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针对口服活性肾素抑制剂设计的研究。1. 影响小肽吸收的一些因素。

Studies directed toward the design of orally active renin inhibitors. 1. Some factors influencing the absorption of small peptides.

作者信息

Rosenberg S H, Spina K P, Woods K W, Polakowski J, Martin D L, Yao Z, Stein H H, Cohen J, Barlow J L, Egan D A

机构信息

Abbott Laboratories, Cardiovascular Research Division, Abbott Park, Illinois 60064.

出版信息

J Med Chem. 1993 Feb 19;36(4):449-59. doi: 10.1021/jm00056a005.

Abstract

A systematic evaluation of structure-absorption relationships using a high throughput intraduodenal rat screening model has led to the delineation of a set of structural parameters that appear to govern bioavailability in a series of peptide-based renin inhibitors. Optimum structures, exemplified by 25 and 41, incorporated a single, solubilizing substituent at the C- or N-terminus combined with a lipophilic P2-site residue. Both inhibitors gave unprecedented plasma drug levels upon intraduodenal administration to monkeys, and the calculated bioavailability for 41 (14 +/- 4%) is the highest reported for any peptidic renin inhibitor.

摘要

使用高通量十二指肠内大鼠筛选模型对结构-吸收关系进行系统评估,已确定了一组结构参数,这些参数似乎决定了一系列基于肽的肾素抑制剂的生物利用度。以25和41为代表的最佳结构在C端或N端并入了一个单一的增溶取代基,并结合了一个亲脂性的P2位点残基。将这两种抑制剂十二指肠内给药于猴子后,均产生了前所未有的血浆药物水平,并且计算得出的41的生物利用度(14±4%)是所有肽类肾素抑制剂中报道的最高值。

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