Total Synthesis of Caprazol

S. Hirano; S. Ichikawa; A. Matsuda

doi:10.1055/s-2005-865339

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Synfacts 2005(0): 0013-0013
DOI: 10.1055/s-2005-865339

Synthesis of Natural Products and Drugs

Total Synthesis of Caprazol

Contributor(s): Philip Kocienski

S. Hirano, S. Ichikawa, A. Matsuda*
Hokkaido University, Japan
Total Synthesis of Caprazol, a Core Structure of the Caprazamycin Antituberculosis Antibiotics
Angew. Chem. Int. Ed. 2005, 44: 1854-1856

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Publication History

Publication Date:
20 July 2005 (online)

Abstract
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Key words

Sharpless asymmetric amino-hydroxylation - glycosylation - glycosyl fluoride

Significance

Caprazol is the core structure of the Caprazamycin antibiotics. The Caprazamycins are isolated from Streptomyces sp MK730-62F2. They inhibit Mra Y, a key enzyme in peptidoglycan synthesis in Mycobacterium tuberculosis. They have no significant toxicity to mice.

Comment

Key steps in the 18-step synthesis of Caprazol were (a) a Sharpless asymmetric aminohydroxylation reaction which converts A to B; glycosylation using a 5-aminoribosyl fluoride C; and (c) a reductive amination to create the diazepanone ring. The stereochemistry of the difficult glycosylation depended strongly on the steric bulk of the 3-pentylidene protecting group and the Lewis acid activator. With BF₃·OEt₂ at -30 °C, the anomeric ratio was α:β = 4:96.

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