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ACS Meeting News

Injectable system responds when blood sugar drops low

Responsive materials for diabetes can release a hormone when glucose drops

by Laurel Oldach
March 20, 2024 | A version of this story appeared in Volume 102, Issue 9

 

Managing diabetes has gotten easier over the years—but maintaining a healthy blood sugar level can still feel like walking a tightrope. Over time, high blood glucose can cause medical problems, so many people with diabetes rely on the hormone insulin to reduce circulating glucose. But using too much insulin can cause a drop in blood sugar that can develop into a life-threatening emergency. At such moments, the best treatment is glucagon, a hormone that releases stored sugar, opposing insulin.

Left side of the image shows several wheel-shaped, red and gray molecules with linear, yellow features, all within a blue membrane. The middle of the diagram shows glucose concentration going down, and then the right side shows what happens when the assembly is in areas with low glucose, the assembly starts breaking down into smaller, less ordered pieces.
Credit: Matthew Webber
A peptide with a glucose-binding moiety forms phase-separated droplets with a glucagon-based drug when glucose is present. When glucose drops below a certain threshold, the interaction breaks up, allowing the glucagon to dissipate.

At ACS Spring 2024 on Tuesday, University of Notre Dame professor Matthew Webber described his work on designing responsive, injectable materials that hold glucagon and release it when glucose concentration drops in their surroundings. Many research groups, including his own, are developing materials that release insulin in response to sugar spikes. But to generate a material that responds to the absence rather than the presence of a molecule, Webber said, is “a little bit of a paradigm shift” for the field.

In a presentation to the Biochemical Technology division, Webber described three chemical approaches researchers in his lab spearheaded by graduate student Sihan Yu have invented to sequester a glucagon drug in responsive hydrogels and coacervates.

The researchers are testing the materials in diabetic animals; each one, they have observed, can reduce the crashing blood sugar that the animals experience. But the materials also have some problems, including slow response kinetics and a tendency to leak glucagon in instances when it is not needed, which can lead to undesirably high blood sugar.

Kaylin Earnest, a medicinal chemist at the University of Cincinnati Clermont College who attended the talk, told C&EN that even though the materials are not ready to be deployed, they’re an exciting advance. While the absence of sugar is more technically challenging to detect and respond to than an excess, she said, it’s also more urgent for patients. “You can come down from a high, but a low is hard to fix.”

Webber hopes to work toward a combined system that can release both insulin and glucagon when appropriate, just as the pancreas does in people who don’t have diabetes.

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