DESIGNING PEPTIDE MIMETICS

被引：78

作者：

MOORE, GJ

机构：

[1] University of Calgary, Calgary, Alta. T2N 4N1

来源：

TRENDS IN PHARMACOLOGICAL SCIENCES | 1994年 / 15卷 / 04期

关键词：

D O I：

10.1016/0165-6147(94)90049-3

中图分类号：

R9 [药学];

学科分类号：

1007 [药学];

摘要：

During this century, the nonpeptidic families of hormones (for example, steroids and catecholamines) have been exploited by medicinal chemists to give an array of clinically important drugs. Although peptides represent the largest class of hormonal substances, they are limited in their potential for treating a variety of diseases because of their lack of oral bioavailability and their shout durations of action resulting from enzymic degradation in vivo. Recently, rapid screening of small molecule libraries anti rational design approaches have produced peptide mimetics as a new generation of promising drug leads. In this review, Graham Moore provides some insight into aspects of the rational design approach to peptide mimicry using angiotensin II as an example.

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页码：124 / 129

页数：6

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