Literature DB >> 30318461

Tetracyclines Modify Translation by Targeting Key Human rRNA Substructures.

Jonathan D Mortison1, Monica Schenone2, Jacob A Myers1, Ziyang Zhang1, Linfeng Chen1, Christie Ciarlo2, Eamon Comer2, S Kundhavai Natchiar3, Steven A Carr2, Bruno P Klaholz3, Andrew G Myers4.   

Abstract

Apart from their antimicrobial properties, tetracyclines demonstrate clinically validated effects in the amelioration of pathological inflammation and human cancer. Delineation of the target(s) and mechanism(s) responsible for these effects, however, has remained elusive. Here, employing quantitative mass spectrometry-based proteomics, we identified human 80S ribosomes as targets of the tetracyclines Col-3 and doxycycline. We then developed in-cell click selective crosslinking with RNA sequence profiling (icCL-seq) to map binding sites for these tetracyclines on key human rRNA substructures at nucleotide resolution. Importantly, we found that structurally and phenotypically variant tetracycline analogs could chemically discriminate these rRNA binding sites. We also found that tetracyclines both subtly modify human ribosomal translation and selectively activate the cellular integrated stress response (ISR). Together, the data reveal that targeting of specific rRNA substructures, activation of the ISR, and inhibition of translation are correlated with the anti-proliferative properties of tetracyclines in human cancer cell lines.
Copyright © 2018 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  RNA-seq; chemoproteomics; diazirine; photocrosslinking; ribosome; target identification; tetracyclines; translation

Mesh:

Substances:

Year:  2018        PMID: 30318461      PMCID: PMC6309532          DOI: 10.1016/j.chembiol.2018.09.010

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


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