Detailed results were published in The Lancet
and simultaneously presented at the European Association for the
Study of Diabetes (EASD) Annual Meeting 2024
INDIANAPOLIS, Sept. 10,
2024 /PRNewswire/ -- Eli Lilly and Company
(NYSE: LLY) today announced detailed results from the QWINT-5
phase 3 trial evaluating once-weekly insulin efsitora alfa
(efsitora) compared to once-daily insulin degludec in adults with
type 1 diabetes who require daily basal and multiple daily mealtime
insulin injections. The data were published in The Lancet
and simultaneously presented today at the European Association for
the Study of Diabetes (EASD) Annual Meeting 2024.
In the trial, efsitora met the primary endpoint of non-inferior
A1C reduction at week 26. For the efficacy
estimand1,2, efsitora reduced A1C by 0.53% compared
to 0.59% for insulin degludec resulting in an A1C of 7.37% and
7.32% respectively3.
In a key secondary endpoint, time in range4 as
measured by continuous glucose monitoring (CGM) was similar between
efsitora and insulin degludec during the four weeks prior to week
26. In an additional key secondary endpoint, the estimated combined
rates of patient-reported clinically significant (blood glucose
<54 mg/dL) or severe nocturnal5 hypoglycemic events
per patient-year of exposure were similar between efsitora and
insulin degludec over the 52-week study period.
"People with type 1 diabetes need insulin every day. Currently,
they can deliver the insulin using an automated insulin delivery
system or by taking a daily basal insulin injection and multiple
mealtime insulin injections each day," said Richard Bergenstal,
M.D., executive director of the International Diabetes
Center, HealthPartners Institute. "This new data shows that
with one dose a week of basal insulin, efsitora was able to achieve
a similar A1C reduction as taking an injection of one of the most
used background insulins every day. I look forward to further
evaluation of these data, including ways to minimize hypoglycemia,
so once-weekly insulin can be one option for personalizing the
management of type 1 diabetes."
Full Results
QWINT-5 Study:
Primary and Secondary Endpoints
|
|
Efficacy
Estimand
|
Treatment-Regimen
Estimand6
|
Primary Endpoint –
A1C Reduction (Resulting A1C) at 26 Weeks
|
Efsitora
|
-0.53%
(7.37%)
|
-0.51%
(7.41%)7
|
Insulin
degludec
|
-0.59%
(7.32%)
|
-0.56%
(7.36%)8
|
Secondary Endpoint –
Percent Time in Range During the 4 Weeks Prior to Week
26
|
Efsitora
|
52.8 %
|
52.5 %
|
Insulin
degludec
|
53.1 %
|
52.9 %
|
Secondary Endpoint
– Estimated Rate of Clinically
Significant9 or Severe Nocturnal
Hypoglycemic Events Per Patient-Year of Exposure through 52
Weeks
|
Efsitora
|
|
1.99
|
Insulin
degludec
|
|
1.96
|
In the trial, estimated combined rates of patient-reported
clinically significant (blood glucose <54 mg/dL) or severe
hypoglycemic events per patient-year of exposure through week 52
were 14.03 with efsitora vs. 11.59 with insulin degludec. There was
no evidence of increased duration of hypoglycemia with efsitora
compared to insulin degludec based on CGM data.
Estimated rates of severe hypoglycemic events per patient-year
of exposure through week 52 were 0.14 with efsitora vs. 0.04 with
insulin degludec. More than half (64%) of the reported severe
hypoglycemic events with efsitora took place during the initial 12
weeks of the trial's treatment period and incidence of severe
hypoglycemia in both treatment groups declined after week
12.
Overall incidence of treatment-emergent adverse events were
comparable across treatment groups. Serious adverse events were
higher in efsitora compared to insulin degludec, driven by severe
hypoglycemic events.
"When we commercialized insulin more than 100 years ago, it
marked the beginning of our commitment to people living with type 1
diabetes – today's announcement continues that legacy," said
Jeff Emmick, M.D., Ph.D., senior
vice president, product development, Lilly. "These results
underscore the potential of efsitora to help some people living
with type 1 diabetes lower their A1C with only one basal insulin
injection per week, while also highlighting the complexity of
treating this chronic disease. With the data we have seen from our
phase 3 program so far, we are confident in efsitora's potential to
transform diabetes care and will continue to pursue new treatment
options until we can eliminate the disease entirely."
Detailed results for QWINT-2 are also being presented at EASD
and simultaneously published in The New England Journal of
Medicine.
