PTI-801 Moving to 14 Day Proof of Concept Study in CF Subjects on Orkambi®
PTI-428 Continues to Enroll 28 Day Proof of Concept Study in CF Subjects on Orkambi®
PTI-808 Investigational New Drug Application Now Active; Phase 1 Study in Healthy Volunteers Initiated
CAMBRIDGE, Mass., July 31, 2017 (GLOBE NEWSWIRE) -- Proteostasis Therapeutics, Inc. (NASDAQ:PTI), a
biopharmaceutical company developing small molecule therapeutics to treat diseases caused by dysfunctional protein processing such
as cystic fibrosis (CF), announced updates across the Company’s later stage development programs in CF, including PTI-428, a cystic
fibrosis transmembrane conductance regulator (CFTR) amplifier, PTI-801, a new generation CFTR corrector, and PTI-808, a CFTR
potentiator.
Proteostasis announced that it has completed dosing of 19 patients as part of the ongoing Phase 1/2 study
designed to evaluate the safety and pharmacokinetics of PTI-428, the Company’s CFTR amplifier. PTI-428 was administered together
with background Orkambi® (lumacaftor/ivacaftor) or as the only CFTR modulator therapy in CF subjects over a 14-day period (7-day
dosing followed by 7-day follow-up period). The trial met its primary safety and pharmacokinetic endpoints, confirming PTI-428’s
safety, tolerability and lack of clinically meaningful drug-drug interaction with ivacaftor and lumacaftor.
“Preliminary data suggests that PTI-428 continues to demonstrate a favorable safety and pharmacokinetic profile,
which has enabled the initiation of Phase 2, enrolling CF subjects on background Orkambi® taking PTI-428 or placebo for 28 days,”
said Meenu Chhabra, President and CEO of Proteostasis Therapeutics. “We continue to make meaningful progress with all three
components of our proprietary triple combination: with the support of US and EU patient advocacy groups for the PTI-801
protocol, we are eligible to begin screening and enrolling CF subjects on background Orkambi® and 40 clinical sites in the US,
Canada and EU have been identified or are in process of activation; enrollment continues in our 28-day study of PTI-428 across 14
active clinical sites in the US, with activation of another 23 sites in both the US and EU in process; and we have initiated a
Phase 1 study of PTI-808 in healthy volunteers.”
In the Phase 1 portion of the PTI-428 study, 11 subjects in the Orkambi® cohort and eight in the PTI-428
monotherapy cohort were enrolled, with each group enrolling 2 placebo subjects. All adverse events (AEs) were mild or
moderate and none occurred in more than one subject. There were no hematology-related adverse events and no serious adverse
events (SAEs) reported. Safety endpoints evaluated included lung function as measured by forced expiratory volume in one
second (FEV1), although the study was not designed to show a statistically significant difference. In the subjects
who received PTI-428 in addition to their background Orkambi, there was no significant improvement of FEV1 compared to
placebo, although there was a numerical increase in FEV1 at day 7. Measurements of sweat chloride and mRNA in
nasal mucosa were used as exploratory biomarkers but the changes were not significant nor correlated with lung function
changes.
Ms. Chhabra added, “While confirming the safety of PTI-428, the phase 1 portion of this study was not expected
to demonstrate efficacy over a 7-day dosing period, as PTI-428, as a CFTR amplifier, is designed to deliver substrate to correctors
and was investigated in combination with Orkambi®, whose signal of efficacy required a 28-day study. As a result, we look
forward to generating data in our 28-day proof-of-concept study to begin understanding the activity profile of PTI-428.”
Proteostasis is enrolling patients in the Phase 2 safety and efficacy portion of the study, which explores PTI-428 dosed over
a 28-day period, and preliminary data is expected in Q4 2017.
Po-Shun Lee, M.D., Executive Vice President, Chief Medical Officer, added: “This is a very exciting time for the
CF community, with the potential of next generation CFTR modulator therapies and combinations just beginning to emerge inclusive of
doublets, triplets and quadruplets. We believe that PTI-428, PTI-801 and PTI-808 have the potential to play a pivotal role in
emerging next generation therapies as proprietary combinations and as add-ons to the evolving standard of care. In fact,
recent clinical data published with triple combinations of CFTR modulators confirms that in vitro assays have high
translational value correlating with improvements in lung function beyond what had been observed to date. This continues to
reinforce the correlation between in vitro chloride transport and FEV1 and further suggests a ceiling on lung
function improvement has not yet been established.”
