– PGN-EDO51 at 5 mg/kg was well tolerated, and
all patients continued to long-term extension portion of trial.
Dosing of second cohort at 10 mg/kg is ongoing –
– Four doses of PGN-EDO51 at 5 mg/kg achieved
mean exon skipping levels of 2.15% after three months of dosing
–
– PGN-EDO51 at 5 mg/kg showed mean
muscle-adjusted dystrophin level of 1.49%, a 0.70% increase from
baseline, after three months of dosing –
– PGN-EDO51 at 5 mg/kg showed mean absolute
dystrophin level of 0.61%, a 0.26% increase from baseline, after
three months of dosing –
– Conference call scheduled for 4:30 p.m. ET
–
PepGen Inc. (Nasdaq: PEPG), a clinical-stage biotechnology
company advancing the next generation of oligonucleotide therapies
with the goal of transforming the treatment of severe neuromuscular
and neurological diseases, today announced positive clinical data
from the first dose cohort (5 mg/kg) of PGN-EDO51, its lead
investigational candidate for patients with Duchenne muscular
dystrophy (DMD) whose mutations are amenable to an exon 51-skipping
approach. In the ongoing CONNECT1-EDO51 Phase 2 open-label trial,
PGN-EDO51 demonstrated higher levels of exon skipping than
previously reported studies with other oligonucleotide therapies at
similar PMO dose levels in DMD patients. The Company also reported
that change from baseline in total dystrophin production and
muscle-adjusted dystrophin production was comparable to, or higher
than, previously reported studies with other oligonucleotide
therapies at similar PMO dose levels in DMD patients. Today at 4:30
p.m. ET, the Company will host a conference call with the CONNECT1
lead investigator Dr. Hugh McMillan to discuss the data being
presented.
“We are encouraged by the early data from our CONNECT1 clinical
trial of PGN-EDO51 in people with DMD. In three months, the
starting monthly dose of 5 mg/kg achieved high levels of exon
skipping and all patients showed increases in dystrophin. PGN-EDO51
produced meaningfully higher levels of exon skipped transcript at
lower doses and in a shorter time period compared to other exon 51
therapies, approved and in development, indicating that our
Enhanced Delivery Oligonucleotide technology is delivering higher
levels of oligonucleotide to the nuclei,” said James McArthur,
Ph.D., President and CEO of PepGen. “Importantly, PGN-EDO51 has
demonstrated a favorable safety profile, supporting our ongoing
evaluation of the 10 mg/kg monthly dose cohort in CONNECT1. We
intend to leverage the early observations from CONNECT1 to optimize
our CONNECT2-EDO51 Phase 2 trial. Based on these initial results,
we are optimistic about the possibility that higher levels of
dystrophin production will be observed in the 10 mg/kg cohort of
CONNECT1. We also look forward to reporting data from the first
cohort of our placebo-controlled multinational study CONNECT2.”
“People with DMD and their families constantly hope for
effective therapies with the potential to change the course of this
relentlessly progressive neuromuscular disease. I was pleased to
see that the 5 mg/kg dose was well tolerated and that all three
participants demonstrated an increase in dystrophin production and
exon skipping after only three months of treatment with PGN-EDO51.
I look forward to seeing the results of exon skipping and
dystrophin production at 10 mg/kg in both CONNECT1 and CONNECT2,”
said Dr. Hugh McMillan, Pediatric Neurologist at the Children’s
Hospital of Eastern Ontario, and Professor in the Department of
Pediatrics at the University of Ottawa.
CONNECT1 Results for the 5 mg/kg Starting Dose Cohort
(n=3)
Exon 51 Skipping and Dystrophin Production Data
- Exon 51 Skipping: PGN-EDO51 produced mean exon skipping
in biceps tissue of 2.15% at week 13 compared to baseline. Compared
to a receptor mediated delivery technology which delivered
comparable levels, on a per-dose basis, of oligonucleotide to
muscle tissue, we believe the levels of exon skipping generated by
PGN-EDO51 at 5 mg/kg suggest PGN-EDO51 has the potential to be
considerably more potent.1
- Dystrophin Production
- PGN-EDO51 achieved a mean muscle-adjusted dystrophin level of
1.49% of normal and a 0.70% change from baseline after 4 doses,
measured at week 13.
