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结核性胸腔积液:进展与争议

Tuberculous pleural effusions: advances and controversies.

作者信息

Vorster Morné J, Allwood Brian W, Diacon Andreas H, Koegelenberg Coenraad F N

机构信息

Department of Medicine, Divisions of Pulmonology, Stellenbosch University & Tygerberg Academic Hospital, Cape Town 8000, South Africa.

出版信息

J Thorac Dis. 2015 Jun;7(6):981-91. doi: 10.3978/j.issn.2072-1439.2015.02.18.

Abstract

On a global scale, tuberculosis (TB) remains one of the most frequent causes of pleural effusions. Our understanding of the pathogenesis of the disease has evolved and what was once thought to be an effusion as a result of a pure delayed hypersensitivity reaction is now believed to be the consequence of direct infection of the pleural space with a cascade of events including an immunological response. Pulmonary involvement is more common than previously believed and induced sputum, which is grossly underutilised, can be diagnostic in approximately 50%. The gold standard for the diagnosis of tuberculous pleuritis remains the detection of Mycobacterium tuberculosis in pleural fluid, or pleural biopsy specimens, either by microscopy and/or culture, or the histological demonstration of caseating granulomas in the pleura along with acid fast bacilli (AFB). In high burden settings, however, the diagnosis is frequently inferred in patients who present with a lymphocytic predominant exudate and a high adenosine deaminase (ADA) level, which is a valuable adjunct in the diagnostic evaluation. ADA is generally readily accessible, and together with lymphocyte predominance justifies treatment initiation in patients with a high pre-test probability. Still, false-negative and false-positive results remain an issue. When adding closed pleural biopsy to ADA and lymphocyte count, diagnostic accuracy approaches that of thoracoscopy. The role of other biomarkers is less well described. Early pleural drainage may have a role in selected cases, but more research is required to validate its use and to define the subpopulation that may benefit from such interventions.

摘要

在全球范围内,结核病(TB)仍然是胸腔积液最常见的病因之一。我们对该疾病发病机制的认识已经有所发展,曾经被认为是单纯迟发型超敏反应导致的胸腔积液,现在认为是胸膜腔直接感染并引发一系列包括免疫反应在内的事件的结果。肺部受累比之前认为的更为常见,诱导痰这一未得到充分利用的检查手段,大约50%的情况下可用于诊断。结核性胸膜炎诊断的金标准仍然是通过显微镜检查和/或培养在胸腔积液或胸膜活检标本中检测到结核分枝杆菌,或者在胸膜中组织学显示干酪样肉芽肿以及抗酸杆菌(AFB)。然而,在高负担地区,对于出现以淋巴细胞为主的渗出液且腺苷脱氨酶(ADA)水平高的患者,通常推断其患有该病,ADA在诊断评估中是一项有价值的辅助检查。ADA一般易于获取,结合淋巴细胞占优势可在检测前概率高的患者中作为开始治疗的依据。不过,假阴性和假阳性结果仍然是个问题。当在ADA和淋巴细胞计数基础上增加闭式胸膜活检时,诊断准确性接近胸腔镜检查。其他生物标志物的作用描述较少。早期胸腔引流在某些特定病例中可能有作用,但需要更多研究来验证其应用并确定可能从这种干预措施中获益的亚组人群。

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