Arecor Therapeutics
plc
("Arecor", the "Company" or the "Group")
ARECOR PRESENTS POSITIVE DATA
FROM PHASE I CLINICAL TRIAL OF ULTRA-CONCENTRATED ULTRA-RAPID
ACTING INSULIN AT278 IN OVERWEIGHT AND OBESE PEOPLE WITH TYPE 2
DIABETES IN LATE-BREAKING ORAL PRESENTATION AT EASD
2024
- AT278 delivers significantly
accelerated early PK/PD profile compared with
NovoRapid® in people with Type 2
Diabetes and high BMI
- Results confirm previous
findings in people with Type 1 diabetes and show that AT278 can
maintain the faster action profile irrespective of diabetes type
and BMI
- Critical enabler in
development of miniaturised next-generation insulin
pumps
- Favourable safety profile
with no safety signals detected
Cambridge, UK, 11 September 2024:
Arecor Therapeutics plc (AIM: AREC), the biopharmaceutical group
advancing today's therapies to enable healthier lives,
today presents positive results from its
Phase I clinical trial of the ultra-concentrated, ultra-rapid
acting insulin candidate, AT278, in Type 2 diabetics with a high
body mass index (BMI), at the 60th Annual
Meeting of the European Association for the Study of Diabetes
(EASD) in
Madrid.
AT278 (500 U/mL) is an ultra-concentrated,
ultra-rapid acting, novel formulation of insulin that accelerates
the absorption of insulin post injection, even when delivered at a
high concentration, and hence a lower injection volume. With no
concentrated (>200 U/mL), rapid acting insulins on the market,
AT278 has potential to be the first, and only, insulin available to
the growing number of patients with high daily insulin requirements
and to be a critical enabler of next-generation miniaturised and
longer wear insulin pumps.
Professor Thomas Pieber, Principal Investigator for the
ARE-278-104 study, said: "The clinical significance
of these findings is considerable. AT278's accelerated early PK/PD
profile compared with NovoRapid® in overweight and obese people
with type 2 diabetes confirms previous findings in people with type
1 diabetes and shows that AT278 can maintain its faster action
profile irrespective of diabetes type and BMI.
The faster onset
and stronger early glucose-lowering effect, consistent across BMI
subgroups, indicate that AT278 could provide significantly better
post-prandial glucose control and improved convenience for anyone
with diabetes who has a high daily insulin need. It also, clearly,
can be a catalyst in the progress towards miniaturised
next-generation insulin pumps, where the size of existing
devices remains a major hurdle for development."
Sarah Howell, Chief Executive Officer of Arecor,
added: "Despite the improvements in
outcomes among people with diabetes who use insulin pumps and
automated insulin delivery systems they are still used by only 40%
of people with Type I diabetes and less than 10% of people with
Type 2 diabetes in the US where use is greatest. A critical barrier
to further uptake is the size and short duration of wear of
existing insulin pumps. We believe the results we are presenting
today clearly demonstrate that AT278 has the potential to break
this barrier and make miniaturised, longer wear insulin pumps a
reality and thereby meet the needs of patients, and of device
companies as they seek to grow a market which is valued at c. $5.5
billion today and forecast to reach more than $15.8bn by
2030."
In the double-blind, randomised,
two-way crossover study, the pharmacokinetic (PK)/pharmacodynamic
(PD) and safety profiles of a single subcutaneous (SC) dose of 0.5
U/kg AT278 (500 U/mL) were compared with those of a single SC dose
of 0.5 U/kg NovoRapid® (100 U/mL), a currently
available gold standard, rapid acting insulin, in 41 participants
with Type 2 diabetes and a median BMI of 29.7 kg/m2. The
trial was conducted in a glucose clamp setting at the Medical
University of Graz and Joanneum Research in Austria, an
internationally recognised centre of excellence in the field of
diabetes research.
The PK/PD profile for AT278 was
accelerated compared with
NovoRapid®. AT278 demonstrated a
1.7-fold (95% CI 1.32; 2.96) higher glucose-lowering effect within
the first 60 minutes which was statistically superior to
NovoRapid® (p< 0.0001). The
glucose-lowering effect remained higher up to 2 hours post-dosing
(treatment ratio [95% CI] 1.19 [1.02; 1.39]). AT278 showed a faster
onset of glucose-lowering effect, with a 5-minute earlier onset of
action and 25-minute earlier tEarly50%GIRmax than
NovoRapid®. It also showed a faster
onset of insulin exposure compared with NovoRapid, with
a 5-minute faster insulin appearance and 24-minute
faster tEarly50%Cmax.
Insulin exposure with AT278 was 1.5-fold higher
within the first 60 minutes (95% CI 1.28;
1.71). The superior early glucose-lowering
effect of AT278 was maintained when the population was divided into
BMI subgroups.
Both insulins were well tolerated.
Adverse events were mostly mild to moderate and not related to the
study drugs.
Arecor is continuing to explore
funding options for AT278, including but not limited to
co-development arrangements, to conduct a clinical pump study to
further demonstrate the potential of AT278 to disrupt the market by
enabling the next generation of truly miniaturised, longer-wear
insulin pumps, a key focus for patients, physicians and the
industry.
Headline data from this clinical
trial were previously announced by the Company in May
2024.
-ENDS-
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Arecor
Therapeutics plc
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www.arecor.com
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Dr Sarah Howell, Chief Executive
Officer
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Tel: +44 (0) 1223 426060
Email: info@arecor.com
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Panmure Liberum
Limited (NOMAD and Broker)
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Freddy Crossley, Emma Earl (Corporate
Finance)
Rupert Dearden (Corporate Broking)
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Tel: +44 (0) 20 7886 2500
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WG Partners LLP
(Financial Advisor)
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Nigel Barnes, Satheesh Nadarajah
David Wilson, Claes Spang
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Tel: +44 (0)203 705 9321
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ICR
Consilium
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Chris Gardner, David Daley, Lindsey
Neville
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Tel: +44 (0) 20 3709 5700
Email: arecor@consilium-comms.com
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Notes to
Editors
The abstract, "Pharmacokinetic and pharmacodynamic
properties of highly concentrated insulin aspart AT278 U500 in
overweight and obese people with type 2 diabetes" is
available on the EASD 2024 website.
About the
EASD
The European Association for the Study of
Diabetes (EASD) is a non-profit, medical scientific association,
founded in 1965 to encourage and support research in the field of
diabetes, the rapid diffusion of acquired knowledge and to
facilitate its application. EASD holds its Annual Meeting in a
different European city each year with more than 15,000 delegates
from over 130 countries attending. The scientific programme
includes more than 1,200 talks and presentations on the latest
results in diabetes research by leading experts in the
field.
About
Arecor
Arecor Therapeutics plc is a globally focused
biopharmaceutical company transforming patient care by bringing
innovative medicines to market through the enhancement of existing
therapeutic products. By applying our innovative proprietary
technology platform, Arestat™, we are developing an internal
portfolio of proprietary products in diabetes and other
indications, as well as working with leading pharmaceutical and
biotechnology companies to deliver therapeutic products. The
Arestat™ platform is supported by an extensive patent
portfolio.
For further details please see our website,
www.arecor.com
