Discordance Between Phenotypic and WGS-Based Drug Susceptibility Testing Results for Some Anti-Tuberculosis Drugs: A Snapshot Study of Paired Mycobacterium tuberculosis Isolates with Small Genetic Distance

IF 2.9 3区 医学 Q2 INFECTIOUS DISEASES Infection and Drug Resistance Pub Date : 2024-08-01 DOI:10.2147/idr.s468997
Darja Sadovska, Anda Nodieva, Ilva Pole, Anda Vīksna, Jānis Ķimsis, Iveta Ozere, Inga Norvaiša, Ineta Bogdanova, Dace Bandere, Renāte Ranka
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Abstract

Background: Current tuberculosis treatment regimens primarily rely on phenotypic drug susceptibility testing and rapid molecular assays. Although whole-genome sequencing (WGS) offers a promising alternative, disagreements between phenotypic and molecular testing methods remain. In this retrospective study, we compared the phenotypic and WGS-predicted drug resistance profiles of paired Mycobacterium tuberculosis isolates with small genetic distances (≤ 10 single nucleotide variants) obtained from patients with longitudinal single-episode or recurrent tuberculosis. Additionally, we investigated the distribution of drug-resistance-conferring variants among the identified M. tuberculosis genotypes.
Methods: Paired M. tuberculosis isolates from 46 patients with pulmonary tuberculosis (2002– 2019) were analyzed. Spoligotyping was performed for all the isolates. WGS data were processed using TB-Profiler software to genotype the strains and detect variants in M. tuberculosis genes associated with drug resistance. The significance of these variants was evaluated using the M. tuberculosis variant catalog developed by the World Health Organization. Phenotypic drug susceptibility test results were obtained from patients’ medical records.
Results: Among the 46 isolate pairs, 25 (54.3%) harbored drug-resistance-associated variants, with 20 demonstrating identical WGS-predicted drug resistance profiles. Drug-resistant isolate pairs belonged to Lineages 2 and 4, with the most common sub-lineages being 2.2.1 (SIT1 and SIT190 spoligotypes), and 4.3.3 (SIT42). Agreement between phenotypic and WGS-based drug susceptibility testing was highest (> 90%) for rifampicin, isoniazid, ethambutol, fluoroquinolones, streptomycin, and amikacin when calculated for M. tuberculosis isolates or isolate pairs. In most discordant cases, isolate pairs harbored variants that could cause low- or moderate-level resistance or were previously associated with variable minimum inhibitory concentrations. Notably, such discrepancies mostly occurred in one isolate from the pair. In addition, differences in resistance-related variant distributions among M. tuberculosis genotypes were observed for most of the analyzed drugs.
Conclusion: The simultaneous performance of phenotypic and WGS-based drug susceptibility testing creates the most accurate drug resistance profile for M. tuberculosis isolates and eliminates important limitations of each method.

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某些抗结核药物的表型和基于 WGS 的药敏测试结果不一致:对遗传距离较小的配对结核分枝杆菌分离株的快照研究
背景:目前的结核病治疗方案主要依赖于表型药敏试验和快速分子检测。尽管全基因组测序(WGS)提供了一种有前途的替代方法,但表型和分子检测方法之间仍存在分歧。在这项回顾性研究中,我们比较了遗传距离较小(≤ 10 个单核苷酸变异)的成对结核分枝杆菌分离株的表型和 WGS 预测的耐药性特征,这些分离株来自纵向单发或复发结核病患者。此外,我们还调查了已确定的结核杆菌基因型中耐药变异的分布情况:分析了 46 名肺结核患者(2002-2019 年)的配对结核杆菌分离物。对所有分离株进行了 Spoligotyping 分析。使用 TB-Profiler 软件处理 WGS 数据,对菌株进行基因分型,并检测与耐药性相关的结核杆菌基因变异。利用世界卫生组织开发的结核杆菌变异体目录对这些变异体的重要性进行了评估。表型药敏试验结果来自患者的医疗记录:结果:在 46 对分离株中,25 株(54.3%)存在耐药性相关变异,其中 20 株显示出相同的 WGS 预测耐药性特征。耐药分离物对属于 2 号系和 4 号系,最常见的亚系是 2.2.1(SIT1 和 SIT190 spoligotype)和 4.3.3(SIT42)。在对结核杆菌分离株或分离株对进行计算时,对利福平、异烟肼、乙胺丁醇、氟喹诺酮类、链霉素和阿米卡星的表型药敏试验与基于 WGS 的药敏试验的一致性最高(90%)。在大多数不一致的病例中,分离物对含有可导致低度或中度耐药性的变异株,或以前与不同的最低抑菌浓度有关。值得注意的是,这种差异大多发生在一对分离物中的一个分离物上。此外,在大多数分析药物中都观察到了结核杆菌基因型间耐药性相关变体分布的差异:结论:同时进行基于表型和 WGS 的药物敏感性检测可为结核杆菌分离物建立最准确的耐药性谱,并消除每种方法的重要局限性。
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来源期刊
Infection and Drug Resistance
Infection and Drug Resistance Medicine-Pharmacology (medical)
CiteScore
5.60
自引率
7.70%
发文量
826
审稿时长
16 weeks
期刊介绍: About Journal Editors Peer Reviewers Articles Article Publishing Charges Aims and Scope Call For Papers ISSN: 1178-6973 Editor-in-Chief: Professor Suresh Antony An international, peer-reviewed, open access journal that focuses on the optimal treatment of infection (bacterial, fungal and viral) and the development and institution of preventative strategies to minimize the development and spread of resistance.
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