Sequential and parallel testing for microbiological confirmation of tuberculosis disease in children in five low-income and middle-income countries: a secondary analysis of the RaPaed-TB study.

IF 36.4 1区 医学 Q1 INFECTIOUS DISEASES
Lancet Infectious Diseases Pub Date : 2025-02-01 Epub Date: 2024-09-20 DOI:10.1016/S1473-3099(24)00494-8
Laura Olbrich, Zoe Franckling-Smith, Leyla Larsson, Issa Sabi, Nyanda Elias Ntinginya, Celso Khosa, Denise Banze, Marriott Nliwasa, Elizabeth Lucy Corbett, Robina Semphere, Valsan Philip Verghese, Joy Sarojini Michael, Marilyn Mary Ninan, Elmar Saathoff, Timothy Daniel McHugh, Alia Razid, Stephen Michael Graham, Rinn Song, Pamela Nabeta, Andre Trollip, Mark Patrick Nicol, Michael Hoelscher, Christof Geldmacher, Norbert Heinrich, Heather Joy Zar
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引用次数: 0

Abstract

Background: Despite causing high mortality worldwide, paediatric tuberculosis is often undiagnosed. We aimed to investigate optimal testing strategies for microbiological confirmation of tuberculosis in children younger than 15 years, including the yield in high-risk subgroups (eg, children younger than 5 years, with HIV, or with severe acute malnutrition [SAM]).

Methods: For this secondary analysis, we used data from RaPaed-TB, a multicentre diagnostic accuracy study evaluating novel diagnostic assays and testing approaches for tuberculosis in children recruited from five health-care centres in Malawi, Mozambique, South Africa, Tanzania, and India conducted between Jan 21, 2019, and June 30, 2021. Children were included if they were younger than 15 years and had signs or symptoms of pulmonary or extrapulmonary tuberculosis; they were excluded if they weighed less than 2 kg, had received three or more doses of anti-tuberculosis medication at time of enrolment, were in a condition deemed critical by the local investigator, or if they did not have at least one valid microbiological result. We collected tuberculosis-reference specimens via spontaneous sputum, induced sputum, gastric aspirate, and nasopharyngeal aspirates. Microbiological tests were Xpert MTB/RIF Ultra (hereafter referred to as Ultra), liquid culture, and Löwenstein-Jensen solid culture, which were followed by confirmatory testing for positive cultures. The main outcome of this secondary analysis was categorising children as having confirmed tuberculosis if culture or Ultra positive on any sample, unconfirmed tuberculosis if clinically diagnosed, and unlikely tuberculosis if neither of these applied.

Findings: Of 5313 children screened, 975 were enrolled, of whom 965 (99%) had at least one valid microbiological result. 444 (46%) of 965 had unlikely tuberculosis, 282 (29%) had unconfirmed tuberculosis, and 239 (25%) had confirmed tuberculosis. Median age was 5·0 years (IQR 1·8-9·0); 467 (48%) of 965 children were female and 498 (52%) were male. 155 (16%) of 965 children had HIV and 110 (11%) children had SAM. 196 (82%) of 239 children with microbiological detection tested positive on Ultra. 110 (46%) of 239 were confirmed by both Ultra and culture, 86 (36%) by Ultra alone, and 43 (18%) by culture alone. 'Trace' was the most common semiquantitative result (93 [40%] of 234). 481 (50%) of 965 children had only one specimen type collected, 99 (21%) of whom had M tuberculosis detected. 484 (50%) of 965 children had multiple specimens collected, 141 (29%) of whom were positive on at least one specimen type. Of the 102 children younger than 5 years with M tuberculosis detected, 80 (78%) tested positive on sputum. 64 (80%) of 80 children who tested positive on sputum were positive on sputum alone; 61 (95%) of 64 were positive on induced sputum, two (3%) of 64 were positive on spontaneous sputum, and one (2%) was positive on both.

Interpretation: High rates of microbiological confirmation of tuberculosis in children can be achieved via parallel sampling and concurrent testing procedures. Sample types and choice of test to be used sequentially should be considered when applying to groups such as children younger than 5 years, living with HIV, or with SAM.

Funding: European and Developing Countries Clinical Trials Partnership programme, supported by the EU, the UK Medical Research Council, Swedish International Development Cooperation Agency, Bundesministerium für Bildung und Forschung, the German Center for Infection Research, and Beckman Coulter.

