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Circulating Mycobacterium tuberculosis DosR latency antigen-specific polyfunctional regulatory IL10+ Th17 CD4 T-cells differentiate latent from active tuberculosis

机译:循环结核分枝杆菌DosR潜伏期抗原特异性多功能调节性IL10 + Th17 CD4 T细胞区分潜伏性结核与活动性结核

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摘要

The functional heterogeneity of T cell responses to diverse antigens expressed at different stages of Mycobacterium tuberculosis (Mtb) infection, in particular early secreted versus dormancy related latency antigens expressed later, that distinguish subjects with latent (LTBI), pulmonary (PTB) or extrapulmonary (EPTB) tuberculosis remains unclear. Here we show blood central memory CD4 T-cell responses specific to Mtb dormancy related (DosR) latency, but not classical immunodominant secretory antigens, to clearly differentiate LTBI from EPTB and PTB. The polyfunctionality score integrating up to 31 DosR-specific CD4 T-cell functional profiles was significantly higher in LTBI than EPTB or PTB subjects. Further analysis of 256 DosR-specific T-cell functional profiles identified regulatory IL10 + Th17 cells (IL10+IL17A+IL17F+IL22+) to be significantly enriched in LTBI; in contrast to pro-inflammatory Th17 cells (IFNγ+IL17A+/IL10) in the blood and lung of EPTB and PTB subjects respectively. A blood polyfunctional, Mtb DosR latency antigen specific, regulatory, central memory response is therefore a novel functional component of T-cell immunity in latent TB and potential correlate of protection.
机译:T细胞对在结核分枝杆菌(Mtb)感染的不同阶段表达的多种抗原的反应的功能异质性,特别是早期表达的与后期表达的与休眠相关的潜伏期抗原,这些抗原区分具有潜伏性(LTBI),肺部(PTB)或肺外( EPTB)结核病仍不清楚。在这里,我们显示了特定于Mtb休眠相关(DosR)潜伏期的血液中枢记忆CD4 T细胞应答,而不是经典的免疫显性分泌抗原,以清楚地区分LTBI与EPTB和PTB。在LTBI中,整合多达31个DosR特异性CD4 T细胞功能特征的多功能评分显着高于EPTB或PTB受试者。进一步分析256种DosR特异性T细胞功能图谱可发现调节性IL10 + Th17细胞(IL10 + IL17A + IL17F + < / sup> IL22 + )以显着丰富LTBI;分别与EPTB和PTB受试者的血液和肺中促炎性Th17细胞(IFNγ + IL17A + / IL10 -)相反。因此,血液多功能Mtb DosR潜伏期抗原特异性的调节性中枢记忆反应是潜在TB中T细胞免疫力的新功能成分,并且是保护的潜在相关因素。

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