- PGN-EDO51 achieved a mean absolute dystrophin level of 0.61% of
normal and a 0.26% change from baseline after 4 doses, measured at
week 13 by Western blot analysis.
Safety and Tolerability Data
The 5 mg/kg dose of PGN-EDO51 was well tolerated by all study
cohort participants through week 13. There were no
discontinuations, dose interruptions or dose reductions.
- The one related treatment-emergent adverse event was mild and
resolved.
- There was no sustained elevation in kidney biomarkers. There
were no cases of hypomagnesemia or hypokalemia. There were also no
changes in electrolytes or hepatic function and no cases of anemia
or thrombocytopenia.
- All three patients in this cohort are continuing to be dosed
with PGN-EDO51 at 5 mg/kg in the long-term extension (LTE) phase of
the clinical trial. PGN-EDO51 continues to be well tolerated during
the LTE as of July 29, 2024.
The Company plans to present additional results from the 5 mg/kg
cohort at a medical meeting later in the year.
Update on PGN-EDO51 10 mg/kg Cohort As of July 29, 2024,
two participants have received a total of four doses at 10 mg/kg in
the ongoing CONNECT1 study. To date, PGN-EDO51 has been generally
well tolerated at this dose level and the Company expects to report
initial results from the 10 mg/kg cohort in early 2025.
Update on CONNECT2-EDO51 Clinical Trial Based on the data
from CONNECT1, including PGN-EDO51’s emerging safety profile to
date, the Company is working to optimize the design of the CONNECT2
Phase 2 double-blind, placebo-controlled 25-week multinational
trial. The CONNECT2 clinical trial is open in the United Kingdom.
The Company continues to engage with regulators in the European
Union and expects to open the clinical trial in the United States
by year-end.
Conference Call Details PepGen will host a conference
call and webcast today at 4:30 p.m. ET to review the data being
presented. To access the call, please dial (866) 400-0049 and
provide the Conference ID 9666330. A live webcast of the
presentation will be available on the Events & Presentations
section of the PepGen investor website, investors.pepgen.com.
About PGN-EDO51 PGN-EDO51, PepGen's lead clinical
candidate for the treatment of Duchenne muscular dystrophy (DMD),
utilizes the Company's proprietary Enhanced Delivery
Oligonucleotide (EDO) technology to deliver a therapeutic
phosphorodiamidate morpholino oligomer (PMO) that is designed to
target the root cause of this devastating disease. PGN-EDO51 is
designed to skip exon 51 of the dystrophin transcript, an
established therapeutic target for approximately 13% of DMD
patients, thereby aiming to restore the open reading frame and
enabling the production of a truncated, yet functional dystrophin
protein. The U.S. Food and Drug Administration has granted
PGN-EDO51 both Orphan Drug and Rare Pediatric Disease Designations
for the treatment of patients with DMD amenable to an exon-51
skipping approach.
About the CONNECT Clinical Program CONNECT1-EDO51 is an
open-label, multiple ascending dose Phase 2 trial designed to
evaluate PGN-EDO51 at up to three different dose levels starting
with 5 mg/kg administered intravenously once every four weeks for
12 weeks in patients with DMD amenable to an exon 51-skipping
approach. The key endpoints for this trial are safety, dystrophin
production and exon skipping. Multiple pharmacokinetic parameters
are also being assessed as part of the trial protocol.
CONNECT2-EDO51 is a double-blind, placebo-controlled, multiple
ascending dose, multinational Phase 2 trial designed to evaluate
PGN-EDO51 at up to three different dose levels intravenously once
every four weeks for 24 weeks in patients with DMD amenable to an
exon 51-skipping approach. Endpoints included in this trial are
safety, dystrophin production, exon skipping and clinical
assessments of mobility, pulmonary function and quality of
life.
