In this work, we have brought the
release of glucagon under the
control of light. The aim of this approach is to allow minimally invasive,
two-hormone control of blood glucose. Glucagon has two major challenges
associated with its therapeutic application: (1) the required amount
and timing of glucagon release is highly variable, and (2) glucagon
rapidly fibrillates in solution, forming aggregates that are inactive.
We have developed a light activated glucagon trimer, in which we have
joined three glucagon molecules via light cleaved linkers. We demonstrated
that this material can be stimulated by light to release glucagon
in a predictable manner. In addition, we demonstrated that in the
absence of light, the trimer does not form fibrils and thus releases
normal unfibrillated glucagon upon irradiation. These qualities make
this material ideal for incorporation into a two hormone light-activated
artificial pancreas system.
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