Towards clinical breakpoints for non-tuberculous mycobacteria – Determination of epidemiological cut off values for the Mycobacterium avium complex and Mycobacterium abscessus using broth microdilution

肉汤微量稀释 脓肿分枝杆菌 阿米卡星 微生物学 分枝杆菌 莫西沙星 最小抑制浓度 非结核分枝杆菌 生物 抗生素 细菌 遗传学
作者
Gabrielle Fröberg,Florian P. Maurer,Erja Chryssanthou,Louise Fernström,Hanaa Benmansour,Samira Boarbi,Anne Torunn Mengshoel,Peter M. Keller,Miguel Viveiros,Diana Machado,Margaret Fitzgibbon,Simone Mok,Jim Werngren,Daniela María Cirillo,Fernando Alcaide,Hanne‐Leena Hyyryläinen,Alexandra Aubry,Sönke Andres,Darshaalini Nadarajan,Erik Svensson
出处
期刊:Clinical Microbiology and Infection [Elsevier BV]
卷期号:29 (6): 758-764 被引量:36
标识
DOI:10.1016/j.cmi.2023.02.007
摘要

For non-tuberculous mycobacteria (NTM), minimum inhibitory concentration (MIC) distributions of wild-type isolates have not been systematically evaluated despite their importance for establishing antimicrobial susceptibility testing (AST) breakpoints. We gathered MIC distributions for drugs used against the Mycobacterium avium complex (MAC) and Mycobacterium abscessus (MAB) obtained by commercial broth microdilution (SLOMYCOI and RAPMYCOI) from 12 laboratories. Epidemiological cut-off values (ECOFFs) and tentative ECOFFs (TECOFFs) were determined by EUCAST methodology including quality control (QC) strains. The clarithromycin ECOFF was 16 mg/L for M. avium (n = 1271) whereas TECOFFs were 8 mg/L for M. intracellulare (n = 415) and 1 mg/L for MAB (n = 1014) confirmed by analysing MAB subspecies without inducible macrolide resistance (n = 235). For amikacin, the ECOFFs were 64 mg/L for MAC and MAB. For moxifloxacin, the WT spanned >8 mg/L for both MAC and MAB. For linezolid, the ECOFF and TECOFF were 64 mg/L for M. avium and M. intracellulare, respectively. Current CLSI breakpoints for amikacin (16 mg/L), moxifloxacin (1 mg/L) and linezolid (8 mg/L) divided the corresponding WT distributions. For QC M. avium and M. peregrinum, ≥95% of MIC values were well within recommended QC ranges. As a first step towards clinical breakpoints for NTM, (T)ECOFFs were defined for several antimicrobials against MAC and MAB. Broad wild-type MIC distributions indicate a need for further method refinement which is now under development within the EUCAST subcommittee for anti-mycobacterial drug susceptibility testing. In addition, we showed that several CLSI NTM breakpoints are not consistent in relation to the (T)ECOFFs.
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