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Tongtong Lin, Jiao Pan, Colin Gregory, Yaohai Wang, Clayton Tincher, Caitlyn Rivera, Michael Lynch, Hongan Long, Yu Zhang. 2023: Contribution of the SOS response and the DNA repair systems to norfloxacin induced mutations in E. coli. Marine Life Science & Technology, 5(4): 538-550. DOI: 10.1007/s42995-023-00185-y
Citation: Tongtong Lin, Jiao Pan, Colin Gregory, Yaohai Wang, Clayton Tincher, Caitlyn Rivera, Michael Lynch, Hongan Long, Yu Zhang. 2023: Contribution of the SOS response and the DNA repair systems to norfloxacin induced mutations in E. coli. Marine Life Science & Technology, 5(4): 538-550. DOI: 10.1007/s42995-023-00185-y

Contribution of the SOS response and the DNA repair systems to norfloxacin induced mutations in E. coli

  • Antibiotic-resistant bacteria severely threaten human health. Besides spontaneous mutations generated by endogenous factors, the resistance might also originate from mutations induced by certain antibiotics, such as the fluoroquinolones. Such antibiotics increase the genome-wide mutation rate by introducing replication errors from the SOS response pathway or decreasing the efficiency of the DNA repair systems. However, the relative contributions of these molecular mechanisms remain unclear, hindering understanding of the generation of resistant pathogens. Here, using newly-accumulated mutations of wild-type and SOS-uninducible Escherichia coli strains, as well as those of the strains deficient for the mismatch repair (MMR) and the oxidative damage repair pathways, we find that the SOS response is the major mutagenesis contributor in mutation elevation, responsible for ~ 30–50% of the total base-pair substitution (BPS) mutation-rate elevation upon treatment with sublethal levels of norfloxacin (0 ~ 50 ng/mL). We further estimate the significance of the effects on other mutational features of these mechanisms (i.e., transversions, structural variations, and mutation spectrum) in E. coli using linear models. The SOS response plays a positive role in all three mutational features (mutation rates of BPSs, transversions, structural variations) and affects the mutational spectrum. The repair systems significantly reduce the BPS mutation rate and the transversion rate, regardless of whether antibiotics are present, while significantly increasing the structural variation rate in E. coli. Our results quantitatively disentangle the contributions of the SOS response and DNA repair systems in antibiotic-induced mutagenesis.
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