Research published in Science Translational Medicine advances
therapies to regenerate beta cells as a potential new treatment for
diabetes
In preclinical studies, a team of researchers from City of Hope®
in Los Angeles and Mount Sinai Health System in New York reports
new findings on a therapeutic combination that regenerated human
insulin-producing beta cells, providing a possible new treatment
for diabetes. The findings were published today in Science
Translational Medicine.
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This work, led by Andrew F. Stewart, M.D., Irene and Dr. Arthur
M. Fishberg Professor of Medicine and Director of the Mount Sinai
Diabetes, Obesity and Metabolism Institute, began at the Icahn
School of Medicine at Mount Sinai in 2015. The studies were a team
effort. Adolfo Garcia-Ocaña, Ph.D., formerly a professor at Mount
Sinai who is now at City of Hope, a leading research center for
diabetes and one of the largest cancer research and treatment
organizations in the United States, and is the Ruth B. & Robert
K. Lanman Chair in Gene Regulation and Drug Discovery Research and
chair of the Department of Molecular & Cellular Endocrinology,
and his research team designed the studies and performed the novel,
extensive and detailed animal transplant and drug treatment models
using beta cells from donors. Final studies took place at City of
Hope in 2023.
For the study, the natural product harmine, which is found in
some plants, was combined with a widely used class of type 2
diabetes therapy called GLP1 receptor agonists. Researchers
transplanted a small number of human beta cells into mice that had
no immune system and that also served as a standard model of type 1
and type 2 diabetes; these mice were treated with the combination
therapy and their diabetes was rapidly reversed. Strikingly, human
beta cell numbers increased by 700% over three months with this
drug combination.
“This is the first time scientists have developed a drug
treatment that is proven to increase adult human beta cell numbers
in vivo. This research brings hope for the use of future
regenerative therapies to potentially treat the hundreds of
millions of people with diabetes,” said Dr. Garcia-Ocaña, the
paper’s corresponding author.
“It has been remarkable to watch this story unfold over the past
15 years,” said Dr. Stewart, who, along with Peng Wang, Ph.D.,
professor of Medicine (Endocrinology, Diabetes and Bone Disease) at
Icahn Mount Sinai, conceived of and performed the initial
high-throughput drug screen that led to the discovery of harmine
described in Nature Medicine in 2015. “The steady progression from
the most basic human beta cell biology, through robotic drug
screening and now moving to human studies, illustrates the
essential role for physician-scientists in academia and
pharma.”
Growing new beta cells
More than 10% of the world’s adult population has diabetes, a
disease defined by high blood sugar levels. In both type 1 and type
2 diabetes, a reduction in both the quantity and quality of
insulin-producing beta cells causes high blood sugar.
Unfortunately, none of the many commonly used diabetes therapies
are able to increase human beta cell numbers, and therefore cannot
completely reverse diabetes.
Fortunately, most people with diabetes have some residual beta
cells, which is what inspired the research team to search for ways
to restore their numbers. The team had previously shown that
several different inhibitors of an enzyme in beta cells called
DYRK1A can induce the proliferation of adult human beta cells in a
tissue culture dish for a few days. But prior to this study, no one
had shown the ability to expand human beta cells numbers in vivo in
human islet grafts used in an animal model over many months.
To accurately measure the mass of human beta cells in the islet
grafts, the team turned to Sarah A. Stanley, M.B.B.Ch., Ph.D.,
associate professor of Medicine (Endocrinology, Diabetes and Bone
Disease), and Neuroscience, at Icahn Mount Sinai. Using an advanced
laser microscopy tool called iDISCO+ that effectively makes
biological tissue transparent, Dr. Stanley saw that beta cell mass
was dramatically increased through mechanisms that included
enhanced proliferation, function and survival of the human beta
cells. The technology allowed for accurate and rigorous
quantitative assessment of engrafted human beta cells for the first
time.
Translating results to the clinic
The Mount Sinai team recently completed a phase 1 clinical trial
of harmine in healthy volunteers to test its safety and
tolerability. At the same time, Robert J. DeVita, Ph.D., professor
of Pharmacological Sciences and director of the Marie-Josée and
Henry R. Kravis Drug Discovery Institute at Mount Sinai, has
developed next-generation DYRK1A inhibitors. Mount Sinai is
conducting studies to test these in humans for potential toxicity
risks and estimate dosing for clinical trials, and is planning to
initiate first-in-human trials with independent research teams next
year. Mount Sinai owns an extensive patent portfolio covering these
technologies.