Proteostasis also announced today that the protocol for the CF portion of its Phase 1/2 study of PTI-801, a new
generation CFTR corrector with Fast Track designation from the FDA, has been endorsed by the Cystic Fibrosis Foundation
Therapeutics Development Network (TDN) Protocol Review Committee and the European Cystic Fibrosis Society Clinical Trial Network
(CTN). Screening of CF subjects for 14-day dosing in this study is in the process of being initiated, with initial data
expected in Q4 2017. A total of 52 healthy volunteers have participated and completed the study. All AEs in the healthy
volunteer portion of the study that have been reported to date were of mild or moderate intensity. No AEs were reported in more
than one subject and no SAEs were reported. PTI-801 was found to be generally well tolerated. Preliminary PK assessments
indicated that PTI-801 was well absorbed following single and multiple oral administrations, and suggest that it could be suitable
for once daily dosing. In vitro studies have shown that the addition of PTI-801 to either a lumacaftor/ivacaftor or
tezacaftor/ivacaftor combination increased the effect of both combinations by approximately three-fold.
The Company also announced today that its Investigational New Drug application with the U.S. Food and Drug
Administration for PTI-808, a CFTR potentiator, is now active and that the Company has initiated a Phase 1 study in healthy
volunteers. If positive efficacy results are achieved in the PTI-428 and PTI-801 programs, Proteostasis intends to initiate a
triple combination study at the end of 2017 with all three agents (also known as PTI-NC-733). The study will explore different
doses of PTI-808 with fixed dose combination of PTI-428 and PTI-801 in an F508del homozygous population who are not taking
Orkambi®.
About Proteostasis Therapeutics, Inc.
Proteostasis Therapeutics, Inc. is a biopharmaceutical company dedicated to the discovery of groundbreaking
therapies to treat diseases caused by dysfunctional protein processing, such as cystic fibrosis (CF). Headquartered in Cambridge,
MA, the Proteostasis Therapeutics team focuses on identifying therapies that restore protein function. In addition to its multiple
programs in cystic fibrosis, Proteostasis Therapeutics has formed a collaboration with Astellas Pharma, Inc. to research and
identify therapies targeting the Unfolded Protein Response (UPR) pathway. For more information, visit www.proteostasis.com.
Safe Harbor
To the extent that statements in this release are not historical facts, they are forward-looking statements
reflecting the current beliefs and expectations of management made pursuant to the safe harbor provisions of the Private Securities
Litigation Reform Act of 1995. Words such as “aim,” “may,” “will,” “expect,” “anticipate,” “estimate,” “intend,” and similar
expressions (as well as other words or expressions referencing future events, conditions or circumstances) are intended to identify
forward-looking statements. Examples of forward-looking statements made in this release include, without limitation,
statements regarding the expected timing of the initiation of, patient enrollment in, data from, and our completion of, our
clinical studies and cohorts for PTI-428, PTI-801, PTI-808 and our triple combination therapy candidate, PTI-NC-733.
Forward-looking statements made in this release involve substantial risks and uncertainties that could cause actual results to
differ materially from those expressed or implied by the forward-looking statements, and we therefore cannot assure you that our
plans, intentions, expectations or strategies will be attained or achieved. Such risks and uncertainties include, without
limitation, the possibility final or future results from our drug candidate trials (including, without limitation, longer duration
studies) do not achieve positive results or are materially and negatively different from or not indicative of the preliminary
results reported in this release, (noting that these results are on a small number of patients and small data set), uncertainties
inherent in the execution and completion of clinical trials (including, without limitation, the possibility FDA requires us to run
cohorts sequentially or conduct additional cohorts or pre-clinical or clinical studies), in the enrollment of CF patients in our
clinical trials, in the timing of availability of trial data, in the results of the clinical trials, in possible adverse events
from our trials, in the actions of regulatory agencies, in endorsement, if any, by therapeutic development arms of CF patient
advocacy groups, and those set forth in our Annual Report on Form 10-K for the year ended December 31, 2016, and our other SEC
filings. We assume no obligation to update or revise any forward-looking statements, whether as a result of new information,
future events or otherwise.
CONTACTS: Investors: David Pitts Argot Partners 212.600.1902 david@argotpartners.com Media: Eliza Schleifstein Argot Partners 973.361.1546 eliza@argotpartners.com