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一种基于症状的精细化方法用于诊断儿童肺结核。

A refined symptom-based approach to diagnose pulmonary tuberculosis in children.

作者信息

Marais Ben J, Gie Robert P, Hesseling Anneke C, Schaaf H Simon, Lombard Carl, Enarson Donald A, Beyers Nulda

机构信息

Desmond Tutu Tuberculosis Centre and Department of Paediatrics and Child Health, Tygerberg Children's Hospital, Stellenbosch University, Cape Town, South Africa.

出版信息

Pediatrics. 2006 Nov;118(5):e1350-9. doi: 10.1542/peds.2006-0519.

Abstract

BACKGROUND

Tuberculosis control programs place an almost exclusive emphasis on adults with sputum smear-positive tuberculosis, because they are most infectious. However, children contribute a significant proportion of the global tuberculosis caseload and experience considerable tuberculosis-related morbidity and mortality, but few children in endemic areas have access to antituberculosis treatment. The diagnostic difficulty experienced in endemic areas with limited resources has been identified as a major factor contributing to poor treatment access. In general, there is a sense of scepticism regarding the potential value of symptom-based diagnostic approaches, because current clinical diagnostic approaches are often poorly validated. The natural history of childhood tuberculosis demonstrates that symptoms may offer good diagnostic value if they are well defined and if appropriate risk stratification is applied. This study aimed to determine the value of well-defined symptoms to diagnose childhood pulmonary tuberculosis in a tuberculosis-endemic area.

METHODS

A prospective, community-based study was conducted in Cape Town, South Africa. Specific well-defined symptoms were documented in all children < 13 years of age reporting a persistent, nonremitting cough of > 2 weeks' duration; study participants were thoroughly evaluated for tuberculosis. In addition, all of the children who received antituberculosis treatment during the study period were reviewed by the investigator, irrespective of study inclusion. This concurrent disease surveillance provided a comprehensive overview of all of the childhood tuberculosis cases, allowing accurate assessment of the possible disadvantages associated with this symptom-based diagnostic approach. In the absence of an acceptable gold standard test, optimal case definition is an important consideration. Children were categorized as "bacteriologically confirmed tuberculosis," "radiologically certain tuberculosis," "probable tuberculosis," or "not tuberculosis." Bacteriologically confirmed tuberculosis was defined as the presence of acid-fast bacilli on sputum microscopy and/or Mycobacterium tuberculosis cultured from a respiratory specimen. Radiologically certain tuberculosis was defined as agreement between both independent experts that the chest radiograph indicated certain tuberculosis in the absence of bacteriologic confirmation. Probable tuberculosis was defined as the presence of suggestive radiologic signs and good clinical response to antituberculosis treatment in the absence of bacteriologic confirmation or radiologic certainty. Good clinical response was defined as complete symptom resolution and weight gain of > or = 10% of body weight at diagnosis, within 3 months of starting antituberculosis treatment. Not tuberculosis was defined as spontaneous symptom resolution or no response to antituberculosis therapy in the absence of bacteriologic confirmation or radiologic signs suggestive of tuberculosis. Pulmonary tuberculosis was defined as a symptomatic child with: (1) bacteriologically confirmed tuberculosis, (2) radiologically confirmed tuberculosis, or (3) probable tuberculosis (as defined), excluding isolated pleural effusion.

RESULTS

In total, 1024 children were referred for evaluation. Resolving symptoms were reported in 596 children (58.2%); 428 (41.8%) children with persistent, nonremitting symptoms at evaluation were investigated for tuberculosis. Pulmonary tuberculosis was diagnosed in 197 children; 96 were categorized as bacteriologically confirmed tuberculosis, 75 as radiologically certain tuberculosis, and 26 as probable tuberculosis. Combining a persistent nonremitting cough of > 2 weeks' duration, documented failure to thrive (in the preceding 3 months), and fatigue provided reasonable diagnostic accuracy in HIV-uninfected children (sensitivity: 62.6%; specificity: 89.8%; positive predictive value: 83.6%); the performance was better in the low-risk group (> or = 3 years; sensitivity: 82.3%; specificity: 90.2%; positive predictive value: 82.3%) than in the high-risk group (< 3 years; sensitivity: 51.8%; specificity: 92.5%; positive predictive value: 90.1%). In children with an uncertain diagnosis at presentation, clinical follow-up was a valuable diagnostic tool that further improved diagnostic accuracy, particularly in the low-risk group. Symptom-based approaches offered little diagnostic value in HIV-infected children. Three (15%) of the 20 HIV-infected children diagnosed with pulmonary tuberculosis failed to report symptoms of sufficient duration to warrant study inclusion, whereas 25% reported persistent, nonremitting symptoms in the absence of tuberculosis. In addition, the tuberculin skin test was positive in < 20% of HIV-infected children diagnosed with pulmonary tuberculosis.