About Duchenne Muscular Dystrophy (DMD) DMD is an
X-linked recessive muscle-wasting disease that predominantly
affects males. This progressively debilitating and fatal disease is
caused by genetic mutations in the gene encoding dystrophin, a
protein critical for healthy muscle function, and is one of the
most prevalent rare genetic diseases, with an incidence rate of
approximately one in every 3,500 to 5,000 male births. DMD is
characterized by progressive muscle weakness, which leads to
patients losing the ability to walk, a loss of upper body function,
cardiac issues and difficulties breathing. DMD is invariably fatal
by young adulthood. Despite significant advances in treatments for
this devastating disease, current exon skipping therapies are
limited by poor delivery to muscle tissue nuclei and have yet to
establish meaningful clinical benefit for DMD patients.
About PepGen PepGen Inc. is a clinical-stage
biotechnology company advancing the next-generation of
oligonucleotide therapies with the goal of transforming the
treatment of severe neuromuscular and neurological diseases.
PepGen’s Enhanced Delivery Oligonucleotide (EDO) platform is
founded on over a decade of research and development and leverages
cell-penetrating peptides to improve the uptake and activity of
conjugated oligonucleotide therapeutics. Using these EDO peptides,
we are generating a pipeline of oligonucleotide therapeutic
candidates designed to target the root cause of serious
diseases.
For more information, please visit www.pepgen.com. Follow PepGen
on LinkedIn and X.
Forward-Looking Statements This press release contains
forward-looking statements within the meaning of the Private
Securities Litigation Reform Act of 1995, as amended. These
statements may be identified by words such as “aims,”
“anticipates,” “believes,” “could,” “estimates,” “expects,”
“forecasts,” “goal,” “intends,” “may,” “plans,” “possible,”
“potential,” “seeks,” “will,” and variations of these words or
similar expressions that are intended to identify forward-looking
statements. Any such statements in this press release that are not
statements of historical fact may be deemed to be forward-looking
statements. These forward-looking statements include, without
limitation, statements regarding the therapeutic potential and
safety profile of PGN-EDO51 based on early data, the potential of
our EDO platform to deliver higher levels of oligonucleotide to the
nuclei, our expectations regarding the potential for increased
levels of exon skipping and dystrophin production following dosing
at 10 mg/kg with a longer treatment period, the design, initiation
and conduct of clinical trials, including expected timelines for
our CONNECT2 Phase 2 trial, the expected timing for additional data
reports from our CONNECT1 trial, and ongoing and planned regulatory
interactions.
Any forward-looking statements in this press release are based
on current expectations, estimates and projections only as of the
date of this release and are subject to a number of risks and
uncertainties that could cause actual results to differ materially
and adversely from those set forth in or implied by such
forward-looking statements. These risks and uncertainties include,
but are not limited to risks related to: delays or failure to
successfully initiate or complete our ongoing and planned
development activities for our product candidates, including
PGN-EDO51; our ability to enroll patients in our clinical trials,
including CONNECT1-EDO51 and CONNECT2-EDO51; that our
interpretation of clinical and preclinical study results may be
incorrect, or that we may not observe the levels of therapeutic
activity in clinical testing that we anticipate based on prior
clinical or preclinical results; our product candidates, including
PGN-EDO51, may not be safe and effective or otherwise demonstrate
safety and efficacy in our clinical trials; adverse outcomes from
our regulatory interactions, including delays in regulatory review,
clearance to proceed or approval by regulatory authorities with
respect to our programs, including clearance to commence planned
clinical studies of our product candidates, or other regulatory
feedback requiring modifications to our development programs,
including in each case with respect to our CONNECT1-EDO51 and
CONNECT2-EDO51 programs; changes in regulatory framework that are
out of our control; unexpected increases in the expenses associated
with our development activities or other events that adversely
impact our financial resources and cash runway; and our dependence
on third parties for some or all aspects of our product
manufacturing, research and preclinical and clinical testing.
Additional risks concerning PepGen’s programs and operations are
described in our most recent annual report on Form 10-K and
quarterly report on Form 10-Q that are filed with the SEC. PepGen
explicitly disclaims any obligation to update any forward-looking
statements except to the extent required by law.
- DYNE-251 DELIVER clinical data update, May 20, 2024
View source
version on businesswire.com: https://www.businesswire.com/news/home/20240730713512/en/
Investors Dave Borah, CFA
SVP, Investor Relations and Corporate Communications
dborah@pepgen.com
Media Julia Deutsch Lyra
Strategic Advisory Jdeutsch@lyraadvisory.com
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