SpecificgyrAgene mutations correlate with high prevalence of discordant levofloxacin resistance inMycobacterium tuberculosisisolates from Beijing, China

Author:

Huo Fengmin,Ma Yifeng,Li Shanshan,Xue Yi,Shang Yuanyuan,Dong Lingling,Li Yunxu,Pang YuORCID

Abstract

ABSTRACTAlthough molecular diagnostics are highly sensitive in the diagnosis of fluroquinolone (FQ)-resistant tuberculosis (TB), the discordant results with the sequential phenotypic drug susceptibility testing (DST) invariably occur. To investigate the prevalence and the cause of discordant results between molecular and phenotypic DST for levofloxacin (LFX), the cases who were determined to be LFX-susceptible using the phenotypic DST but LFX-resistant using the MeltPro assay were retrospectively reviewed in Beijing, China. We measured LFX minimal inhibitory concentrations (MICs) using Middlebrook 7H9 broth. Sanger sequencing was used to determine genotypic characteristics of discordant isolates. Between January and December 2018, 126 (22.1%) out of 571 smear-positive TB patients were identified as LFX-resistant TB by MeltPro assay. Among the 126 LFX-resistant TB, there were 34 isolates identified as LFX-susceptible TB by phenotypical DST. This result demonstrated a discordance prevalence of 27.0%. LFX MICs were majorly centered around the critical concentration, and 7 (21.2%) and 13 (39.4%) had MICs of 2.0 mg/l and 4.0 mg/l, respectively. The most prevalent mutations conferring discordant LFX resistance were the amino acid substitutions of Ser to Leu in 90 codon (13, 39.4%) and Asp to Ala in 94 codon ofgyrA(11, 33.3mg/l belonged to Ala90Val and Asp94Ala group. In conclusion, our data demonstrate that more than one quarter of LFX-resistant isolates by molecular method are susceptible to LFX using the phenotypic DST. The high prevalence of discordant LFX resistance is majorly due to the isolates with specific mutations withingyrAgene conferring proximity of MICs to the critical concentration.

Publisher

Cold Spring Harbor Laboratory

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1. Stepwise selection of mutation conferring fluroquinolone resistance: multisite MDR-TB cohort study;European Journal of Clinical Microbiology & Infectious Diseases;2021-02-18

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