Zealand Pharma announces positive topline results from 13-week
Phase 1b multiple ascending dose clinical trial with GLP-1/GLP-2
receptor dual agonist dapiglutide
Company announcement – No. 44 / 2024
Zealand Pharma announces positive topline results from
13-week Phase 1b multiple ascending dose clinical trial with
GLP-1/GLP-2 receptor dual agonist dapiglutide
- Placebo-adjusted reductions in body weight of up to a mean of
8.3% with dapiglutide after 13 weekly doses
- Dapiglutide treatment with doses up to 13 mg was assessed to be
safe and well-tolerated with gastrointestinal adverse events
consistent with the profile reported with other incretin-based
therapies
- Higher doses up to 26 mg over a 28-week treatment period are
being evaluated in the ongoing Part 2 of the trial with topline
results expected in the first half of 2025
Copenhagen, Denmark, 9 September
2024 – Zealand Pharma A/S ("Zealand") (Nasdaq: ZEAL),
(CVR-no. 20 04 50 78), a biotechnology company focused on the
discovery and development of innovative peptide-based medicines,
today announces positive topline clinical results from a Phase 1b
multiple ascending dose (MAD) trial, investigating safety,
tolerability, and clinical effects of 13 weeks of dosing with
dapiglutide, a long-acting GLP-1/GLP-2 receptor dual agonist in
development for weight management1.
“We are both excited and very encouraged by these data from this
short-term trial showing substantial and clinically relevant
reductions in body weight. Preliminary data further support that
dapiglutide possesses a differentiated profile based on its unique
dual agonist effects which we expect to translate to a positive
effect on inflammation,” said David Kendall, MD, Chief Medical
Officer of Zealand Pharma. “We are now evaluating the potential use
of higher doses of dapiglutide up to 26 mg over a longer treatment
duration of 28 weeks in Part 2 of this ongoing trial and anticipate
topline results in the first half of 2025. Importantly, today’s
exciting data give us the confidence needed to rapidly progress
dapiglutide into a comprehensive Phase 2b trial in people living
with overweight and obesity planned for initiation in the first
half of 2025.”
In Part 1 of the Phase 1b trial, a total of 54 participants
(~85% male) with a median age of 46 years and a median baseline BMI
of 30.0 kg/m2 were randomized to receive 13 weekly doses
of either dapiglutide or placebo (14:4) within three dose cohorts.
At week 13, the estimated mean body weight had decreased by up to
8.3% on a placebo-corrected basis among participants on dapiglutide
treatment (up to 6.2% mean weight loss on dapiglutide; 2.1% mean
weight gain on placebo)2. No lifestyle modifications,
such as diet or exercise, were included in the trial.
Dapiglutide was assessed to be safe and well-tolerated in Part 1
of the trial, with no severe treatment-emergent adverse events
(TEAEs) and one serious AE, which was deemed not related to the
drug. The most common TEAEs were gastrointestinal (GI), including
nausea and vomiting. Only two participants discontinued treatment
due to AEs, which were related to the GI system (moderate
vomiting). Overall, the number of GI events observed were
consistent with clinical trials of other incretin-based therapies
with a similar, rapid dose escalation scheme. A low number of
participants reported injection site reactions, all of which were
mild. Anti-drug antibodies were observed in 14.3% of participants.
Part 2 of this Phase 1b trial is evaluating higher doses of
dapiglutide up to 26 mg over a 28-week treatment period with
up-titration every fourth week. Zealand expects to report topline
results from Part 2 in the first half of 2025 and present further
details from Part 1 and Part 2 of this Phase 1b trial at a future
scientific congress. The company plans to progress the clinical
development of dapiglutide into a Phase 2b trial in people living
with overweight and obesity, with initiation expected in the first
half of 2025. Also, the company expects to evaluate the potential
of dapiglutide in select obesity-related comorbidities.
About the Phase 1b trial
The Phase 1b trial is a single-center, randomized, double-blind,
placebo-controlled clinical trial in participants with overweight
or obesity (eligible BMI 27.0 to 39.9 kg/m2),
investigating safety, tolerability, pharmacokinetics, and
pharmacodynamics of multiple doses of dapiglutide as subcutaneous
injections using a dose escalation scheme (NCT06000891). The trial
consists of Part 1 and Part 2. Part 1 includes 54 participants in
three cohorts receiving 13 once-weekly doses of dapiglutide or
placebo, with rapid up-titration every second week. Participants
randomized to the highest dose cohort (13 mg) received
the target dose for a period of 5 weeks. Part 2 of the trial
includes 30 participants receiving 28 once-weekly doses of
dapiglutide or placebo within one dose cohort, with up-titration
every fourth week. Participants will receive the target dose of 26
mg for a period of 4 weeks. No lifestyle modifications, such as
diet or exercise, are included in the trial.
