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Ribosome-Targeting Antibiotics: Modes of Action, Mechanisms of Resistance, and Implications for Drug Design

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posted on 2018-10-18, 00:00 authored by Jinzhong Lin, Dejian Zhou, Thomas A. Steitz, Yury S. Polikanov, Matthieu G. Gagnon
Genetic information is translated into proteins by the ribosome. Structural studies of the ribosome and of its complexes with factors and inhibitors have provided invaluable information on the mechanism of protein synthesis. Ribosome inhibitors are among the most successful antimicrobial drugs and constitute more than half of all medicines used to treat infections. However, bacterial infections are becoming increasingly difficult to treat because the microbes have adapted to become resistant to the most effective antibiotics, creating a major public health care threat. This has spurred a renewed interest in structure-function studies of protein synthesis inhibitors and, in few cases, compounds have been developed into potent therapeutic agents against drug-resistant pathogens. In this review, we describe the modes of action of many ribosome-targeting antibiotics, highlight the major resistance mechanisms developed by pathogenic bacteria, and discuss recent advances in structure-assisted design of new molecules.

Funding

We thank Peter B. Moore for critical reading of the manuscript and valuable suggestions. This work was supported by grants from the National Natural Science Foundation of China (No. 31770784) to J.L., the National Institutes of Health (GM022778) to T.A.S., and by Illinois State startup funds to Y.S.P..

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Copyright @ Annual Reviews

Citation

Lin, J., Zhou, D., Steitz, T. A., Polikanov, Y. S., & Gagnon, M. G. (2018) Ribosome-Targeting Antibiotics: Modes of Action, Mechanisms of Resistance, and Implications for Drug Design. In: Vol. 87. Annual Review of Biochemistry (pp. 451-478).

Publisher

Annual Reviews

Language

  • en

issn

0066-4154

Issue date

2018-03-23

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