Solid-Phase Synthesis of Triostin A Using a Symmetrical Bis(diphenylmethyl) Linker System

Triostin A is a symmetric bicyclic depsipeptide with very potent antitumoral activity because of its bisintercalation into DNA. In this study, we report a new synthetic strategy that exploits a structural symmetry of triostin A. First, we prepared a novel symmetric linker molecule that is labile und...

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Bibliographic Details
Published inJournal of organic chemistry Vol. 80; no. 15; pp. 7486 - 7494
Main Authors Sable, Ganesh A, Lim, Dongyeol
Format Journal Article
LanguageEnglish
Published WASHINGTON American Chemical Society 07.08.2015
Amer Chemical Soc
Subjects
amino acids
Chemistry
Chemistry, Organic
Cyclization
depsipeptides
Depsipeptides - chemical synthesis
Depsipeptides - chemistry
diketopiperazines
DNA
DNA - chemistry
organic chemistry
Oxidation-Reduction
Physical Sciences
Quinoxalines - chemical synthesis
Quinoxalines - chemistry
Science & Technology
Solid-Phase Synthesis Techniques
Solutions
Sulfhydryl Compounds - chemistry
synthesis
thiols
ORGANIC-SYNTHESIS
CYCLIC PEPTIDE
SEQUENCE SPECIFICITY
N-TETRAMETHYLTRIOSTIN-A
MARINE MICROMONOSPORA
BIFUNCTIONAL INTERCALATION
BISINTERCALATOR NATURAL-PRODUCTS
QUINOXALINE ANTIBIOTICS
ANTITUMOR-ACTIVITY
PEPTIDE-SYNTHESIS
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Summary:Triostin A is a symmetric bicyclic depsipeptide with very potent antitumoral activity because of its bisintercalation into DNA. In this study, we report a new synthetic strategy that exploits a structural symmetry of triostin A. First, we prepared a novel symmetric linker molecule that is labile under mildly acidic conditions and suitable for a solid-phase synthesis procedure. Two Cys units were attached to a linker-resin conjugate via their free thiol groups, and double deprotection and double coupling reactions were then applied to synthesize linear tetradepsipeptides. Subsequently, the key biscyclization of the tetradepsipeptides was performed on the resin, and the resulting cyclic octapeptide was detached from the linker-resin conjugate to give a peptide with two free thiols. Finally, triostin A was obtained by oxidizing the free thiols in solution to produce a disulfide. The yield was improved through exploration of two different solid-phase synthetic approaches under similar strategy. Mainly, this strategy was developed to enable the ease and rapid preparation of libraries of symmetric bicyclic depsipeptides. It also addresses several synthetic problems with our synthesis, including diketopiperazine (DKP) formation, poor cyclization yields and preparation of noncommercial N-methyl amino acids in good yields.
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ISSN:0022-3263
1520-6904
1520-6904
DOI:10.1021/acs.joc.5b01055