About dapiglutide
Dapiglutide is a long-acting, dual GLP-1/GLP-2 receptor agonist for
the potential treatment of overweight and obesity. This is a
first-in-class peptide designed to leverage the weight loss effects
of a potent GLP-1 agonist and address co-morbidities associated
with low-grade inflammation through improved intestinal barrier
function by GLP-2.
Previous Phase 1 results of dapiglutide in healthy volunteers
demonstrated dose-dependent weight loss of up to 4.3% from baseline
body weight after four weeks of treatment (NCT04612517).
Dapiglutide also delayed gastric emptying and reduced plasma
glucose and insulin concentrations in a dose-dependent manner.
Pharmacokinetics showed a mean half-life of 123-129 hours across
the four dose cohorts, which supports once-weekly dose
administration. Multiple weekly doses of dapiglutide were
well-tolerated and the safety profile was as expected for GLP-1 and
GLP-2 receptor agonists. These results were presented at the ADA
82nd Scientific Sessions in June 2022.
About obesity and low-grade inflammation
Obesity is a chronic disease that results in substantial global
morbidity and mortality. Excess fat storage associated with obesity
can trigger low-grade systemic inflammation through reduced
intestinal barrier integrity, or “leaky gut”. Obesity-related
low-grade inflammation may result in several comorbidities,
including cardiovascular disease, liver disease, inflammatory bowel
disease, and neuro-inflammation.
About Zealand Pharma
Zealand Pharma A/S (Nasdaq: ZEAL) ("Zealand") is a biotechnology
company focused on the discovery and development of peptide-based
medicines. More than 10 drug candidates invented by Zealand have
advanced into clinical development, of which two have reached the
market and three candidates are in late-stage development. The
company has development partnerships with a number of pharma
companies as well as commercial partnerships for its marketed
products.
Zealand was founded in 1998 and is headquartered in Copenhagen,
Denmark, with a presence in the U.S. For more information about
Zealand, please visit www.zealandpharma.com.
Forward-looking statements
This company announcement contains forward-looking statements that
provide Zealand Pharma’s expectations or forecasts of future events
regarding the research, development and commercialization of
pharmaceutical products. These forward-looking statements may be
identified by words such as “aim,” “anticipate,” “believe,”
“could,” “estimate,” “expect,” “forecast,” “goal,” “intend,” “may,”
“plan,” “possible,” “potential,” “will,” “would” and other words
and terms of similar meaning. You should not place undue reliance
on these statements, or the scientific data presented. The reader
is cautioned not to rely on these forward-looking statements. Such
forward-looking statements are subject to risks, uncertainties and
inaccurate assumptions, which may cause actual results to differ
materially from expectations set forth herein and may cause any or
all of such forward-looking statements to be incorrect, and which
include, but are not limited to, the occurrence of adverse safety
events; risks of unexpected costs or delays; unexpected concerns
that may arise from additional data, analysis or results obtained
during clinical trials; failure to protect and enforce our data,
intellectual property and other proprietary rights and
uncertainties relating to intellectual property claims and
challenges; regulatory authorities may require additional
information or further studies, or may fail to approve or may delay
approval of our drug candidates or expansion of product labelling;
failure to obtain regulatory approvals in other jurisdictions; and
product liability claims. If any or all of such forward-looking
statements prove to be incorrect, our actual results could differ
materially and adversely from those anticipated or implied by such
statements. The foregoing sets forth many, but not all, of the
factors that could cause actual results to differ from our
expectations in any forward-looking statement. All such
forward-looking statements speak only as of the date of this
company announcement and are based on information available to
Zealand Pharma as of the date of this announcement. We do not
undertake to update any of these forward-looking statements to
reflect events or circumstances that occur after the date hereof.
Information concerning pharmaceuticals (including compounds under
development) contained within this material is not intended as
advertising or medical advice.
Contacts:
Adam Lange (Investors)
Investor Relations Officer
Zealand Pharma
alange@zealandpharma.com
Anna Krassowska (Investors and Media)
Vice President, Investor Relations & Corporate
Communications
Zealand Pharma
akrassowska@zealandpharma.com
Sources
1ClinicalTrials.gov. A Trial Assessing Safety,
Tolerability, Pharmacokinetics and Pharmacodynamics of ZP7570.
Available at https://clinicaltrials.gov/study/NCT06000891. Last
accessed September 2024.
2Hypothetical estimand = treatment effect if all
participants adhered to treatment (also known as the efficacy
estimand).
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