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Design and synthesis of herboxidiene derivatives that potently inhibit in vitro splicing.


ABSTRACT: Herboxidiene is a potent antitumor agent that targets the SF3B subunit of the spliceosome. Herboxidiene possesses a complex structural architecture with nine stereocenters and design of potent less complex structures would be of interest as a drug lead as well as a tool for studying SF3B1 function in splicing. We investigated a number of C-6 modified herboxidiene derivatives in an effort to eliminate this stereocenter and, also to understand the importance of this functionality. The syntheses of structural variants involved a Suzuki-Miyaura cross-coupling reaction as the key step. The functionalized tetrahydrofuran core has been constructed from commercially available optically active tri-O-acetyl-d-glucal. We investigated the effect of these derivatives on splicing chemistry. The C-6 alkene derivative showed very potent splicing inhibitory activity similar to herboxidiene. Furthermore, the C-6 gem-dimethyl derivative also exhibited very potent in vitro splicing inhibitory activity comparable to herboxidiene.

SUBMITTER: Ghosh AK 

PROVIDER: S-EPMC8911528 | biostudies-literature | 2021 Feb

REPOSITORIES: biostudies-literature

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Design and synthesis of herboxidiene derivatives that potently inhibit <i>in vitro</i> splicing.

Ghosh Arun K AK   Allu Srinivasa Rao SR   Reddy Guddeti Chandrashekar GC   Lopez Adriana Gamboa AG   Mendez Patricia P   Jurica Melissa S MS  

Organic & biomolecular chemistry 20210201 6


Herboxidiene is a potent antitumor agent that targets the SF3B subunit of the spliceosome. Herboxidiene possesses a complex structural architecture with nine stereocenters and design of potent less complex structures would be of interest as a drug lead as well as a tool for studying SF3B1 function in splicing. We investigated a number of C-6 modified herboxidiene derivatives in an effort to eliminate this stereocenter and, also to understand the importance of this functionality. The syntheses of  ...[more]

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