Literature DB >> 28457705

Inhibition of Eukaryotic Translation by the Antitumor Natural Product Agelastatin A.

Brandon McClary1, Boris Zinshteyn2, Mélanie Meyer3, Morgan Jouanneau4, Simone Pellegrino3, Gulnara Yusupova3, Anthony Schuller2, Jeremy Chris P Reyes5, Junyan Lu6, Zufeng Guo1, Safiat Ayinde1, Cheng Luo6, Yongjun Dang7, Daniel Romo8, Marat Yusupov9, Rachel Green10, Jun O Liu11.   

Abstract

Protein synthesis plays an essential role in cell proliferation, differentiation, and survival. Inhibitors of eukaryotic translation have entered the clinic, establishing the translation machinery as a promising target for chemotherapy. A recently discovered, structurally unique marine sponge-derived brominated alkaloid, (-)-agelastatin A (AglA), possesses potent antitumor activity. Its underlying mechanism of action, however, has remained unknown. Using a systematic top-down approach, we show that AglA selectively inhibits protein synthesis. Using a high-throughput chemical footprinting method, we mapped the AglA-binding site to the ribosomal A site. A 3.5 Å crystal structure of the 80S eukaryotic ribosome from S. cerevisiae in complex with AglA was obtained, revealing multiple conformational changes of the nucleotide bases in the ribosome accompanying the binding of AglA. Together, these results have unraveled the mechanism of inhibition of eukaryotic translation by AglA at atomic level, paving the way for future structural modifications to develop AglA analogs into novel anticancer agents.
Copyright © 2017 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  agelastatin A; brain cancer; chemical footprinting; drug design; marine alkaloid; molecular docking; peptidyl transferase center; rRNA seq; ribosome; translation elongation

Mesh:

Substances:

Year:  2017        PMID: 28457705      PMCID: PMC5562292          DOI: 10.1016/j.chembiol.2017.04.006

Source DB:  PubMed          Journal:  Cell Chem Biol        ISSN: 2451-9448            Impact factor:   8.116


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