Literature DB >> 25675515

Glucose-responsive insulin activity by covalent modification with aliphatic phenylboronic acid conjugates.

Danny Hung-Chieh Chou1, Matthew J Webber2, Benjamin C Tang2, Amy B Lin2, Lavanya S Thapa2, David Deng2, Jonathan V Truong2, Abel B Cortinas3, Robert Langer4, Daniel G Anderson4.   

Abstract

Since its discovery and isolation, exogenous insulin has dramatically changed the outlook for patients with diabetes. However, even when patients strictly follow an insulin regimen, serious complications can result as patients experience both hyperglycemic and hypoglycemic states. Several chemically or genetically modified insulins have been developed that tune the pharmacokinetics of insulin activity for personalized therapy. Here, we demonstrate a strategy for the chemical modification of insulin intended to promote both long-lasting and glucose-responsive activity through the incorporation of an aliphatic domain to facilitate hydrophobic interactions, as well as a phenylboronic acid for glucose sensing. These synthetic insulin derivatives enable rapid reversal of blood glucose in a diabetic mouse model following glucose challenge, with some derivatives responding to repeated glucose challenges over a 13-h period. The best-performing insulin derivative provides glucose control that is superior to native insulin, with responsiveness to glucose challenge improved over a clinically used long-acting insulin derivative. Moreover, continuous glucose monitoring reveals responsiveness matching that of a healthy pancreas. This synthetic approach to insulin modification could afford both long-term and glucose-mediated insulin activity, thereby reducing the number of administrations and improving the fidelity of glycemic control for insulin therapy. The described work is to our knowledge the first demonstration of a glucose-binding modified insulin molecule with glucose-responsive activity verified in vivo.

Entities:  

Keywords:  diabetes; glucose sensing; molecular engineering; protein modification; smart therapy

Mesh:

Substances:

Year:  2015        PMID: 25675515      PMCID: PMC4345600          DOI: 10.1073/pnas.1424684112

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


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