Researchers also want to address the fact that in patients with
type 1 diabetes, the immune system will continue to kill new beta
cells. At City of Hope, Dr. Garcia-Ocaña and colleague Alberto
Pugliese, M.D., Samuel Rahbar Chair in Diabetes & Drug
Discovery, chair of the Department of Diabetes Immunology and
director of The Wanek Family Project for Type 1 Diabetes within the
Arthur Riggs Diabetes & Metabolism Research Institute, plan to
test inducers of beta cell regeneration together with
immunomodulators that regulate the immune system. Their goal is for
the combination to allow new beta cells to thrive and improve
insulin levels.
“Our studies pave the way for moving DYRK1A inhibitors into
human clinical trials, and it's very exciting to be close to seeing
this novel treatment used in patients,” Dr. Garcia-Ocaña said.
“There is nothing like this available to patients right now.”
The work outlined in the Science Translational Medicine paper
was funded by grants from the National Institutes of Health (NIH),
the National Institute of Diabetes and Digestive and Kidney
Disease, and BreakthroughT1D (formerly JDRF), as well as from
philanthropic donations to Mount Sinai, support from The Wanek
Family Project for Type 1 Diabetes at City of Hope and additional
generous philanthropic gifts.
Other critical members of the team include Mount Sinai’s
Carolina Rosselot, Ph.D., Yansui Li, Ph.D., and Alexandra
Alvarsson, Ph.D. Additional City of Hope authors on the paper are
Geming Lu, M.D., assistant research professor, and Randy Kang,
senior research associate, who are both members of Dr.
Garcia-Ocaña’s lab.
Drs. Stewart and DeVita are named co-inventors on patent
applications for DYRK1A inhibitors, such as harmine, for the
treatment of diabetes. These patent applications are filed through
the Icahn School of Medicine at Mount Sinai and are currently
unlicensed.
About City of Hope
City of Hope's mission is to make hope a reality for all touched
by cancer and diabetes. Founded in 1913, City of Hope has grown
into one of the largest cancer research and treatment organizations
in the U.S. and one of the leading research centers for diabetes
and other life-threatening illnesses. City of Hope research has
been the basis for numerous breakthrough cancer medicines, as well
as human synthetic insulin and monoclonal antibodies. With an
independent, National Cancer Institute-designated comprehensive
cancer center at its core, City of Hope brings a uniquely
integrated model to patients spanning cancer care, research and
development, academics and training, and innovation initiatives.
City of Hope’s growing national system includes its Los Angeles
campus, a network of clinical care locations across Southern
California, a new cancer center in Orange County, California, and
cancer treatment centers and outpatient facilities in the Atlanta,
Chicago and Phoenix areas. City of Hope’s affiliated group of
organizations includes Translational Genomics Research Institute
and AccessHopeTM. For more information about City of Hope, follow
us on Facebook, X, YouTube, Instagram and LinkedIn.
About the Mount Sinai Health System
Mount Sinai Health System is one of the largest academic medical
systems in the New York metro area, with 48,000 employees working
across eight hospitals, more than 400 outpatient practices, more
than 600 research and clinical labs, a school of nursing, and a
leading school of medicine and graduate education. Mount Sinai
advances health for all people, everywhere, by taking on the most
complex health care challenges of our time—discovering and applying
new scientific learning and knowledge; developing safer, more
effective treatments; educating the next generation of medical
leaders and innovators; and supporting local communities by
delivering high-quality care to all who need it.
Through the integration of its hospitals, labs, and schools,
Mount Sinai offers comprehensive health care solutions from birth
through geriatrics, leveraging innovative approaches such as
artificial intelligence and informatics while keeping patients’
medical and emotional needs at the center of all treatment. The
Health System includes approximately 9,000 primary and specialty
care physicians and 11 free-standing joint-venture centers
throughout the five boroughs of New York City, Westchester, Long
Island, and Florida. Hospitals within the System are consistently
ranked by Newsweek’s® “The World’s Best Smart Hospitals, Best in
State Hospitals, World Best Hospitals and Best Specialty Hospitals”
and by U.S. News & World Report's® “Best Hospitals” and “Best
Children’s Hospitals.” The Mount Sinai Hospital is on the U.S. News
& World Report® “Best Hospitals” Honor Roll for 2023-2024.
For more information, visit https://www.mountsinai.org or find
Mount Sinai on Facebook, Twitter and YouTube.
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version on businesswire.com: https://www.businesswire.com/news/home/20240710267036/en/
City of Hope Letisia Marquez 626-476-7593
lemarquez@coh.org
Mount Sinai Health System Laura Ruocco-Duran 646-877-6727
Laura.Ruocco-Duran@mountsinai.org