Join today and have your say! It’s FREE!

Become a member today, It's free!

We will not release or resell your information to third parties without your permission.
Please Try Again
{{ error }}
By providing my email, I consent to receiving investment related electronic messages from Stockhouse.

or

Sign In

Please Try Again
{{ error }}
Password Hint : {{passwordHint}}
Forgot Password?

or

Please Try Again {{ error }}

Send my password

SUCCESS
An email was sent with password retrieval instructions. Please go to the link in the email message to retrieve your password.

Become a member today, It's free!

We will not release or resell your information to third parties without your permission.
Quote  |  Bullboard  |  News  |  Opinion  |  Profile  |  Peers  |  Filings  |  Financials  |  Options  |  Price History  |  Ratios  |  Ownership  |  Insiders  |  Valuation

Theratechnologies Inc T.TH

Alternate Symbol(s):  THTX

Theratechnologies Inc. is a Canada-based clinical-stage biopharmaceutical company. The Company is focused on the development and commercialization of therapies addressing unmet medical needs. It markets prescription products for people with human immunodeficiency viruses (HIV) in the United States. The Company's research pipeline focuses on specialized therapies addressing unmet medical needs in HIV, nonalcoholic steatohepatitis (NASH) and oncology. Its medicines include Trogarzo and EGRIFTA SV (tesamorelin for injection). Trogarzo (ibalizumab-uiyk) injection is a long-acting monoclonal antibody which binds to domain 2 of the CD4 T cell receptors. EGRIFTA SV (tesamorelin for injection) is approved in the United States for the reduction of excess abdominal fat in people with HIV who have lipodystrophy. Its portfolio includes Phase I clinical trial of sudocetaxel zendusortide (TH1902), a novel peptide-drug conjugate (PDC), in patients with advanced ovarian cancer.


TSX:TH - Post by User

Post by SPCEO1on Sep 17, 2021 12:51pm
178 Views
Post# 33877950

Cancer Trial Status

Cancer Trial StatusI wish the company would be a bit more forthcoming on the status of the phase 1a but we can do our best to infer where things are at despite that. This entails assumptions and that means we can be off the mark by a decent amount due to incorrect assumptions. But some on this board may have the knowledge to help hone those assumptions.

Here are a couple of assumptions:

1.) THTX would have to inform us if the trial was halted as that would be viewed as a material event.

2.) If two patients had toxic reactions, the trial would stop moving to higher dose level and a new group of patients would be treated at the lower dose to make sure they did not have toxicity at the lower dose level to confirm the previous result. But apparently, there are also appeal methods regarding whether or not what was judged to be toxicity was actually toxic for the patient. If TH pursued such an appeal process, let's assume the process takes three weeks.

So, since we have not been informed that the trial has stopped, we can pretty much assume it was ongoing at the end of August (three weeks ago assuming a three week appeal process and a notification that the trial was halted tomorrow). If so, and assuming there were not any signiifcant wiggles in the trial's progress earlier, then can we feel confident that patients have received a dosage level that is pretty high without a toxic reaction through the latter part of August? 

Clearly, the more Docetaxel that can be pushed into a cancerous cell, the better the potential ouotcome on the efficacy front. In the case of TH-1902, what I am hoping for is not only some efficacy on those phase 1a patients who presented with sortilin overexpressing tumors (hopefully 2/3rds of them) but also no neutropinia so that the combination of efficacy and the length of time treatment can be pursued is better than any other treatment alternative.

Also, another question for the science team - for those patients in the phase 1a who do not have sortilin overexpressing tumors, I assume the PDC washes out through their system without causing any harm. Is that correct? Or would some of the Docetaxel still negatively impact healthy cells if it could not find any sortilin receptor to adhere to? Also, since we are now at higher dose levels, could the non-sortilin expressing tumor patients be facing some nasty side-effects since there likely are some sortilin receptors on healthy cells since the heavier Docetaxel doses are potentially putting more sortilin into healthy cells? Could that lead to the trial being stopped? 

Sorry in advance for all the assumptions, questions and general lack of knowledge (or ability to fully remember when these things were addressed previously).

It seems to me that the stock should logically creep upward every day that w e do not have an indication that the trial has stopped as the chances for success are likely improved with each passing day. 
<< Previous
Bullboard Posts
Next >>