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Researchers
develop, patent promising Oral Insulin for
treatment of Diabetes
Newswise — Syracuse University researchers have designed,
tested and patented a new method of oral
insulin delivery that can potentially help
reduce daily insulin injections for millions
of people with diabetes who require therapy
for optimal glycemic control.
The pharmaceutical journal ChemMedChem will publish in
its December issue this research conducted
by Robert Doyle, assistant professor of
chemistry in SU’s College of Arts and
Sciences; Timothy J. Fairchild, assistant
professor of exercise science in SU’s School
of Education; and Amanda Petrus and Anthony
Vortherms, both chemistry graduate students
in Doyle’s laboratory.
The non-invasive, basal delivery of insulin has been a major
goal for the treatment of diabetes mellitus
(DM), which affects more than 21 million
individuals in the United States.
Basal therapy describes a low, continuous dosage of insulin
(commonly administered through a slow-acting
insulin injection) that replaces the lack of
insulin output by the pancreas in diabetics.
This works together with bolus therapy,
which is a dosage of insulin intended to
replace a meal or to make a large
glucose-level correction.
Up to this point, basal oral insulin deliveries have not been
possible due to proteolytic degradation
(digestion of proteins by cellular enzymes)
and inefficient enteric uptake, meaning that
free insulin delivered orally is never
effectively delivered to the bloodstream
because it is destroyed as it passes through
the gastrointestinal tract (GIT), before it
reaches its necessary receptors.
The team of SU researchers has now developed a method of oral
insulin delivery that eliminates the
breakdown of insulin in the GIT, allowing
for the transport of insulin to the
bloodstream.
This was accomplished by binding an insulin peptide to
vitamin B-12, which acts as a carrier for
the insulin and protects it as it is
transported through the GIT. Because the
insulin peptide is still intact as it enters
the blood stream, it can be carried
throughout the body as continuously as the
B-12 vitamin is. This is a Trojan horse
strategy, as the B-12 hides the insulin and
carries it across the GIT's “walls.”
Mammals have an active transport mechanism in their GIT for
the absorption and uptake of the relatively
large vitamin B-12. Because of this, the
length of this linkage is optimized so that
the biological activity of both the B-12 and
the biologically active substance (in this
case, insulin) is maintained.
At this point in the research, the SU team has focused
on one insulin peptide carried by one B-12,
which has a residence time in rats of about
eight hours. However, they are now
investigating whether more insulin can be
attached to the B-12, which would provide a
longer residence time—optimally 12 hours—so
that potentially diabetics could take one
insulin pill in the morning, and one at
night for greater metabolic control
throughout 24 hours.
This basal approach also helps prevent the continuous,
unstabilized glucose uptake that is related
to the development of metabolic-related
complications in diabetics, including
retinopathy and blindness, kidney failure,
nerve damage, heart disease and stroke.
Right now, the only options for this type of basal therapy
are multiple injections of pre-prandial,
short-acting insulin taken throughout the
day. By providing long-lasting insulin
analogues through this oral delivery,
coupled with an inhalation bolus insulin
therapy, diabetics in the future may rely on
an entirely non-evasive delivery system for
insulin using a basal/bolus regime.
Doyle believes that human investigations into the
effectiveness of the team’s oral insulin
delivery therapy may be a few years away,
with new derivatives to be assembled and
extensive further testing to be performed.
“We have been interested in the oral delivery of insulin and
also certain neuro-peptides, and have been
exploring a variety of ways to achieve our
goals,” says Doyle. “In the case of insulin,
we had a hypothesis, we set about testing
our hypothesis, and we were rewarded for the
effort. Having things go your way doesn’t
happen in science often enough, so when it
does it’s very rewarding.”
Fairchild, in collaboration with the team, conducted the
testing in diabetic rat models, focusing on
the experimental protocol—dosage, methods of
blood sampling and frequency—that should be
used.
“This is a very exciting time in diabetes-related research,”
says Fairchild. “There are many research
groups approaching potential treatment
strategies for diabetes using a number of
avenues, but the possibility of having an
oral insulin medication has tremendous
feasibility, particularly with children and
in less-developed countries where sterile
needles and adequate training—for injection
site and frequency, as well as needle
disposal—may not always be available.”
Petrus, a third-year graduate student studying inorganic
chemistry in Doyle’s lab, served as the
principal researcher. This research on oral
insulin is her doctoral degree project and
will be the bulk of her dissertation, which
she will defend in two to three years.
She carried out the synthesis of B-12/insulin and is
currently working with new derivatives of it
to try to gain improvement on its activity.
“I am very honored to be contributing to a
project with the potential to help people,”
says Petrus. “It means a great deal to me
that my dissertation will be addressing an
issue that touches so many people. Diabetes
runs in my family, and several of my friends
are dealing with the early stages of the
disease.”
“It is great to be a part of something that has the potential
to help so many people,” says Vortherms,
also a third-year chemistry graduate student
at SU. “It is always exciting when you take
something and you can do the unexpected with
it. That kind of science turns heads and is
what gets talked about years down the road.”
The journal, ChemMedChem, called these findings by
Doyle, Fairchild, Petrus and Vortherms
“pharmacologically and clinically highly
relevant.” The article is now available
online at ChemMedChem's website
http://www.chemmedchem.com.
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