KU-32, a Novel Drug for Diabetic Neuropathy, Is Safe for Human Islets and ImprovesIn VitroInsulin Secretion and Viability

Author:

Farmer Kevin1,Williams S. Janette2,Novikova Lesya2,Ramachandran Karthik2,Rawal Sonia2,Blagg Brian S. J.3,Dobrowsky Rick1,Stehno-Bittel Lisa2

Affiliation:

1. Department of Pharmacology and Toxicology, University of Kansas, 5064 Malott Hall, Lawrence, KS 66045, USA

2. Department of Physical Therapy and Rehabilitation Science, University of Kansas Medical Center, MS 2002, Kansas City, KS 66160, USA

3. Department of Medicinal Chemistry, University of Kansas, Lawrence, KS 66045, USA

Abstract

KU-32 is a novel, novobiocin-based Hsp90 inhibitor that protects against neuronal glucotoxicity and reverses multiple clinical indices of diabetic peripheral neuropathy in a rodent model. However, any drug with potential for treating diabetic complications must also have no adverse effects on the function of pancreatic islets. Thus, the goal of the current study was to assess the effect of KU-32 on thein vitroviability and function of human islets. Treating human islets with KU-32 for 24 hours showed no toxicity as assessed using the alamarBlue assay. Confocal microscopy confirmed that with a minimum of 2-day exposure, KU-32 improved cellular viability by blocking apoptosis. Functionally, isolated human islets released more glucose-stimulated insulin when preincubated in KU-32. However, diabetic BKS-db/db mice, a model for type 2 diabetes, administered KU-32 for 10 weeks did not show any significant changes in blood glucose and insulin levels, despite having greater insulin staining/beta cell in the pancreas compared to untreated BKS db/db mice. In summary, KU-32 did not harm isolated human islets and may even be protective. However, the effect does not appear significant enough to alter thein vivometabolic parameters of diabetic mice.

Funder

National Institutes of Health

Publisher

Hindawi Limited

Subject

General Medicine,Endocrinology, Diabetes and Metabolism

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