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Antibe Therapeutics Inc(Pre-Merger) ATBPF

Antibe Therapeutics Inc. is a clinical-stage biotechnology company. The Company is leveraging its hydrogen sulfide (H2S) platform to develop therapies to target inflammation arising from a range of medical conditions. The Company’s pipeline includes assets that seek to overcome the gastrointestinal ulcers and bleeding associated with nonsteroidal anti-inflammatory drugs (NSAIDs). Its lead drug, otenaproxesul, is in clinical development as an alternative to opioids and NSAIDs for acute pain. Its second pipeline drug, ATB-352, is being developed for a specialized pain indication. The Company also focuses on inflammatory bowel disease (IBD). Otenaproxesul combines a moiety that releases hydrogen sulfide with naproxen, a non-steroidal, anti-inflammatory drug. ATB-352 is an H2S-releasing derivative of ketoprofen, a potent NSAID commonly prescribed for acute pain. Its IBD candidates are being designed to maintain the efficacy, safety, and pharmacokinetic properties of ATB-429.


GREY:ATBPF - Post by User

Comment by Wriggleson Nov 04, 2022 2:08am
249 Views
Post# 35072034

RE:RE:There we are ...

RE:RE:There we are ...
https://www.fda.gov/regulatory-information/search-fda-guidance-documents/development-non-opioid-analgesics-acute-pain-draft-guidance-industry
 
Fully agree with that.  I would add that enhanced dissolution could possibly allow maintenance doses for chronic to be achieved with smaller but more frequent dosing.  Chronic is still a risk management issue IMO.
 
I think that the new formulation solves the poor solubility issue, which is important in an acute pain setting.  Perhaps what is more important is that the new formulation provides a second argument for a new Oten Patent (new composition).  Extended IP is taking on increasing relevance as the clock ticks IMO.  This by itself could justify the change in approach.   
 
There is an interesting discussion paper at link. Well worth a read if you haven't already done so.  It gives the FDA's evolving thoughts on acute pain trials, opioid sparing and expedited review.  It provides some guidance for selecting primary/secondary endpoints during trials and some considerations when seeking enhanced labeling for opioid sparing. A backdrop for future Oten acute development.
 


TriumphSpitSix wrote: "Just wish we really understood what "significant dose reduction" meant and how it affects Acute and Chronic drug development.  Acute is easy to understand but how the dose reduction affects a Chronic plan is anyone's guess."

Not a doctor or chemist but from reading the NR, I believe it is primarily related to an increase in "bioavailability" i.e., how much of the drug actually enters circulation within the body and is then available to reduce pain, inflammation, etc... Presumably, higher bioavailability would allow them to decrease the doses in both Chronic and Acute applications since more of the drug is actually utilized instead of being flushed out of the body.

Hopefully, lowering the dose would address the "elevated LTEs" which doomed the Ph.2 chronic study.

Maybe they combined it with something else or found a way to treat it to make it more soluble? Dunno, just thinking out loud...


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