Total Synthesis of the Antitumor Depsipeptide FE399 and its S-Benzyl Derivative: A Macrolactamization Approach

Takayuki Tonoi; Miyuki Ikeda; Teruyuki Sato; Takehiko Inohana; Ryo Kawahara; Takatsugu Murata; Isamu Shiina

doi:10.26434/chemrxiv.12017796.v2

Organic Chemistry

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Total Synthesis of the Antitumor Depsipeptide FE399 and its S-Benzyl Derivative: A Macrolactamization Approach

24 March 2020, Version 2

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This content is a preprint and has not undergone peer review at the time of posting.

Abstract

An efficient and practical method for the synthesis of (9R,14R,17R)-FE399, a novel antitumor bicyclic depsipeptide, was developed. A 2-methyl-6-nitrobenzoic anhydride (MNBA)-mediated dehydration condensation reaction was effectively employed for the formation of the 16-membered macrocyclic depsipeptide moiety of FE399. FE399 was found to exist as an inseparable equilibrium mixture of conformational isomers; the mixture was quantitatively transformed into the corresponding S-benzyl product and isolated as a single isomer. Thus, we could confirm that the molecular structure of FE399 obtained by this method is identical to that of the natural product.

Keywords

FE399

Antitumor bicyclic depsipeptide

MNBA

macrolactamization

Supplementary materials

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200324 CoverLett-ChemRxiv

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200324 SI-ChemRxiv (rev)

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