Rapid Identification of Subtype-Selective Agonists of the Somatostatin Receptor Through Combinatorial Chemistry

Author:

Rohrer Susan P.1,Birzin Elizabeth T.1,Mosley Ralph T.1,Berk Scott C.1,Hutchins Steven M.1,Shen Dong-Ming1,Xiong Yusheng1,Hayes Edward C.1,Parmar Rupa M.1,Foor Forrest1,Mitra Sudha W.1,Degrado Sylvia J.1,Shu Min1,Klopp John M.1,Cai Sheng-Jian1,Blake Allan1,Chan Wanda W. S.1,Pasternak Alex1,Yang Lihu1,Patchett Arthur A.1,Smith Roy G.1,Chapman Kevin T.1,Schaeffer James M.1

Affiliation:

1. S. P. Rohrer, E. T. Birzin, E. C. Hayes, R. M. Parmar, F. Foor, S. W. Mitra, S.-J. Cai, A. Blake, W. W. S. Chan, R. G. Smith, J. M. Schaeffer, Department of Cell Biochemistry and Physiology, Merck Research Laboratories, Post Office Box 2000, Rahway, NJ 07065, USA. R. T. Mosley, S. C. Berk, S. M. Hutchins, D.-M. Shen, Y. Xiong, S. J. Degrado, M. Shu, J. M. Klopp, K. T. Chapman, Department of Molecular Design and Diversity, Merck Research Laboratories, Post Office Box 2000, Rahway, NJ 07065, USA. A....

Abstract

Nonpeptide agonists of each of the five somatostatin receptors were identified in combinatorial libraries constructed on the basis of molecular modeling of known peptide agonists. In vitro experiments using these selective compounds demonstrated the role of the somatostatin subtype-2 receptor in inhibition of glucagon release from mouse pancreatic alpha cells and the somatostatin subtype-5 receptor as a mediator of insulin secretion from pancreatic beta cells. Both receptors regulated growth hormone release from the rat anterior pituitary gland. The availability of high-affinity, subtype-selective agonists for each of the somatostatin receptors provides a direct approach to defining their physiological functions.

Publisher

American Association for the Advancement of Science (AAAS)

Subject

Multidisciplinary

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