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A Systematic Review on Novel Mycobacterium tuberculosis Antigens and Their Discriminatory Potential for the Diagnosis of Latent and Active Tuberculosis

机译:新型结核分枝杆菌抗原及其对潜伏性和活动性肺结核的诊断潜力的系统评价

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摘要

>Background: Current immunodiagnostic tests for tuberculosis (TB) are based on the detection of an immune response toward mycobacterial antigens injected into the skin or following an in-vitro simulation in interferon gamma-release assays. Both tests have limited sensitivity and are unable to differentiate between tuberculosis infection (LTBI) and active tuberculosis disease (aTB). To overcome this, the use of novel Mycobacterium tuberculosis (M. tuberculosis) stage-specific antigens for the diagnosis of LTBI and aTB has gained interest in recent years. This review summarizes current evidence on novel antigens used for the immunodiagnosis of tuberculosis and discrimination of LTBI and aTB. In addition, results on measured biomarkers after stimulation with novel M. tuberculosis antigens were also reviewed.>Methods: A systematic literature review was performed in Pubmed, EMBASE and web of science searching articles from 2000 up until December 2017. Only articles reporting studies in humans using novel antigens were included.>Results: Of 1,533 articles screened 34 were included in the final analysis. A wide range of novel antigens expressed during different stages and types of LTBI and aTB have been assessed. M. tuberculosis antigens Rv0081, Rv1733c, Rv1737c, Rv2029c, Rv2031 and Rv2628, all encoded by the dormancy of survival regulon, were among the most widely studied antigens and showed the most promising results. These antigens have been shown to have best potential for differentiating LTBI from aTB. In addition, several studies have shown that the inclusion of cytokines other than IFN-γ can improve sensitivity.>Conclusion: There is limited evidence that the inclusion of novel antigens as well as the measurement of other biomarkers than IFN-γ may improve sensitivity and may lead to a discrimination of LTBI from aTB.
机译:>背景:当前的结核病(TB)免疫诊断测试是基于对注射到皮肤中的分枝杆菌抗原的免疫反应的检测,或者是在干扰素γ释放试验中进行的体外模拟。两种测试的灵敏度均有限,无法区分结核感染(LTBI)和活动性结核病(aTB)。为了克服这个问题,近年来,新型结核分枝杆菌(M. tuberculosis)阶段特异性抗原在LTBI和aTB诊断中的应用引起了人们的兴趣。这篇综述总结了用于结核病免疫诊断和LTBI和aTB鉴别的新型抗原的最新证据。此外,还审查了新型结核分枝杆菌抗原刺激后测得的生物标志物的结果。>方法:从2000年至2017年12月,在Pubmed,EMBASE和科学网络上进行了系统的文献综述>结果:最终筛选的1,533篇文章中筛选出34篇。已经评估了在LTBI和aTB的不同阶段和类型中表达的各种新型抗原。结核分枝杆菌抗原Rv0081,Rv1733c,Rv1737c,Rv2029c,Rv2031和Rv2628均由存活调节子的休眠编码,是研究最广泛的抗原,并显示出最有希望的结果。这些抗原已显示出将LTBI与aTB区分的最佳潜力。此外,一些研究表明,除IFN-γ以外的其他细胞因子的加入都可以提高敏感性。>结论:仅有有限的证据表明,除IFN以外,还包含新抗原以及其他生物标志物的测定-γ可能会提高灵敏度,并可能导致LTBI与aTB的区别。

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