QurAlis' QRA-244 — An Alternative for Retigabine (Trobalt)?

Tezcatlipoca

Tezcatlipoca

Member
Author
Mar 1, 2021
469
#1
Hello! I have been looking into Retigabine. We all know how great it was for tinnitus (with a lot of users' tinnitus lowering to 1/10), however the side effects were many and life threatening, so it was finally discontinued in June 2017.

Now, after looking around, I found this Pharmaceutical Company:

QurAlis

They are an ALS focused biotech developing a Kv 7.2/7.3 ion channel opener optimized for both safety and efficacy as a potential treatment for motor neuron hyperexcitability-induced neurodegeneration in ALS patients.

"QRA-244 a Potent, Selective KCNQ2/3 Opener and a Potential Therapy for Motor System Hyperexcitability induced Disease Progression in ALS Patients," showed that QRA-244 has comparable effects to retigabine (ezogabine) at up to 20-fold lower concentration in motor neurons differentiated from patient-derived iPSCs as measured by an all-optical electrophysiology experiment. Importantly, QRA-244 showed dramatic reductions in side effects associated with retigabine including fatigue/somnolence, dizziness and bladder retention in head-to-head pre-clinical studies."
The full article can be found here:

QurAlis' Selective Kv7 Opener, a Drug Candidate for ALS, Demonstrates up to 20-Fold Increase in Potency and Dramatic Reduction in Side Effects Compared to Retigabine in Preclinical Models
 
#2
Tezcatlipoca said:
Hello! I have been looking into Retigabine. We all know how great it was for tinnitus (with a lot of users' tinnitus lowering to 1/10), however the side effects were many and life threatening, so it was finally discontinued in June 2017.

Now, after looking around, I found this Pharmaceutical Company:

QurAlis

They are an ALS focused biotech developing a Kv 7.2/7.3 ion channel opener optimized for both safety and efficacy as a potential treatment for motor neuron hyperexcitability-induced neurodegeneration in ALS patients.

"QRA-244 a Potent, Selective KCNQ2/3 Opener and a Potential Therapy for Motor System Hyperexcitability induced Disease Progression in ALS Patients," showed that QRA-244 has comparable effects to retigabine (ezogabine) at up to 20-fold lower concentration in motor neurons differentiated from patient-derived iPSCs as measured by an all-optical electrophysiology experiment. Importantly, QRA-244 showed dramatic reductions in side effects associated with retigabine including fatigue/somnolence, dizziness and bladder retention in head-to-head pre-clinical studies."
The full article can be found here:

QurAlis' Selective Kv7 Opener, a Drug Candidate for ALS, Demonstrates up to 20-Fold Increase in Potency and Dramatic Reduction in Side Effects Compared to Retigabine in Preclinical Models
Click to expand...
Great find. Hopefully they will start clinical development soon. I think Xenon is furthest along with their Retigabine reformulations - XEN-496 is now entering Phase 3.
 
#4
Tezcatlipoca said:
Interesting. I remember reading about them but I am not really knowledgeable about their reformulation. Were they able to get rid of the side effects too?
Click to expand...
Yes, their intention with reformulation was to get a safer product without the side effects of the original Retigabine. Although being realistic I am guessing it's not free of side effects but hopefully none that would land them with a black-box warning...
 
#5
serendipity1996 said:
Great find. Hopefully they will start clinical development soon. I think Xenon is furthest along with their Retigabine reformulations - XEN-496 is now entering Phase 3.
Click to expand...
XEN-496 is the same active molecule as Retigabine. XEN-1101 is their newer molecule with reduced side effects.
 
#7
Tezcatlipoca said:
So we can expect the same side effects for XEN-496, but fewer side effects for XEN-1101?
Click to expand...
Probably. XEN-1101 is in Phase 2. Xenon Pharma claimed that no adverse events occurred in Phase 1. I'm not sure if they're looking for the visual snow problems that Retigabine had, it seems like fixing the urinary retention and skin pigmentation were their biggest concerns.

Edit: no serious adverse events, except for somebody who passed out from having their blood drawn :D
 
#8
Croaker said:
Probably. XEN-1101 is in Phase 2. Xenon Pharma claimed that no adverse events occurred in Phase 1. I'm not sure if they're looking for the visual snow problems that Retigabine had, it seems like fixing the urinary retention and skin pigmentation were their biggest concerns.

Edit: no serious adverse events, except for somebody who passed out from having their blood drawn :D
Click to expand...
Oh so it's safe now? That's fantastic!
 
#10
weab00 said:
What is the mechanism of action for channel blockers possibly ameliorating hyperacusis?
Click to expand...
Along with the anecdotes we've got on here, there's this from Dr. Fuchs.

Relevant part of the abstract:

"Here, we show that type II afferents are activated when outer hair cells are damaged. This response depends on both ionotropic (P2X) and metabotropic (P2Y) purinergic receptors, binding ATP released from nearby supporting cells in response to hair cell damage. Selective activation of P2Y receptors increased type II afferent excitability by the closure of KCNQ-type potassium channels, a potential mechanism for the painful hypersensitivity (that we term "noxacusis" to distinguish from hyperacusis without pain) that can accompany hearing loss. Exposure to the KCNQ channel activator retigabine suppressed the type II fiber's response to hair cell damage."​
 
#11
Croaker said:
Along with the anecdotes we've got on here, there's this from Dr. Fuchs.

