Rifampicin is a clinically important antibiotic that binds to, and blocks the DNA/RNA channel of bacterial RNA polymerase (RNAP). Stalled, nonfunctional RNAPs can be removed from DNA by HelD proteins; this is important for maintenance of genome integrity. Recently, it was reported that HelD proteins from high G+C Actinobacteria, called HelR, are able to dissociate rifampicin-stalled RNAPs from DNA and provide rifampicin resistance. This is achieved by the ability of HelR proteins to dissociate rifampicin from RNAP. The HelR-mediated mechanism of rifampicin resistance is discussed here, and the roles of HelD/HelR in the transcriptional cycle are outlined. Moreover, the possibility that the structurally similar HelD proteins from low G+C Firmicutes may be also involved in rifampicin resistance is explored. Finally, the discovery of the involvement of HelR in rifampicin resistance provides a blueprint for analogous studies to reveal novel mechanisms of bacterial antibiotic resistance.
What the Hel: recent advances in understanding rifampicin resistance in bacteria.
真相:细菌利福平耐药性研究的最新进展
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作者:Sudzinová Petra, Å anderová Hana, Koval' Tomáš, Skálová Tereza, Borah Nabajyoti, Hnilicová Jarmila, Kouba Tomáš, Dohnálek Jan, Krásný Libor
| 期刊: | FEMS Microbiology Reviews | 影响因子: | 12.300 |
| 时间: | 2023 | 起止号: | 2023 Nov 1; 47(6):fuac051 |
| doi: | 10.1093/femsre/fuac051 | 研究方向: | 微生物学 |
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