DISCUSSION

The combined presence of 3 well-defined symptoms at presentation (persistent, nonremitting cough of > 2 weeks' duration; objective weight loss [documented failure to thrive] during the preceding 3 months; and reported fatigue) provided good diagnostic accuracy in HIV-uninfected children > or = 3 years of age, with clinical follow-up providing additional value. The approach performed less well in children < 3 years. However, the presence of a persistent, nonremitting cough together with documented failure to thrive still provided a fairly accurate diagnosis (sensitivity: 68.3%; specificity: 80.1%; positive predictive value: 82.1%), illustrating the importance of regular weight monitoring in young children. Clinical follow-up also offered additional diagnostic value, but caution is required, because very young children have an increased risk of rapid disease progression. The approach performed poorly in HIV-infected children. Recent household contact with an adult index case seemed to provide more diagnostic value than a positive tuberculin skin test, but novel T-cell-based assays may offer the only real improvement in sensitivity to diagnose M. tuberculosis infection in HIV-infected children. The variable diagnostic value offered by this symptom-based diagnostic approach illustrates the importance of risk stratification, as demonstrated by the fact that 11 (91.7%) of 12 children with severe disease manifestations who failed to meet the entry criteria were < 3 years of age or HIV infected. Particular emphasis should be placed on the provision of preventive chemotherapy after documented exposure and/or infection in these high-risk children. Study limitations include the small number of HIV-infected children, but on the positive side, the large number of HIV-uninfected children permitted adequate evaluation in this important group. It is often forgotten that HIV-uninfected children constitute the majority of child tuberculosis cases, even in settings where HIV is endemic. This study demonstrates the importance of ascertaining a child's HIV status before symptom-based diagnosis is attempted. Because children were recruited at both the clinic and hospital level, some selection bias may have been introduced; however, the only significant difference between the 2 groups was the proportion of HIV-infected children. Pulmonary tuberculosis was diagnosed with different levels of certainty, but no significant differences were recorded between these groups.

CONCLUSIONS

Pulmonary tuberculosis can be diagnosed with a reasonable degree of accuracy in HIV-uninfected children using a simple symptom-based approach. This offers the exciting prospect of improving treatment access for children, particularly in resource-limited settings where current access to antituberculosis treatment is poor.

摘要

背景

结核病控制项目几乎只专注于痰涂片阳性的成年结核病患者,因为他们传染性最强。然而,儿童在全球结核病病例中占相当大比例,且结核病相关的发病率和死亡率颇高,但在结核病流行地区,很少有儿童能获得抗结核治疗。在资源有限的流行地区,诊断困难被认为是导致治疗可及性差的主要因素。总体而言,人们对基于症状的诊断方法的潜在价值持怀疑态度,因为当前的临床诊断方法往往缺乏充分验证。儿童结核病的自然病程表明,如果症状定义明确且进行适当的风险分层,症状可能具有良好的诊断价值。本研究旨在确定在结核病流行地区,明确的症状对诊断儿童肺结核的价值。