Relevant part of the abstract:

"Here, we show that type II afferents are activated when outer hair cells are damaged. This response depends on both ionotropic (P2X) and metabotropic (P2Y) purinergic receptors, binding ATP released from nearby supporting cells in response to hair cell damage. Selective activation of P2Y receptors increased type II afferent excitability by the closure of KCNQ-type potassium channels, a potential mechanism for the painful hypersensitivity (that we term "noxacusis" to distinguish from hyperacusis without pain) that can accompany hearing loss. Exposure to the KCNQ channel activator retigabine suppressed the type II fiber's response to hair cell damage."​
Click to expand...
So theoretically, if we can restore OHCs using FX-322, would this stop noxacusis?

If FX-322 doesn't help, how long would we need to take Retigabine for?

Which Retigabine drug is closest to come out in the market?
 
#12
It opens the channels, it doesn't close them. Big difference. It isn't a fast acting inhibitor, more like a threshold setter channel making it more hyperpolarized via K ion slippage.
 
#13
To open the Potassium channels, does it make sense to supplement with Potassium? I think there are some studies which show correlation between high Potassium intake and better ear health, but has it also some effect on the Potassium channels?
 
#14
Lucifer said:
So theoretically, if we can restore OHCs using FX-322, would this stop noxacusis?

If FX-322 doesn't help, how long would we need to take Retigabine for?

Which Retigabine drug is closest to come out in the market?
Click to expand...
My theory and research into this has always suggested yes. Before the Phase 2 readout I was planning on making a post going into further detail as to why but having had the rug pulled from under our feet I can't be bothered now. I know that @100Hz has also been doing some similar research but I'm not at liberty to say much more. OHCs to me are the culprit. I think @FGG has some reservations in that sensitisation may remain even after you've fixed/replaced the OHCs. I'm a little more hopeful about this just from looking at other examples of peripheral-centralised pain as well as from looking at a lot of anecdotal experiences of hyperacusis - many people get better, suggesting then that sensitisation is reversible, at least in some people and to some extent.
 
#15
Which Retigabine drug is closest to coming out in the market?

I had a look at XEN-496 and it's going to take them awhile for them to complete Phase 3. It has a study completion date of December 2022.
 
#16
xyz said:
To open the Potassium channels, does it make sense to supplement with Potassium? I think there are some studies which show correlation between high Potassium intake and better ear health, but has it also some effect on the Potassium channels?
Click to expand...
No. K ions leak from the inside to the outside of the membrane to maintain constant charge delta.

More on the outside will do nothing unless you were deficient.

K channel drugs help to increase the charge differential (hyperpolarization) by opening pores to let K ions slip out of the cell.
Lucifer said:
Which Retigabine drug is closest to coming out in the market?

I had a look at XEN-496 and it's going to take them awhile for them to complete Phase 3. It has a study completion date of December 2022.
Click to expand...
XEN-496 will work. The mechanism is sound as f. Hugs Kv7.1 subunits like white on rice.

XEN-1101 is pretty novel in its shape and mechanism, but same target.
 
#17
Lucifer said:
So theoretically, if we can restore OHCs using FX-322, would this stop noxacusis?

If FX-322 doesn't help, how long would we need to take Retigabine for?

Which Retigabine drug is closest to come out in the market?
Click to expand...
I'm a bit hazy on this, haven't done much on it for a while but the conclusion I came to is that FX-322 could work as long as it either, a) fixed wherever rogue ATP / cytokines etc. were being released from (so if the broken ATP release site was replaced by PCA process then it would fix it but if it was from a gap junction hemi-channel for instance then maybe not as it might not be covered by the scope of PCA), or b) if noxacusis is down to enlarged ribbons then FX-322 could replace the OHCs that have enlarged ribbons but only if they were damaged enough to be flagged for PCA.

What Trobalt's mechanism suggests to me from what I read about it is that it masks, or disables the tinnitus causing mechanism (and I hope the pain causing mechanism as well), and not just that but it seems to do it very consistently in comparison to other meds. FX-322 has much more of unknown factor about it where noxacusis is concerned in my opinion because a) we don't typically have much apparent hearing loss and b) people with loads of hearing loss typically don't have noxacusis.

I believe Xen etc. would need to be taken for life, but hope also (complete speculation this bit) maybe as a preventative measure for when you wanted to do something noisy if it wasn't a requirement to keep it sustained at a constant level in the system.
 
#18
Croaker said:
Along with the anecdotes we've got on here, there's this from Dr. Fuchs.

