uORF-mediated riboregulation controls transcription of whiB7/wblC antibiotic resistance gene
- Authors
- Lee, Ju-Hyung; Lee, Eun-Jin; Roe, Jung-Hye
- Issue Date
- 1월-2022
- Publisher
- WILEY
- Keywords
- antibiotic resistance; antiterminator; Mycobacterium; Streptomyces; transcription attenuation
- Citation
- MOLECULAR MICROBIOLOGY, v.117, no.1, pp.179 - 192
- Indexed
- SCIE
SCOPUS
- Journal Title
- MOLECULAR MICROBIOLOGY
- Volume
- 117
- Number
- 1
- Start Page
- 179
- End Page
- 192
- URI
- https://scholar.korea.ac.kr/handle/2021.sw.korea/136654
- DOI
- 10.1111/mmi.14834
- ISSN
- 0950-382X
- Abstract
- WhiB7/WblC is a transcriptional factor of actinomycetes conferring intrinsic resistance to multiple translation-inhibitory antibiotics. It positively autoregulates its own transcription in response to the same antibiotics. The presence of a uORF and a potential Rho-independent transcription terminator in the 5 ' leader region has suggested a possibility that the whiB7/wblC gene is regulated via a uORF-mediated transcription attenuation. However, experimental evidence for the molecular mechanism to explain how antibiotic stress suppresses the attenuator, if any, and induces transcription of the whiB7/wblC gene has been lacking. Here we report that the 5 ' leader sequences of the whiB7/wblC genes in sub-clades of actinomycetes include conserved antiterminator RNA structures. We confirmed that the putative antiterminator in the whiB7/wblC leader sequences of both Streptomyces and Mycobacterium indeed suppresses Rho-independent transcription terminator and facilitates transcription readthrough, which is required for WhiB7/WblC-mediated antibiotic resistance. The antibiotic-mediated suppression of the attenuator can be recapitulated by amino acid starvation, indicating that translational inhibition of uORF by multiple signals is a key to induce whiB7/wblC expression. Our findings of a mechanism leading to intrinsic antibiotic resistance could provide an alternative to treat drug-resistant mycobacteria.
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