Optimization of the 4-aryl group of 4-aryl-pyridine glucagon antagonists: Development of an efficient, alternative synthesis

Roger A. Smith; Donald L. Hertzog; Martin H. Osterhout; Gaetan H. Ladouceur; Mary Korpusik; Mark A. Bobko; J. Howard Jones; Kathleen Phelan; Romulo H. Romero; Thomas Hundertmark; Margit L. MacDougall; James N. Livingston; William R. Schoen

Journal Article

Optimization of the 4-aryl group of 4-aryl-pyridine glucagon antagonists: Development of an efficient, alternative synthesis

Bioorganic and Medicinal Chemistry Letters (2002) 12(9) 1303-1306

DOI: 10.1016/S0960-894X(02)00143-9

17Citations

8Readers

Get full text

Abstract

A narrow structure-activity relationship was established for the 4-aryl group in 4-aryl-pyridine glucagon antagonists, with only small substituents being well-tolerated, and only at the 3′- and 4′-positions. However, substitution with a 2′-hydroxy group gave a ca. 3-fold increase in activity (e.g., 4′-fluoro-2′-hydroxy analogue 33, IC50=190 nM). For efficient preparation of 2′-substituted phenylpyridines, a novel synthesis via pyrones and 4-methoxy-pyridines was developed. © 2002 Elsevier Science Ltd. All rights reserved.

Cite

CITATION STYLE

APA

Smith, R. A., Hertzog, D. L., Osterhout, M. H., Ladouceur, G. H., Korpusik, M., Bobko, M. A., … Schoen, W. R. (2002). Optimization of the 4-aryl group of 4-aryl-pyridine glucagon antagonists: Development of an efficient, alternative synthesis. Bioorganic and Medicinal Chemistry Letters, 12(9), 1303–1306. https://doi.org/10.1016/S0960-894X(02)00143-9

Optimization of the 4-aryl group of 4-aryl-pyridine glucagon antagonists: Development of an efficient, alternative synthesis

Abstract

Cite

Register to see more suggestions