STUDIES TOWARD THE LARGE-SCALE SYNTHESIS OF THE HIV PROTEINASE-INHIBITOR RO-31-8959

被引：119

作者：

PARKES, KEB

BUSHNELL, DJ

CRACKETT, PH

DUNSDON, SJ

FREEMAN, AC

GUNN, MP

HOPKINS, RA

LAMBERT, RW

MARTIN, JA

MERRETT, JH

REDSHAW, S

SPURDEN, WC

THOMAS, GJ

机构：

[1] Roche Products Limited, Hertfordshire AL7 3AY, 40 Broadwater Road, Welwyn Garden City

来源：

JOURNAL OF ORGANIC CHEMISTRY | 1994年 / 59卷 / 13期

关键词：

D O I：

10.1021/jo00092a026

中图分类号：

O62 [有机化学];

学科分类号：

070303 ; 081704 ;

摘要：

Ro 31-8959 (1), a potent and selective inhibitor of HIV proteinase, is currently in phase III clinical trials. Six approaches for the large-scale synthesis of this compound have been studied. All routes employ an initial disconnection to an electrophilic L-phenylalanine homologue equivalent 13 and the decahydroisoquinoline derivative 5. They differ in adopting either an epoxide, a cyclic sulfate, or an aldehyde as the electrophilic entity and develop chirality from L-phenylalanine, dimethyl D-tartrate, or a Sharpless epoxidation. The preferred route starts from N-phthaloyl-L-phenylalaninyl chloride and uses tris((trimethylsilyl)oxy)ethene to effect homologation to hydroxy ketone 30, which is elaborated in a five-step two-pot procedure to N-phthaloyl epoxide 33 and hence 1. Kilogram quantities of Ro 31-8959 have been prepared using this route.

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页码：3656 / 3664

页数：9

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