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结核病和结节病的共同特征。

Common features of tuberculosis and sarcoidosis.

作者信息

Mortaz Esmaeil, Masjedi Mohammad Reza, Abedini Atefeh, Matroodi Soheila, Kiani Arda, Soroush Dina, Adcock Ian M

机构信息

Division of Pharmacology, Utrecht Institute for Pharmaceutical Sciences, Faculty of Science, Utrecht University, Utrecht, The Netherlands; Chronic Respiratory Disease Research Center, National Research Institute of Tuberculosis and Lung Disease, Masih Daneshvari Hospital, Shahid Beheshti University of Medical Sciences, Tehran, Iran.

Chronic Respiratory Disease Research Center, National Research Institute of Tuberculosis and Lung Disease, Masih Daneshvari Hospital, Shahid Beheshti University of Medical Sciences, Tehran, Iran.

出版信息

Int J Mycobacteriol. 2016 Dec;5 Suppl 1:S240-S241. doi: 10.1016/j.ijmyco.2016.09.031. Epub 2016 Nov 9.

DOI:10.1016/j.ijmyco.2016.09.031
PMID:28043581
Abstract

Tuberculosis (TB) is a disease caused by Mycobacterium tuberculosis. Despite the availability of novel therapeutic approaches, TB is considered as one of the leading causes of death due to infectious diseases worldwide. Alveolar macrophages are the first line of defense against M. tuberculosis; they ingest and sequester the bacilli within granulomatous structures. Control and resolution of the infection requires activated T lymphocytes as well as Th1 cytokines. There are two forms of TB: active TB and latent TB. Latent TB is a state in which M. tuberculosis survives in the body without causing overt signs and symptoms. People with latent TB are noncontagious. However, M. tuberculosis can become active in the body, multiply, and cause overt TB. Sarcoidosis, on the other hand, is an autoimmune disease of unknown etiology which can affect multiple systems of the body. Nonspecific constitutional symptoms, such as fever, fatigue, malaise, and weight loss, are present in approximately one-third of patients. Chest X-ray usually shows hilar and mediastinal lymphadenopathy. Although the lungs are the most common sites of inflammation, sarcoidosis can also involve other organs, such as the eyes (intraocular and adnexal), skin, lymph nodes, salivary glands, heart, spleen, liver, and the nervous system. Recent investigations have provided further insights into the genetic basis of sarcoidosis and the way genotype determines the clinical presentation and phenotype of patients. Histopathologic features are usually insufficient for diagnosis of sarcoidosis. Diagnosis of sarcoidosis in endemic areas for TB can become a great challenge. Both TB and sarcoidosis are granulomatous diseases; TB is characterized by caseating granulomas, whereas sarcoidosis is characterized by noncaseating granulomas. New cases of sarcoidosis are increasingly being diagnosed in areas endemic for TB due to increased orientation of physicians and availability of diagnostic modalities. However, it is often difficult to differentiate sarcoidosis from TB, especially when caseous necrosis is not seen and acid-fast staining is negative in the biopsy specimen of patient with TB. Granulomatous inflammation in sarcoidosis is believed to be caused by the presence of a persistent poorly degradable unknown antigen in combination with a nonresolving host response. M. tuberculosis has been extensively studied as a possible cause of sarcoidosis. Results suggest that granulomas form in the lungs as a result of the immune response to inhaled M. tuberculosis and serve as the central site of host-pathogen interaction during M. tuberculosis infection. M. tuberculosis DNA detection in sarcoidosis samples by traditional polymerase chain reaction (PCR) has been used for the pathological study of sarcoidosis; however, it is likely that real time quantitative PCR analysis of specific mRNAs and microRNAs will be necessary as a sensitive, precise, and rapid diagnostic test for detecting trace of TB in Sarcoidosis. In conclusion, diagnosis of sarcoidosis in areas with a high burden of TB poses a significant challenge. Improved diagnostic tests including genetic tests can improve our knowledge and help in distinguishing these two diseases.

摘要

结核病(TB)是一种由结核分枝杆菌引起的疾病。尽管有了新的治疗方法,但结核病仍被认为是全球因传染病导致死亡的主要原因之一。肺泡巨噬细胞是抵御结核分枝杆菌的第一道防线;它们摄取并将杆菌隔离在肉芽肿结构内。感染的控制和消退需要活化的T淋巴细胞以及Th1细胞因子。结核病有两种形式:活动性结核病和潜伏性结核病。潜伏性结核病是结核分枝杆菌在体内存活但不引起明显体征和症状的一种状态。潜伏性结核病患者没有传染性。然而,结核分枝杆菌可在体内活化、繁殖并导致明显的结核病。另一方面,结节病是一种病因不明的自身免疫性疾病,可影响身体的多个系统。约三分之一的患者会出现非特异性全身症状,如发热、疲劳、不适和体重减轻。胸部X线检查通常显示肺门和纵隔淋巴结肿大。虽然肺部是最常见的炎症部位,但结节病也可累及其他器官,如眼睛(眼内和附属器)、皮肤、淋巴结、唾液腺、心脏、脾脏、肝脏和神经系统。最近的研究进一步深入了解了结节病的遗传基础以及基因型决定患者临床表现和表型的方式。组织病理学特征通常不足以诊断结节病。在结核病流行地区诊断结节病可能是一项巨大挑战。结核病和结节病都是肉芽肿性疾病;结核病的特征是干酪样肉芽肿,而结节病的特征是非干酪样肉芽肿。由于医生的关注度提高和诊断方法的可用性,在结核病流行地区越来越多地诊断出结节病新病例。然而,通常很难将结节病与结核病区分开来,尤其是当在结核病患者的活检标本中未见干酪样坏死且抗酸染色为阴性时。结节病中的肉芽肿性炎症被认为是由持续存在的难以降解的未知抗原与无法消退的宿主反应共同引起的。结核分枝杆菌作为结节病的可能病因已得到广泛研究。结果表明,肺部肉芽肿是对吸入的结核分枝杆菌免疫反应的结果,并且在结核分枝杆菌感染期间作为宿主 - 病原体相互作用的中心部位。通过传统聚合酶链反应(PCR)检测结节病样本中的结核分枝杆菌DNA已用于结节病的病理研究;然而,作为一种检测结节病中微量结核病的灵敏、精确和快速的诊断试验,可能需要对特定mRNA和微小RNA进行实时定量PCR分析。总之,在结核病负担高的地区诊断结节病构成了重大挑战。包括基因检测在内的改进诊断试验可以增进我们的认识并有助于区分这两种疾病。

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