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全基因组测序分析导致治疗失败和宿主内进化的串联耐多药结核菌株。

Analysis of Serial Multidrug-Resistant Tuberculosis Strains Causing Treatment Failure and Within-Host Evolution by Whole-Genome Sequencing.

机构信息

Department of Infectious Diseases, Huashan Hospital, Fudan University, Shanghai, China.

Department of Infectious Diseases, Wenzhou Central Hospital, Affiliated Dingli Clinical Institute of Wenzhou Medical University, Wenzhou, China.

出版信息

mSphere. 2020 Dec 23;5(6):e00884-20. doi: 10.1128/mSphere.00884-20.

Abstract

The cure rate of multidrug-resistant tuberculosis (MDR-TB) is relatively low in China. The reasons for the treatment failure and within-host evolution during treatment have not been sufficiently studied. All MDR-TB patients receiving standard treatment from January 2014 to September 2016 at a designated TB Hospital in Zhejiang Province were retrospectively included and grouped according to their known treatment outcome. Clinical information was collected. Baseline strains of all patients and serial strains of treatment-failure patients were revived. Drug susceptibility tests (DSTs) of 14 drugs and single nucleotide polymorphism (SNP) analysis based on whole-genome sequencing (WGS) were performed. The genetic distance and within-host evolution were investigated based on SNPs. In total, 20 treatment failure patients and 74 patients who succeeded in treatment were included. The number of effective drugs for patients who failed treatment was no more than three. Eighteen (90.0%) treatment-failure patients were characterized by a continuous infection of the primary strain, of which 14 patients (77.8%) developed phenotypic or genotypic acquired drug resistance under ineffective treatment. Acquired resistance to amikacin and moxifloxacin (2.0 mg/ml) was detected most frequently, in 5 and 4 patients, respectively. The insufficient number of effective drugs in the combined treatment regimen was the main reason for MDR-TB treatment failure. The study emphasizes the importance of DST for second-line drugs when implementing the second-line drug regimen in MDR-TB patients. For patients with risk factors for MDR-TB, DST of second-line antituberculosis drugs should be performed at initiation of treatment. Second-line drugs should be selected based on the results of DST to avoid acquired resistance. WGS detects low-frequency resistance mutations and heterogeneous resistance with high sensitivity, which is of great significance for guiding clinical treatment and preventing acquired resistance. Few studies have focused on the reasons for the low cure rate of multidrug-resistant tuberculosis in China and within-host evolution during treatment, which is of great significance for improving clinical treatment regimens. Acquired resistance events were common during the ineffective treatment, among which resistance to amikacin and high-level moxifloxacin were the most common. The main reason for the treatment failure of MDR-TB patients was insufficient effective drugs, which may lead to higher levels of drug resistance in MDR-TB strains. Therefore, the study emphasizes the importance of DST in the development of second-line treatment regimen when there is a risk of MDR. By performing whole-genome sequencing of serial strains from patients with treatment failure, we found that WGS can detect low-frequency resistance mutations and heterogeneous resistance with high sensitivity. It is thus recommended to conduct drug susceptibility tests at the beginning of treatment and repeat the DST when the sputum bacteria remain positive.

摘要

中国耐多药结核病(MDR-TB)的治愈率相对较低。治疗失败和治疗期间宿主内进化的原因尚未得到充分研究。

2014 年 1 月至 2016 年 9 月,浙江省某指定结核病医院对所有接受标准治疗的 MDR-TB 患者进行回顾性研究,并根据已知的治疗结果进行分组。收集临床信息。所有患者的基线菌株和治疗失败患者的连续菌株均被复苏。进行了 14 种药物的药敏试验(DST)和基于全基因组测序(WGS)的单核苷酸多态性(SNP)分析。基于 SNP 研究了遗传距离和宿主内进化。共纳入 20 例治疗失败患者和 74 例治疗成功患者。治疗失败患者有效的药物数量不超过三种。18 例(90.0%)治疗失败患者表现为原发性菌株的持续感染,其中 14 例(77.8%)患者在无效治疗下表现出表型或基因型获得性药物耐药性。最常检测到对阿米卡星和莫西沙星(2.0mg/ml)的获得性耐药,分别在 5 例和 4 例患者中检测到。联合治疗方案中有效药物数量不足是 MDR-TB 治疗失败的主要原因。研究强调在 MDR-TB 患者实施二线药物方案时,DST 对二线抗结核药物的重要性。对于 MDR-TB 发生风险的患者,在开始治疗时应进行二线抗结核药物的 DST。应根据 DST 结果选择二线药物,以避免获得性耐药。WGS 以高灵敏度检测低频耐药突变和异质性耐药,对指导临床治疗和预防获得性耐药具有重要意义。很少有研究关注中国耐多药结核病低治愈率和治疗期间宿主内进化的原因,这对于改善临床治疗方案具有重要意义。在无效治疗期间经常发生获得性耐药事件,其中对阿米卡星和高水平莫西沙星的耐药性最为常见。MDR-TB 患者治疗失败的主要原因是有效药物不足,这可能导致 MDR-TB 菌株的耐药水平更高。因此,该研究强调了在存在 MDR 风险时,DST 在二线治疗方案开发中的重要性。通过对治疗失败患者的连续菌株进行全基因组测序,我们发现 WGS 可以以高灵敏度检测低频耐药突变和异质性耐药。因此,建议在治疗开始时进行药敏试验,并在痰菌仍阳性时重复 DST。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7c18/7763549/5ff2bf1cd8ff/mSphere.00884-20-f0001.jpg

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