Synthesis of (+)-Cortistatin A

Ryan A. Shenvi, Carlos A. Guerrero, Jun Shi, Chuang-Chuang Li and Phil S. Baran
Department of Chemistry, The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, California 92037
J. Am. Chem. Soc., 2008, 130 (23), pp 7241–7243
DOI: 10.1021/ja8023466
Publication Date (Web): May 14, 2008
Copyright © 2008 American Chemical Society
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Abstract

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Cortistatin A is a marine steroid with highly selective and perhaps mechanistically unique antiangiogenic activity. Herein we report a synthesis of this natural product by way of “cortistatinone”, an intermediate ideally suited for investigating the key pharmacophore of the cortistatin family. The synthesis begins with a terrestrial steroid and traverses a route to cortistatin A through the discovery of unique chemical reactivity. Specifically, we demonstrate the first example of a directed, geminal C−H bisoxidation, a new fragmentation cascade to access expanded B-ring steroid systems, a chemoselective cyclization to install the hallmark oxabicycle of the cortistatin family, and a remarkably selective hydrogenation reaction, which should find extensive use in future syntheses of the cortistatins and designed analogues. The synthesis displays a level of brevity, efficiency, and practicality that will be crucial in evaluating the medicinal potential of this fascinating class of marine steroids.

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History

  • Published In Issue June 11, 2008
  • Article ASAPMay 14, 2008
  • Received: March 31, 2008

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