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Literature DB >> 30595437

The Translation Inhibitor Rocaglamide Targets a Bimolecular Cavity between eIF4A and Polypurine RNA.

Shintaro Iwasaki¹, Wakana Iwasaki², Mari Takahashi², Ayako Sakamoto², Chiduru Watanabe³, Yuichi Shichino⁴, Stephen N Floor⁵, Koichi Fujiwara⁶, Mari Mito⁴, Kosuke Dodo⁷, Mikiko Sodeoka⁷, Hiroaki Imataka⁸, Teruki Honma³, Kaori Fukuzawa⁹, Takuhiro Ito¹⁰, Nicholas T Ingolia¹¹.

Abstract

A class of translation inhibitors, exemplified by the natural product rocaglamide A (RocA), isolated from Aglaia genus plants, exhibits antitumor activity by clamping eukaryotic translation initiation factor 4A (eIF4A) onto polypurine sequences in mRNAs. This unusual inhibitory mechanism raises the question of how the drug imposes sequence selectivity onto a general translation factor. Here, we determined the crystal structure of the human eIF4A1⋅ATP analog⋅RocA⋅polypurine RNA complex. RocA targets the "bi-molecular cavity" formed characteristically by eIF4A1 and a sharply bent pair of consecutive purines in the RNA. Natural amino acid substitutions found in Aglaia eIF4As changed the cavity shape, leading to RocA resistance. This study provides an example of an RNA-sequence-selective interfacial inhibitor fitting into the space shaped cooperatively by protein and RNA with specific sequences.

Entities: CellLine Chemical Disease Gene Species

Keywords: FMO; Ribo-Seq; Rocaglamide; X-ray; crystal structure; eIF4A; evolution; ribosome profiling; sequence specificity; translation

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Substances：

Year: 2018 PMID： 30595437 PMCID： PMC6386617 DOI： 10.1016/j.molcel.2018.11.026

Source DB: PubMed Journal: Mol Cell ISSN： 1097-2765 Impact factor: 17.970

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Cited

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