方法

在南非开普敦进行了一项基于社区的前瞻性研究。记录了所有年龄小于13岁、报告持续咳嗽超过2周且不缓解的儿童的特定明确症状;对研究参与者进行了全面的结核病评估。此外,研究期间所有接受抗结核治疗的儿童,无论是否纳入研究,均由研究者进行复查。这种同步的疾病监测全面概述了所有儿童结核病病例,从而能够准确评估这种基于症状的诊断方法可能存在的弊端。由于缺乏可接受的金标准检测,最佳病例定义是一个重要的考虑因素。儿童被分为“细菌学确诊的结核病”“影像学确诊的结核病”“疑似结核病”或“非结核病”。细菌学确诊的结核病定义为痰涂片显微镜检查发现抗酸杆菌和/或从呼吸道标本中培养出结核分枝杆菌。影像学确诊的结核病定义为两位独立专家均认为胸部X线片显示为确诊结核病但无细菌学证实。疑似结核病定义为在无细菌学证实或影像学确诊的情况下,存在提示性的影像学征象且对抗结核治疗有良好的临床反应。良好的临床反应定义为在开始抗结核治疗3个月内,症状完全缓解且体重增加达到或超过诊断时体重的10%。非结核病定义为在无细菌学证实或提示结核病的影像学征象的情况下,症状自行缓解或对抗结核治疗无反应。肺结核定义为有症状的儿童,具备以下情况之一:(1)细菌学确诊的结核病,(2)影像学确诊的结核病,或(3)疑似结核病(如上述定义),不包括单纯性胸腔积液。

结果

共有1024名儿童被转诊进行评估。596名儿童(58.2%)报告症状缓解;428名(41.8%)在评估时仍有持续不缓解症状的儿童接受了结核病调查。197名儿童被诊断为肺结核;96名被分类为细菌学确诊的结核病,75名被分类为影像学确诊的结核病,26名被分类为疑似结核病。对于未感染HIV的儿童,持续咳嗽超过2周、记录在案的发育不良(在前3个月内)和疲劳这三个症状组合具有合理的诊断准确性(敏感性:62.6%;特异性:89.8%;阳性预测值:83.6%);在低风险组(年龄≥3岁)中表现更好(敏感性:82.3%;特异性:90.2%;阳性预测值:82.3%),而在高风险组(年龄<3岁)中表现较差(敏感性:51.8%;特异性:92.5%;阳性预测值:90.1%)。对于初诊时诊断不确定的儿童,临床随访是一种有价值的诊断工具,可进一步提高诊断准确性,尤其是在低风险组。基于症状的方法在感染HIV的儿童中诊断价值不大。20名被诊断为肺结核的感染HIV儿童中,有3名(15%)未报告足够长时间的症状以符合研究纳入标准,而25%的儿童在无结核病的情况下报告了持续不缓解的症状。此外,在被诊断为肺结核的感染HIV儿童中,结核菌素皮肤试验阳性率低于20%。

讨论

初诊时出现三种明确症状(持续咳嗽超过2周、在前3个月内有客观体重减轻[记录为发育不良]以及报告有疲劳)的组合,对于年龄≥3岁的未感染HIV儿童具有良好的诊断准确性,临床随访具有额外价值。该方法在年龄<3岁的儿童中表现较差。然而,持续咳嗽加上记录在案的发育不良仍能提供相当准确的诊断(敏感性:68.3%;特异性:80.1%;阳性预测值:82.1%),这说明了定期监测幼儿体重的重要性。临床随访也具有额外的诊断价值,但需要谨慎,因为幼儿疾病进展迅速的风险增加。该方法在感染HIV的儿童中表现不佳。近期与成人索引病例的家庭接触似乎比结核菌素皮肤试验阳性提供了更多的诊断价值,但新型基于T细胞的检测方法可能是提高感染HIV儿童中结核分枝杆菌感染诊断敏感性的唯一真正改进方法。这种基于症状的诊断方法提供的可变诊断价值说明了风险分层的重要性,事实证明,12名有严重疾病表现但未符合纳入标准的儿童中,有11名(91.7%)年龄<3岁或感染了HIV。对于这些高风险儿童,在记录有接触和/或感染后,应特别强调提供预防性化疗。研究局限性包括感染HIV儿童数量较少,但从积极方面来看,大量未感染HIV儿童使得能够对这一重要群体进行充分评估。人们常常忘记,即使在HIV流行地区未感染HIV的儿童也占儿童结核病病例的大多数。本研究表明,在尝试基于症状的诊断之前确定儿童的HIV状态非常重要。由于儿童是在诊所和医院层面招募的,可能引入了一些选择偏倚;然而,两组之间唯一的显著差异是感染HIV儿童的比例。肺结核的诊断有不同程度的确定性,但这些组之间未记录到显著差异。

结论

使用简单的基于症状的方法可以在未感染HIV的儿童中以合理的准确度诊断肺结核。这为改善儿童治疗可及性带来了令人兴奋的前景,特别是在当前抗结核治疗可及性差的资源有限环境中。

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