Vanadium(II)- and niobium(III)-induced, diastereoselective pinacol coupling of peptide aldehydes to give a C-2-symmetrical HIV protease inhibitor

被引：54

作者：

Kammermeier, B ^{[1
]}

Beck, G ^{[1
]}

Holla, W ^{[1
]}

Jacobi, D ^{[1
]}

Napierski, B ^{[1
]}

Jendralla, H ^{[1
]}

机构：

[1] LANDES ENTWICKLUNGS GESELLSCH, D-70182 STUTTGART, GERMANY

来源：

CHEMISTRY-A EUROPEAN JOURNAL | 1996年 / 2卷 / 03期

关键词：

enzyme inhibitors; niobium complexes; peptide aldehydes; pinacol coupling; vanadium complexes;

D O I：

10.1002/chem.19960020312

中图分类号：

O6 [化学];

学科分类号：

0703 ;

摘要：

Peptide aldehydes 15 a-c are prepared without epimerization from enantiomerically pure (S)-alpha-amino acids (Scheme 3), Reductive pinacol homocoupling of 15 a-c, induced by vanadium complex 11 or niobium complex 16 in refluxing THF, yields C-2-symmetrical (S,R,R,S)-configurated 6 a, 6 b and 2, respectively, with moderate to high stereoselectivity (Scheme 4), In a novel protocol for the preparation and utilization of THF solutions of 11, the isolation of air-sensitive intermediates can be avoided and the potent HIV protease inhibitor 2 prepared in enantio- and diastereomerically pure form on a kilogram scale without chromatographic purification. The (S,R,R,S) selectivity of the pinacol homocouplings is confirmed by means of an independent, stereochemically unequivocal synthesis of 6 a and 2 from D-mannitol 4 (Scheme 1).

引用

页码：307 / 315

页数：9

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