Division of Infection and Global Health, School of Medicine, University of St Andrews, St Andrews, UK; Infectious Diseases Research Collaboration, Kampala, Uganda.
Department of Biochemistry and Sports Sciences, Makerere University, Kampala, Uganda.
Lancet Microbe. 2024 Apr;5(4):e345-e354. doi: 10.1016/S2666-5247(23)00367-1. Epub 2024 Mar 5.
In 2018, the tuberculosis molecular bacterial load assay (TB-MBLA), a ribosomal RNA-based test, was acknowledged by WHO as a molecular assay that could replace smear microscopy and culture for monitoring tuberculosis treatment response. In this study, we evaluated the accuracy of TB-MBLA for diagnosis and monitoring of treatment response in comparison with standard-of-care tests.
For this longitudinal prospective study, patients aged 18 years or older with presumptive tuberculosis (coughing for at least 2 weeks, night sweats, and weight loss) were enrolled at China-Uganda Friendship Hospital Naguru (Kampala, Uganda). Participants were evaluated for tuberculosis by TB-MBLA in comparison with Xpert MTB/RIF Ultra (Xpert-Ultra) and smear microscopy, with Mycobacteria Growth Indicator Tube (MGIT) culture as a reference test. Participants who were positive on Xpert-Ultra were enrolled on a standard 6-month anti-tuberculosis regimen, and monitored for treatment response at weeks 2, 8, 17, and 26 after initiation of treatment and then 3 months after treatment.
Between Nov 15, 2019, and June 15, 2022, 210 participants (median age 35 years [IQR 27-44]) were enrolled. 135 (64%) participants were male and 72 (34%) were HIV positive. The pretreatment diagnostic sensitivities of TB-MBLA and Xpert-Ultra were similar (both 99% [95% CI 95-100]) but the specificity was higher for TB-MBLA (90% [83-96]) than for Xpert-Ultra (78% [68-86]). Ten participants were Xpert-Ultra trace positive, eight (80%) of whom were negative by TB-MBLA and MGIT culture. Smear microscopy had lower diagnostic sensitivity (75% [65-83]) but higher specificity (98% [93-100]) than TB-MBLA and Xpert-Ultra. Among participants who were smear microscopy negative, the sensitivity of TB-MBLA was 96% (95 CI 80-100) and was 100% (95% CI 86-100) in those who were HIV positive. 129 (61%) participants were identified as tuberculosis positive by Xpert-Ultra and these individuals were enrolled in the treatment group and monitored for treatment response. According to TB-MBLA, 19 of these patients cleared bacillary load to zero by week 2 of treatment and remained negative throughout the 6-month treatment follow-up. Positivity for tuberculosis decreased with treatment as measured by all tests, but the rate was slower with Xpert-Ultra. Consequently, 31 (33%) of 95 participants were still Xpert-Ultra positive at the end of treatment but were clinically well and negative on TB-MBLA and culture at 6 months of treatment. Two patients were still Xpert-Ultra positive with a further 3 months of post-treatment follow-up. The rate of conversion to negative of the DNA-based Xpert-Ultra was 3·3-times slower than that of the rRNA-based TB-MBLA. Consequently for the same patient, it would take 13 weeks and 52 weeks to reach complete tuberculosis negativity by TB-MBLA and Xpert-Ultra, respectively. Participants who were positive on smear microscopy at 8 weeks, who received an extra month of intensive treatment, had a similar TB-MBLA-measured bacillary load at 8 weeks to those who were smear microscopy negative.
TB-MBLA has a similar performance to Xpert-Ultra for pretreatment diagnosis of tuberculosis, but is more accurate at detecting and characterising the response to treatment than Xpert-Ultra and standard-of-care smear microscopy.
European and Developing Countries Clinical Trials Partnership, Makerere University Research and Innovation Fund, US National Institutes of Health.
2018 年,结核分枝杆菌分子细菌载量检测(TB-MBLA),一种基于核糖体 RNA 的检测方法,被世卫组织认可为可替代痰涂片显微镜检查和培养的分子检测方法,用于监测结核病治疗反应。在这项研究中,我们评估了 TB-MBLA 在诊断和监测治疗反应方面的准确性,与标准护理检测方法进行了比较。
这项纵向前瞻性研究纳入了 2019 年 11 月 15 日至 2022 年 6 月 15 日在中国-乌干达友谊医院纳古鲁(坎帕拉,乌干达)就诊的年龄在 18 岁及以上、疑似患有肺结核(咳嗽至少 2 周、盗汗和体重减轻)的患者。通过 TB-MBLA 与 Xpert MTB/RIF Ultra(Xpert-Ultra)和痰涂片显微镜检查进行比较,以分枝杆菌培养管(MGIT)培养为参考检测方法,评估参与者的肺结核情况。Xpert-Ultra 阳性的参与者被纳入标准的 6 个月抗结核治疗方案,并在治疗开始后第 2、8、17 和 26 周以及治疗结束后 3 个月进行治疗反应监测。
在 210 名参与者(中位年龄 35 岁[IQR 27-44])中,有 135 名(64%)为男性,72 名(34%)为 HIV 阳性。TB-MBLA 和 Xpert-Ultra 的预处理诊断敏感度相似(均为 99%[95%CI 95-100]),但 TB-MBLA 的特异性(90%[83-96%])高于 Xpert-Ultra(78%[68-86%])。10 名参与者的 Xpert-Ultra 检测结果为痕量阳性,其中 8 名(80%)为 TB-MBLA 和 MGIT 培养阴性。痰涂片显微镜检查的诊断敏感度较低(75%[65-83%]),但特异性较高(98%[93-100%]),高于 TB-MBLA 和 Xpert-Ultra。在痰涂片阴性的参与者中,TB-MBLA 的敏感度为 96%(95%CI 80-100%),HIV 阳性者的敏感度为 100%(95%CI 86-100%)。129 名(61%)参与者的 Xpert-Ultra 检测结果为阳性,这些患者被纳入治疗组,并进行治疗反应监测。根据 TB-MBLA,19 名患者在治疗第 2 周时清除了细菌载量至零,并且在整个 6 个月的治疗随访期间保持阴性。所有检测方法均显示,随着治疗的进行,结核病的阳性率下降,但 Xpert-Ultra 下降速度较慢。因此,95 名参与者中有 31 名(33%)在治疗结束时仍为 Xpert-Ultra 阳性,但临床状况良好,在治疗结束后 6 个月时 TB-MBLA 和培养均为阴性。两名患者在进一步的 3 个月治疗随访后仍为 Xpert-Ultra 阳性。Xpert-Ultra 检测 DNA 的转化率比 TB-MBLA 检测 rRNA 的转化率慢 3.3 倍。因此,对于同一患者,TB-MBLA 和 Xpert-Ultra 分别需要 13 周和 52 周才能达到完全的结核病阴性。在第 8 周时痰涂片阳性并接受额外一个月强化治疗的患者,其第 8 周时的 TB-MBLA 检测细菌载量与痰涂片阴性的患者相似。
TB-MBLA 在结核病的预处理诊断方面与 Xpert-Ultra 具有相似的性能,但在检测和评估治疗反应方面比 Xpert-Ultra 和标准护理痰涂片显微镜检查更准确。
欧洲和发展中国家临床试验伙伴关系、马凯雷雷大学研究和创新基金、美国国立卫生研究院。