Relevant part of the abstract:

"Here, we show that type II afferents are activated when outer hair cells are damaged. This response depends on both ionotropic (P2X) and metabotropic (P2Y) purinergic receptors, binding ATP released from nearby supporting cells in response to hair cell damage. Selective activation of P2Y receptors increased type II afferent excitability by the closure of KCNQ-type potassium channels, a potential mechanism for the painful hypersensitivity (that we term "noxacusis" to distinguish from hyperacusis without pain) that can accompany hearing loss. Exposure to the KCNQ channel activator retigabine suppressed the type II fiber's response to hair cell damage."​
Click to expand...
Although I have a very superficial understanding of this matter, I wonder why researchers haven't continued on this particular track of finding a cure to pain hyperacusis. To me, this sounds like the most promising area of a possible hyperacusis treatment, but I could be wrong. Why are there no more studies done on the role of the KNCQ channel in the experience of pain hyperacusis? It has been seven years since the study came out and as far as I know nothing came of it. I seriously do not understand what is taking so long.
100Hz said:
I believe Xen etc. would need to be taken for life
Click to expand...
Why do you think this is so?
 
#19
In addition to my previous post, here is an interesting part of the book 'Hyperacusis and Disorders of Sound Intolerance: Clinical and Research Perspectives', written in 2018:

"In the future, a better understanding of the physiology of type II ANFs, especially regarding their activation in patients who experience sound-induced pain, might facilitate development of new treatments for hyperacusis. However, a better understanding of the physiology, and the development of new drugs, requires an animal model of pain hyperacusis, which is unfortunately not available yet. Nevertheless, the finding that retigabine can block the damage response of type II AN fibers (Liu et al., 2015) provides a promising start for the development of pharmacological interventions, as this drug is already approved for human use. Moreover, if the induction of auditory pain in hyperacusis is at the periphery, then the side-effects of retigabine (and those of any other potential new drug) could be minimized if delivered locally through systems for drug administration to the inner ear, and we might thus see some progress toward clinical trials in the not too distant future" (Fagelson & Baguley, 2018, p. 72).
 
#22
StoneInFocus said:
Moreover, if the induction of auditory pain in hyperacusis is at the periphery, then the side-effects of retigabine (and those of any other potential new drug) could be minimized if delivered locally through systems for drug administration to the inner ear, and we might thus see some progress toward clinical trials in the not too distant future" (Fagelson & Baguley, 2018, p. 72).
Click to expand...
I have very little knowledge of the anatomy of the ear, but I wonder if an intratympanic injection of Retigabine would yield similar results on humans as the application of the substance to the nerve fibers of rats did.

On a side note, would it be possible to get one's hands on some samples of QRA-244 or one of the chemicals developed by Xenon Pharmaceuticals through some sort of early access program?
 
#23
So I've checked their website, QRA-244 is not listed as being currently in the pipeline.

However, the company is developing another Kv7.2/7.3 opener named QRL-101.

The description reads:

"Our lead therapeutic product candidates are QRL-201 and QRL-101. QRL-201 is a first-in-class molecule for the treatment of ALS that aims to restore STMN2 expression in ALS patients and QRL-101 is a first-in-class Kv7 opener for the treatment of ALS that aims to reduce hyperexcitability-induced neurodegeneration."​

I have sent the company an email asking when they expect QRL-101 to enter its clinical phase and whether they've already considered a compassionate use program, this was their response:

"Dear [StoneInFocus],

Thank you for your interest in the QurAlis QRL-101 program. We expect QRL-101 to reach the clinic end of this year or early next year.


As you may know, there are many steps in clinical development and unfortunately, we are still a significant amount of time away from a consideration of a compassionate use program."​
 
#25
Great find. Transformative therapeutics have never been closer to becoming reality. The Kv 7.2 modulator race is on.
 
#26
#29
InNeedOfHelp said:
https://www.iconclinicaltrials.com/

This is where the trial is hosted, they give you money to participate so groups tend to fill up quite fast.
Click to expand...
I didn't see the trial listed on their website, so I contacted the customer service but they couldn't tell me which of their researches corresponded to the one on ClinicalTrials.gov. So it's possible that the trial hasn't been registered on their website yet. Customer service will try to contact the doctor involved with the trial. I will be phoned back.

EDIT: It's not possible to participate in the trial anymore, the group is already full :(.
 
#30
StoneInFocus said:
I didn't see the trial listed on their website, so I contacted the customer service but they couldn't tell me which of their researches corresponded to the one on ClinicalTrials.gov. So it's possible that the trial hasn't been registered on their website yet. Customer service will try to contact the doctor involved with the trial. I will be phoned back.

EDIT: It's not possible to participate in the trial anymore, the group is already full :(.
Click to expand...
I wonder how that went so fast. I guess they have an inner circle of "regulars" who they use for testing all their Phase 1s.

The good news is that the trial is very short, 4 months max and we might expect a Phase 2 very soon this year. This might even come faster to market then the epilepsy drugs as this is for ALS. It might have shorter follow up period and more people joining the trial. ALS kills within years. The amount of ALS specific centers is very limited, I suspect a close connection between clinical trials and the ALS centers. I'm sure they will not have a problem searching for participants for Phase 2, and getting compassionate use out there.
 

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