About the QWINT clinical trial program
The QWINT phase
3 global clinical development program for insulin efsitora alfa
(efsitora) in diabetes began in 2022 and has enrolled more than
4,000 people living with type 1 or type 2 diabetes across five
global registration studies.
QWINT-5 (NCT05463744) is a multicenter, treat-to-target,
randomized, parallel-design, open-label study comparing the
efficacy and safety of efsitora as a once-weekly basal insulin to
insulin degludec in participants with type 1 diabetes treated with
daily basal and multiple daily mealtime insulin injections. The
trial consisted of a 52-week treatment period with the primary
endpoint measured at 26 weeks. 692 participants across the U.S.,
Argentina, Japan, Poland, Puerto
Rico, Slovakia and
Taiwan were randomized to receive
efsitora once weekly or insulin degludec once daily administered
subcutaneously. The primary objective of the study is to
demonstrate non-inferiority in reducing A1C at week 26 with
efsitora compared to insulin degludec. Throughout the study,
participants used unblinded CGM.
About Insulin Efsitora Alfa
Insulin efsitora alfa
(efsitora) is a once-weekly basal insulin, a fusion protein that
combines a novel single-chain variant of insulin with a
human IgG2 Fc domain. It is specifically designed for
once-weekly subcutaneous administration, and with its low
peak-to-trough ratio, has the potential to provide more stable
glucose levels (less glucose variability) throughout the week.
Efsitora is in phase 3 development for adults with type 1 and 2
diabetes.
About Lilly
Lilly is a medicine company turning
science into healing to make life better for people around the
world. We've been pioneering life-changing discoveries for nearly
150 years, and today our medicines help more than 51 million people
across the globe. Harnessing the power of biotechnology, chemistry
and genetic medicine, our scientists are urgently advancing new
discoveries to solve some of the world's most significant health
challenges: redefining diabetes care; treating obesity and
curtailing its most devastating long-term effects; advancing the
fight against Alzheimer's disease; providing solutions to some of
the most debilitating immune system disorders; and transforming the
most difficult-to-treat cancers into manageable diseases. With each
step toward a healthier world, we're motivated by one thing: making
life better for millions more people. That includes delivering
innovative clinical trials that reflect the diversity of our world
and working to ensure our medicines are accessible and affordable.
To learn more, visit Lilly.com and Lilly.com/news, or follow
us on Facebook, Instagram and LinkedIn. P-LLY
Cautionary Statement Regarding Forward-Looking
Statements
This press release contains forward-looking
statements (as that term is defined in the Private Securities
Litigation Reform Act of 1995), including statements about insulin
efsitora alfa as a potential treatment for people with type 1
diabetes and the timeline for future readouts, presentations, and
other milestones relating to insulin efsitora alfa and its clinical
trials, and reflects Lilly's current beliefs and expectations.
However, as with any pharmaceutical product, there are substantial
risks and uncertainties in the process of drug research,
development, and commercialization. Among other things, there is no
guarantee that planned or ongoing studies will be completed as
planned, that future study results will be consistent with study
results to date, that insulin efsitora alfa will prove to be a safe
and effective treatment for type 1 diabetes, that insulin efsitora
alfa will receive regulatory approval, or that Lilly will execute
its strategy as expected. For further discussion of these and other
risks and uncertainties that could cause actual results to differ
from Lilly's expectations, see Lilly's Form 10-K and Form 10-Q
filings with the United States Securities and Exchange Commission.
Except as required by law, Lilly undertakes no duty to update
forward-looking statements to reflect events after the date of this
release.
1 The efficacy estimand represents the treatment
effect had all participants adhered to the study drug without
initiating rescue therapy for persistent severe hyperglycemia.
2 95% CI for treatment difference (-0.075% to
0.19%).
3 From a baseline A1C of 7.89% for efsitora and 7.93%
for insulin degludec.
4 Glucose 70-180 mg/dL.
5 Any event that occurred between
midnight and 6 a.m.
6 Treatment-regimen estimand represents the efficacy
irrespective of adherence to the investigational medicine or
introduction of rescue therapy for persistent severe
hyperglycemia.
7 From a baseline A1C of 7.88% for efsitora and 7.94%
for insulin degludec.
8 95% CI for treatment difference (-0.077% to
0.181%).
9 Blood glucose <54 mg/dL.
Refer
to:
|
Niki Smithers,
smithers_niki@lilly.com; 317-358-9074 (Media)
|
|
Joe Fletcher;
jfletcher@lilly.com, 317-296-2884 (Investors)
|
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SOURCE Eli Lilly and Company