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Total Synthesis and Structural Revision of Clavilactone D.

Ken-Ichi TakaoRyuichi NemotoKento MoriAyumi NambaKeisuke YoshidaAkihiro Ogura
Published in: Chemistry (Weinheim an der Bergstrasse, Germany) (2017)
A structural revision of clavilactone D, a potent inhibitor of protein tyrosine kinases, was achieved by total syntheses of two newly proposed structures. The syntheses relied on ring-opening/ring-closing metathesis, which transformed a cyclobutenecarboxylate into a γ-butenolide. The syntheses confirmed that the correct structure of clavilactone D has an amino group at C-3 instead of a hydroxy group at C-2 in the originally proposed structure.
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