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结核病的生物标志物和诊断:进展、需求及转化为实践。

Biomarkers and diagnostics for tuberculosis: progress, needs, and translation into practice.

机构信息

Pfizer, New London, CT, USA.

出版信息

Lancet. 2010 May 29;375(9729):1920-37. doi: 10.1016/S0140-6736(10)60359-5. Epub 2010 May 18.

Abstract

Human infection with Mycobacterium tuberculosis can progress to active disease, be contained as latent infection, or be eradicated by the host response. Tuberculosis diagnostics classify a patient into one of these categories. These are not fixed distinct states, but rather are continua along which patients can move, and are affected by HIV infection, immunosuppressive therapies, antituberculosis treatments, and other poorly understood factors. Tuberculosis biomarkers-host or pathogen-specific-provide prognostic information, either for individual patients or study cohorts, about these outcomes. Tuberculosis case detection remains difficult, partly because of inaccurate diagnostic methods. Investments have yielded some progress in development of new diagnostics, although the existing pipeline is limited for tests for sputum-smear-negative cases, childhood tuberculosis, and accurate prediction of reactivation of latent tuberculosis. Despite new, sensitive, automated molecular platforms for detection of tuberculosis and drug resistance, a simple, inexpensive point-of-care test is still not available. The effect of any new tests will depend on the method and extent of their introduction, the strength of the laboratories, and the degree to which access to appropriate therapy follows access to diagnosis. Translation of scientific progress in biomarkers and diagnostics into clinical and public health programmes is possible-with political commitment, increased funding, and engagement of all stakeholders.

摘要

人类感染结核分枝杆菌后可能会发展为活动性疾病,也可能被宿主的免疫反应控制为潜伏感染,或者被清除。结核病诊断将患者分为这几类。这些类别并不是固定不变的,而是连续的,患者可以在其中移动,受 HIV 感染、免疫抑制治疗、抗结核治疗以及其他尚未完全理解的因素影响。结核生物标志物——宿主或病原体特异性——为个体患者或研究队列提供预后信息,包括这些结局。由于诊断方法不准确,结核病的病例发现仍然很困难。尽管新的、敏感的、自动化的分子平台用于检测结核病和耐药性,但仍然没有简单、廉价的即时检测点。任何新检测的效果都将取决于其引入的方法和程度、实验室的实力以及适当治疗与诊断之间的关联程度。将生物标志物和诊断方面的科学进展转化为临床和公共卫生方案是可行的,需要有政治承诺、增加资金投入并让所有利益相关方参与其中。

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