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DOI: 10.1055/s-0030-1254126
© Georg Thieme Verlag KG Stuttgart · New York
Brevinin-2-related Peptide and its [D4K] Analogue Stimulate Insulin Release In Vitro and Improve Glucose Tolerance in Mice Fed a High Fat Diet
Publication History
received 05.03.2010
accepted 28.04.2010
Publication Date:
21 May 2010 (online)
Abstract
The cationic, α-helical frog skin antimicrobial peptide B2RP (brevinin-2-related peptide) shows sequence similarity to antimicrobial peptides belonging to the brevinin-2 family, but lacks the C-terminal cyclic heptapeptide domain (Cys-Lys-Xaa4-Cys). Synthetic B2RP produced a significant (p<0.05) stimulation of insulin release (148% of basal rate at a concentration of 1 μM with a maximum response of 222% of basal rate at a concentration of 3 μM) from BRIN-BD11 clonal β-cells without increasing the release of the cytosolic enzyme, lactate dehydrogenase. Increasing cationicity of B2RP while maintaining amphipathicity by the substitution Asp4 → Lys enhanced the insulin-releasing potency (137% of basal rate at a concentration of 0.3 μM; p<0.05) with no stimulation of lactate dehydrogenase release. In contrast, the L18K, and D4K, L18K analogues were toxic to the cells, and the K16A analogue, with increased amphipathicity and hydrophobicity, showed reduced potency. Administration of [D4K]B2RP (100 nmol/kg body weight) to mice fed a high fat diet to induce obesity and insulin-resistance significantly (p<0.05) enhanced insulin release and improved glucose tolerance during the 60-minute period following an intraperitoneal glucose load (18 mmol/kg body weight). B2RP shows potential for development into an agent for the treatment of type 2 diabetes.
Key words
incretin peptide - frog skin - type 2 diabetes
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Correspondence
J. M. Conlon
Department of Biochemistry
Faculty of Medicine and Health
Sciences
United Arab Emirates University
17666 Al-Ain
UAE
Phone: +971/3/713 7484
Fax: +971/3/767 2033
Email: jmconlon@uaeu.ac.ae