Efficient syntheses of benzothiazepines as antagonists for the mitochondrial sodium-calcium exchanger: potential therapeutics for type II diabetes

Pei, Yazhong ; Lilly, Michael J. ; Owen, David J. ; D'Souza, Lawrence J. ; Tang, Xiao-Qing ; Yu, Jinghua ; Nazarbaghi, Ramina ; Hunter, Andrew ; Anderson, Christen M. ; Glasco, Susan ; Ede, Nicholas J. ; James, Ian W. ; Maitra, Uday ; Chandrasekaran, S. ; Moos, Walter H. ; Ghosh, Soumitra S. (2003) Efficient syntheses of benzothiazepines as antagonists for the mitochondrial sodium-calcium exchanger: potential therapeutics for type II diabetes Journal of Organic Chemistry, 68 (1). pp. 92-103. ISSN 0022-3263

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Official URL: http://pubs.acs.org/doi/abs/10.1021/jo020446t

Related URL: http://dx.doi.org/10.1021/jo020446t

Abstract

Type II diabetes mellitus is a chronic metabolic disorder that can lead to serious cardiovascular, renal, neurologic, and retinal complications. While several drugs are currently prescribed to treat type II diabetes, their efficacy is limited by mechanism-related side effects (weight gain, hypoglycemia, gastrointestinal distress), inadequate efficacy for use as monotherapy, and the development of tolerance to the agents. Consequently, combination therapies are frequently employed to effectively regulate blood glucose levels. We have focused on the mitochondrial sodium-calcium exchanger (mNCE) as a novel target for diabetes drug discovery. We have proposed that inhibition of the mNCE can be used to regulate calcium flux across the mitochondrial membrane, thereby enhancing mitochondrial oxidative metabolism, which in turn enhances glucose-stimulated insulin secretion (GSIS) in the pancreatic β-cell. In this paper, we report the facile synthesis of benzothiazepines and derivatives by S-alkylation using 2-aminobenzhydrols. The syntheses of other bicyclic analogues based on benzothiazepine, benzothiazecine, benzodiazecine, and benzodiazepine templates are also described. These compounds have been evaluated for their inhibition of mNCE activity, and the results from the structure-activity relationship (SAR) studies are discussed.

Item Type:Article
Source:Copyright of this article belongs to American Chemical Society.
ID Code:7203
Deposited On:25 Oct 2010 12:11
Last Modified:28 May 2011 11:10

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