Arecor
Therapeutics plc(“Arecor” or “the
Company”)
AT278 ULTRA-CONCENTRATED ULTRA-RAPID
ACTING INSULIN DEMONSTRATES SUPERIORITY IN PHASE I CLINICAL TRIAL
IN OVERWEIGHT AND OBESE PEOPLE WITH TYPE 2 DIABETES
- AT278
demonstrates significantly
accelerated PK/PD profile
compared to
NovoRapid® and Humulin® R U-500
in people with Type 2
Diabetes and high BMI
- Confirms previous trial
results in people with Type 1 diabetes, demonstrating AT278 can
maintain fast and superior onset of action and glucose lowering
profile irrespective of diabetes type and BMI
- Enables delivery of a highly
concentrated, low volume injection, offering more effective
mealtime glucose control to meet growing unmet need in patients
requiring high daily doses of insulin
- Creates potential
to be the first, and
only, ultra-concentrated (500 U/mL)
ultra-rapid insulin product
enabling miniaturisation of next-generation insulin
pumps
- Company will host a CEO and
key opinion leader webinar to discuss the results on Tuesday 21 May
at 14.30 BST
Cambridge, UK, 20 May 2024.
Arecor Therapeutics plc (AIM: AREC), the biopharmaceutical group
advancing today’s therapies to enable healthier lives, today
announces that its ultra-concentrated, ultra-rapid acting insulin
candidate, AT278, met all primary and secondary endpoints, and also
demonstrated superiority to NovoRapid® and Humulin® R U-500, in a
Phase I clinical trial in Type 2 diabetics with a high body mass
index (BMI).
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.
Sarah Howell,
Chief Executive
Officer of
Arecor, said: "We are delighted
with the clinical results from this second Phase I study,
demonstrating AT278’s superiority over NovoRapid® and Humulin® R
U-500 in Type 2 diabetics with a high BMI. They further add to the
positive results from our previous clinical study in Type 1
diabetic patients, where superiority was also demonstrated. This is
a significant step in AT278’s development and extends our
confidence in its clear potential to provide a superior insulin
treatment option that lowers burden and improves outcomes for
people living with diabetes who require high daily doses of
insulin. Such patients make up a large segment of the target
market. In addition, as the only concentrated, yet very rapid
acting, insulin in development, AT278 has the capability 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.”
Many Type 2 diabetics with a high BMI are
currently not well controlled, and improved treatments options such
as AT278 are needed to reduce patient burden through fewer
injections per day, reduced injection volumes and dosing
flexibility around mealtimes. This lowering of burden for patients
improves treatment adherence and, allied with AT278’s superior
efficacy, should improve both blood glucose control and outcomes.
In addition, a truly ultra-rapid, ultra-concentrated insulin is a
critical step towards next-generation miniaturised and long-wearing
insulin pumps, which are predicted to transform future diabetes
management.
Professor Thomas Pieber, Principal
Investigator for the ARE-278-104 clinical trial, said:
“These results are highly significant, AT278 has clearly
demonstrated faster insulin absorption with an accelerated
Pharmacokinetic (PK) and Pharmacodynamic (PD) profile compared to
the lower concentration standard insulin aspart (NovoRapid®). The
PK/PD profile of AT278 (500 U/mL) was also greatly accelerated
compared to Humulin® R U-500 (500 U/mL). Together
with its superior profile in the earlier Phase I clinical study in
Type 1 diabetic patients1 AT278 has demonstrated its ability to
maintain a fast and superior onset of action and glucose lowering
profile irrespective of diabetes type and BMI. This makes AT278
completely unique in the competitive field of insulin analogues.
Not only does it have the potential to significantly improve
post-prandial glucose control whilst lowering burden for anybody
with diabetes who has a high daily insulin need, it can act as a
catalyst in the development of miniaturised insulin delivery
systems, where the size of existing devices is a significant
barrier to use for many patients.”
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 treatment, in 39
participants with Type 2 diabetes within a BMI range of 25 and 39
kg/m2, in a euglycemic clamp setting. The PK/PD profile of 0.5 U/kg
AT278 (500 U/mL) was also compared to a single SC dose of 0.5U/kg
Humulin® R U-500 (500 U/mL) in an open label
manner.
