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有机化学
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有机化学 ›› 2008, Vol. 28 ›› Issue (03): 511-514. 上一篇    下一篇

研究简报

奈必洛尔的不对称合成

余婧,张稳稳,李映红,李盛男,何菱*   

  1. (四川大学华西药学院 靶向药物教育部重点实验室 成都 610041)
  • 收稿日期:2007-03-28 修回日期:2007-08-22 发布日期:2008-03-18
  • 通讯作者: 何菱

Asymmetric Synthesis of Nebivolol

YU Jing,ZHANG Wen-Wen,LI Ying-Hong,LI Sheng-Nan,HE Ling*   

  1. (Key Laboratory of Drug-Targeting, Ministry of Education, West China School of Pharmacy, Si-chuan University,
    Chengdu 610041)
  • Received:2007-03-28 Revised:2007-08-22 Published:2008-03-18
  • Contact: HE Ling

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1474

被引次数

6

首先合成4-氟-2-(5-羟基戊烷基-3-烯)-苯酚(2), 再经Sharpless不对称环氧化等反应分别得到2-氨基-1-[6-氟- (2S)-3,4-二氢-2H-2-苯并吡喃]-(1R)-1-乙醇(6)和6-氟-2-[(2R)-2-环氧乙烷基]-(2R)-3,4-二氢苯并吡喃(10). 最后, 610发生亲核开环反应即得到目标产物奈比洛尔. 整个合成路线简单易行, 并在原有文献的基础上有较大改进, 使收率大大提高, 总收率由文献的2.1%提高到14.1%.

关键词: 奈必洛尔, Sharpless不对称环氧化, 抗高血压药

The convenient enantioselective synthesis of nebivolol (1) was described. The key steps of this total synthesis were based on a Sharpless asymmetric epoxidation methodology employing 4-fluoro-2-(5- hydroxypent-3-enyl)phenol (2) as a substrate and the efficient formation of (2S,1R)-2-(2-amino-1-hydroxy ethyl)-6-fluorochroman (6) and (R,R)-6-fluoro-2-oxiranyl-chroman (10). Simultaneously, the approach was inves-tigated for the nucleophilic ring opening of epoxide 10. Finally, 10 was afforded in an ex-cellent yield and the ring cleavage of 10 led to the formation of 1 in a 14.1% overall yield over steps after optimization of the steps which accompanied a 2.1% overall yield in literature.

Key words: Sharpless asymmetric epoxidation, nebivolol, hypertensive agent