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Literature DB >> 24359706

Second-generation derivatives of the eukaryotic translation initiation inhibitor pateamine A targeting eIF4A as potential anticancer agents.

Woon-Kai Low¹, Jing Li², Mingzhao Zhu², Sai Shilpa Kommaraju³, Janki Shah-Mittal³, Ken Hull², Jun O Liu⁴, Daniel Romo⁵.

Abstract

A series of pateamine A (1) derivatives were synthesized for structure/activity relationship (SAR) studies and a selection of previous generation analogs were re-evaluated based on current information regarding the mechanism of action of these translation inhibitors. Structural modifications in the new generation of derivatives focused on alterations to the C19-C22 Z,E-diene and the trienyl side chain of the previously described simplified, des-methyl, des-amino pateamine A (DMDAPatA, 2). Derivatives were tested for anti-proliferative activity in cell culture and for inhibition of mammalian cap-dependent translation in vitro. Activity was highly dependent on the rigidity and conformation of the macrolide and the functionality of the side chain. The only well tolerated substitutions were replacement of the N,N-dimethyl amino group found on the side chain of 2 with other tertiary amine groups. SAR reported here suggests that this site may be modified in future studies to improve serum stability, cell-type specificity, and/or specificity towards rapidly proliferating cells.

Entities: CellLine Chemical Disease Gene Species

Keywords: DMDAPatA; Pateamine A; Stille coupling; Translation initiation; eIF4A

Mesh：

Substances：

Year: 2013 PMID： 24359706 PMCID： PMC3958936 DOI： 10.1016/j.bmc.2013.11.046

Source DB: PubMed Journal: Bioorg Med Chem ISSN： 0968-0896 Impact factor: 3.641

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