could anyone know that the got two doses since the data has not been unblinded yet? Am I missing something?They also got only two doses of FX-322.
Audiogram is flawed too. The patient could fake the deficit just like word score, and not click the button when they first hear the tone so it looks like they have a greater loss. It also shows a total of 11 specific frequencies across the 22,000 that most can hear, so isn't that representative. Also, it doesn't test for IHC function. Also, for people with dysacusis/distorted hearing, it produces errors in tone matching. The audiogram hasn't changed since the 40's - how many other medical tests are we still using today that are 80 years old that haven't had some revision?As much as it saddens me the fact is FREQ does not work! The WR and WIN is always going to be a subjective measurement which is why seeing results on the audiogram is so important. We haven't seen any of this even on the EHF. You can argue as much as you want that the audiogram is outdated etc but it is the only accurate measure!
This is what worries me the most, to be honest. What if FX-322 actually regenerates some inner structure (synapses and whatnot) improving subjective conditions (tinnitus, hyperacusis, WR, intelligibility, etc.), but it is shut down because it cannot be proved objectively?Just thinking out loud. If I understood correctly, hidden hearing loss is not shown on audiograms, even at high frequencies. Let's say FX-322 hits and improves that hidden frequency, then that improvement won't show up either on the audiogram even if it's actually happened. Call it "hidden improvement"? But the patient can still benefit from it — see better word score, anecdotal decreased tinnitus, etc. I was let down by the lack of changes in the audiograms, but thinking twice I question if they are any relevant.
I'm not sure if it makes sense at all or maybe I'm just trying to save the unsavable out of despair.
The FDA is a bureaucratic institution that does more harm than good. Case in point.Right? The placebo improved their hearing. How dumb does that sound to you? It's another clear indication the FDA process has failed.
How about SPI-1005?Others will try their candidates but there won't anything on the market in the so called near future.
Many drugs just improve subjective conditions and get approved... consider most anti-depressants, for example.This is what worries me the most, to be honest. What if FX-322 actually regenerates some inner structure (synapses and whatnot) improving subjective conditions (tinnitus, hyperacusis, WR, intelligibility, etc.), but it is shut down because it cannot be proved objectively?
They said that only two of the injections burned when injected. So that's how they knew or thought they only received two of FX-322.I'm confused. How would they know they only got two doses of FX-322 if everyone, including patients, is still blinded at the individual level? You even then say it was an unknown amount.
I've just woken up and all I feel about this process is complete and utter anger because I've realised there's only one of two possibilities: either this drug doesn't do anything in humans and we've all been misled, or a bunch of selfish, desperate people have knowingly lied to get into the trial and potentially ruined the one and only chance for the rest of us to rebuild our lives. I am livid. If you are one those patients and happen to be lurking this forum, I only have two words for you. No prizes for guessing what those words might be.
And someone in the Sound Pharmaceuticals thread is already paying a lab to make this for them now...How about SPI-1005?
I mean, what if FX-322 is killed/shut down (e.g., due to incapacity to objectively prove improvements in audiograms or EHF) before Frequency Therapeutics can conduct specific trials on specific subjective conditions? I feel like FX-322 is hanging by a thread, with Phase 1b serving as the thread. If they can't prove positive results from Phase 1b when the full readout is released in June (for what it is worth, I don't expect the full readout of Phase 2a to show anything meaningful), FX-322 and Frequency Therapeutics may well be doomed...Many drugs just improve subjective conditions and get approved... consider most anti-depressants, for example.
Sounds plausible but I don't think that's enough to make any kind of wider inference, unfortunately. I do recall FX-322 having a stable form of vitamin C in it, so I wonder if that contributes to the burning at all (assuming it was FX-322).They said that only two of the injections burned when injected. So that's how they knew or thought they only received two of FX-322.
This is an interesting thought. I think they didn't know about the Phase 2A that far back. Re-listening to the call this morning, I heard executives that were in the process of pivoting. If they had thought it out more, there would have been a much more controlled presentation with an actual deck, and some deep rationale for the new game plan, and how it would benefit investors + patients. None of that happened. They probably got the results, shit their pants, got back on the phone with the FDA, and came up with the single-dose strategy. This pivoting activity, and the way it was handled with a teleconference call, shows that they're in red-alert right now, and have been for a short period of time. Not to mention, the Q&A was happening in real-fucking-time... if they were in a prepared spin mode... there would have been no Q&A, it would have been polished.Re the additional Phase 1b trials that were announced quite out of the blue if remember correctly - I wonder if these studies were made up quickly due to early indication that Phase 2a was not doing well and Frequency Therapeutics needed something to reinforce original trial results and keep an iron in the fire. I could be misinformed on this so shoot it down if need be.
@FGG, @Zugzug, I didn't know that WR was not an important factor in recruitment in Phase 1/2 and this has given me a bit of hope (how about the Phase 1b trials though?). The next Phase 1b studies will be really interesting, however, still not enough to prove anything even if results appear good unless I'm missing something.
I'm coming to the conclusion that worst case scenario is that the good WR result from the Phase 1/2 & 1b trial were fluke, or bias (which I have slightly more confidence that this is unlikely now), or best case scenario it works but can't be proven with audiogram because likely it is down to something like only IHC regenerate, or both IHC and OHC regenerate but only IHC regenerate functionally.
I need to be re-convinced again that FX-322 even works. Good results from the Phase 1b trials will go a way to doing that but not conclusively.
They should just say fuck it and run another Phase 1b study on the home-bound, bed-bound, pain-ridden, crippled tinnitus and noxacusis sufferers and see if we get our social lives, music, careers, family and friend connections, quality of life back.
Frequency Therapeutics has $200MM cash in the bank, hardly hanging by a thread lol.I mean, what if FX-322 is killed/shut down (e.g., due to incapacity to objectively prove improvements in audiograms or EHF) before Frequency Therapeutics can conduct specific trials on specific subjective conditions? I feel like FX-322 is hanging by a thread, with Phase 1b serving as the thread. If they can't prove positive results from Phase 1b when the full readout is released in June (for what it is worth, I don't expect the full readout of Phase 2a to show anything meaningful), FX-322 and Frequency Therapeutics may well be doomed...