- The trial met the primary endpoint
of non-inferiority with respect to glucose lowering actions
compared with NovoRapid®
- AT278 (500 U/mL) demonstrated a
significantly accelerated (superior) early PK/PD profile compared
to NovoRapid® (100 U/mL), despite a 5-fold
increase in concentration
- AT278 (500 U/mL) demonstrated a
significantly accelerated (superior) PK/PD profile compared to
Humulin® R U-500 (500 U/mL), the only other
insulin available at a concentration of 500 U/mL
- No safety signals were
detected
With around 537m people living with diabetes
worldwide, there are growing numbers of people who require insulin
to manage their blood glucose and, for many, their diabetes is
still poorly controlled. There is a growing need for highly
concentrated, much faster, and more physiological insulins to
effectively manage diabetes. In the US alone, nearly 10% of insulin
scripts written in 2022 were for products with a concentration of
>100 U/mL2. Furthermore, despite the improvements in outcomes
among people with diabetes who use insulin pumps and automated
delivery systems, they are still only used by less than 40% of
people with Type 1 diabetes and less than 10% of people with Type 2
diabetes in the US3. The size and short duration of wear of
existing insulin pumps remains a significant barrier to use. AT278
has the potential to be the only highly concentrated, ultra-rapid
acting insulin to enable the next generation of miniaturised,
longer wear insulin pumps. The insulin pump market is valued at
circa $5.5bn market today4, with a significant opportunity for
substantial growth in this market by expanding use across the Type
1 and Type 2 patient population that can be further enabled by
AT278 and a next generation insulin pump.
A full analysis of the trial data is now
underway to enable the Company to determine and pursue a strategy
for AT278 that maximises value for shareholders and patients.
Detailed data from the trial will be submitted for publication and
presentation at a future international diabetes
conference.
AT278 clinical results CEO and KOL
webinar - Tuesday 21 MayDr Sarah Howell, Chief Executive
Officer, and Professor Thomas Pieber, Principal Investigator for
the ARE-278-104 clinical trial and Professor of Medicine, Head of
the Division of Endocrinology and Metabolism and Chairman of the
Department of Internal Medicine at Medical University of Graz,
Austria will host a CEO and key opinion leader webinar to discuss
the clinical results on Tuesday 21 May at 14.30 BST.
To register to join the live webcast click here
and to register for the conference line to ask questions click
here.
Please contact ICR Consilium for details on
arecor@consilium-comms.com.
This announcement contains inside information
for the purposes of the retained UK version of the EU Market Abuse
Regulation (EU) 596/2014 ("UK MAR").
-ENDS-
References
- Pharmacokinetics and Pharmacodynamics of a Novel U500 Insulin
Aspart Formulation: A Randomized, Double-Blind, Crossover Study in
People With Type 1 Diabetes Care 2023;46(4):757–764:
https://doi.org/10.2337/dc22-1054
- 2022 reports from Symphony. Retrieved October 2023
- Seagrove Partners Diabetes Bluebook 2022
- Insulin pump company annual reports and Company estimates
For more information, please contact:
|
Arecor Therapeutics plc |
www.arecor.com |
|
Dr Sarah Howell, Chief Executive Officer |
Tel: +44 (0) 1223 426060Email: info@arecor.com |
|
|
|
|
Susan Lowther, Chief Financial Officer |
Tel: +44 (0) 1223 426060Email: info@arecor.com |
|
|
|
|
Panmure Gordon (UK) Limited (NOMAD and
Broker) |
|
|
Freddy Crossley, Emma Earl (Corporate Finance)Rupert Dearden
(Corporate Broking) |
Tel: +44 (0) 20 7886 2500 |
|
|
|
|
WG Partners LLP (Financial Advisor) |
|
|
Nigel Barnes, Satheesh NadarajahDavid Wilson, Claes Spang |
Tel: +44 (0)203 705 9321 |
|
|
|
|
ICR Consilium |
|
|
Chris Gardner, David Daley, Lindsey Neville |
Tel: +44 (0) 20 3709 5700Email: arecor@consilium-comms.com |
|
|
|
Notes to Editors
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
Grafico Azioni American Resources (NASDAQ:AREC)
Storico
Da Dic 2024 a Gen 2025
Grafico Azioni American Resources (NASDAQ:AREC)
Storico
Da Gen 2024 a Gen 2025