五个中低收入国家儿童结核病微生物学确证的顺序和平行检验:对 RaPaed-TB 研究的二次分析。
背景:尽管小儿结核病在全球范围内造成了很高的死亡率,但却常常得不到诊断。我们旨在调查 15 岁以下儿童结核病微生物学确诊的最佳检测策略,包括高风险亚组(如 5 岁以下儿童、艾滋病毒感染者或严重急性营养不良[SAM]儿童)的检测率:在这项二次分析中,我们使用了 RaPaed-TB 的数据。RaPaed-TB 是一项多中心诊断准确性研究,旨在评估从马拉维、莫桑比克、南非、坦桑尼亚和印度的五个医疗保健中心招募的儿童结核病新型诊断方法和检测方法,研究时间为 2019 年 1 月 21 日至 2021 年 6 月 30 日。年龄小于 15 岁、有肺部或肺外结核病症状或体征的儿童均被纳入其中;体重小于 2 千克、入组时接受过 3 次或 3 次以上抗结核药物治疗、当地调查人员认为病情危重或没有至少一次有效微生物学结果的儿童则被排除在外。我们通过自发痰、诱导痰、胃吸液和鼻咽吸液收集结核病参考标本。微生物检测包括 Xpert MTB/RIF Ultra(以下简称 Ultra)、液体培养和 Löwenstein-Jensen 固体培养,阳性培养物还需进行确证检测。这项二次分析的主要结果是,如果任何样本的培养或 Ultra 均呈阳性,则将儿童归类为确诊肺结核;如果经临床诊断,则归类为未确诊肺结核;如果两者均不适用,则归类为不可能的肺结核:在接受筛查的 5313 名儿童中,有 975 人被纳入筛查范围,其中 965 人(99%)至少有一项有效的微生物学结果。965人中有444人(46%)可能患有肺结核,282人(29%)未确诊肺结核,239人(25%)确诊肺结核。中位年龄为 5-0 岁(IQR 1-8-9-0);965 名儿童中有 467 名(48%)为女性,498 名(52%)为男性。965 名儿童中有 155 名(16%)感染了 HIV,110 名(11%)感染了 SAM。在微生物检测呈阳性的 239 名儿童中,196 人(82%)在 Ultra 检测中呈阳性。239名儿童中有110名(46%)经Ultra和培养证实,86名(36%)仅经Ultra证实,43名(18%)仅经培养证实。痕量 "是最常见的半定量结果(234 人中有 93 人[40%])。在 965 名儿童中,有 481 名(50%)只采集了一种标本,其中 99 名(21%)检测出 M 型结核。965 名儿童中有 484 名(50%)采集了多种标本,其中 141 名(29%)至少有一种标本呈阳性。在 102 名检测出 M 型结核病的 5 岁以下儿童中,80 人(78%)的痰液检测呈阳性。在痰液检测呈阳性的 80 名儿童中,有 64 人(80%)仅在痰液检测中呈阳性;64 人中有 61 人(95%)在诱导痰液检测中呈阳性,64 人中有 2 人(3%)在自发痰液检测中呈阳性,1 人(2%)在两种检测中均呈阳性:解释:通过平行采样和同步检测程序,儿童结核病的微生物学确诊率很高。在适用于小于 5 岁的儿童、艾滋病病毒感染者或患有严重急性呼吸系统综合症的儿童等群体时,应考虑样本类型和选择依次使用的检测方法:欧洲与发展中国家临床试验合作计划,由欧盟、英国医学研究理事会、瑞典国际发展合作署、德国联邦教育与研究部、德国感染研究中心和贝克曼库尔特公司共同支持。
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来源期刊
Lancet Infectious Diseases
Lancet Infectious Diseases 医学-传染病学
CiteScore
60.90
自引率
0.70%
发文量
1064
审稿时长
6-12 weeks
期刊介绍: The Lancet Infectious Diseases was launched in August, 2001, and is a lively monthly journal of original research, review, opinion, and news covering international issues relevant to clinical infectious diseases specialists worldwide.The infectious diseases journal aims to be a world-leading publication, featuring original research that advocates change or sheds light on clinical practices related to infectious diseases. The journal prioritizes articles with the potential to impact clinical practice or influence perspectives. Content covers a wide range of topics, including anti-infective therapy and immunization, bacterial, viral, fungal, and parasitic infections, emerging infectious diseases, HIV/AIDS, malaria, tuberculosis, mycobacterial infections, infection control, infectious diseases epidemiology, neglected tropical diseases, and travel medicine. Informative reviews on any subject linked to infectious diseases and human health are also welcomed.
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