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Identification of novel Mycobacterium tuberculosis CD4 T-cell antigens via high throughput proteome screening

机译:通过高通量蛋白质组学筛选鉴定新型结核分枝杆菌CD4 T细胞抗原

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摘要

Elicitation of CD4 IFN-gamma T cell responses to Mycobacterium tuberculosis (MTB) is a rational vaccine strategy to prevent clinical tuberculosis. Diagnosis of MTB infection is based on T-cell immune memory to MTB antigens. The MTB proteome contains over four thousand open reading frames (ORFs). We conducted a pilot antigen identification study using 164 MTB proteins and MTB-specific T-cells expanded in vitro from 12 persons with latent MTB infection. Enrichment of MTB-reactive T-cells from PBMC used cell sorting or an alternate system compatible with limited resources. MTB proteins were used as single antigens or combinatorial matrices in proliferation and cytokine secretion readouts. Overall, our study found that 44 MTB proteins were antigenic, including 27 not previously characterized as CD4 T-cell antigens. Antigen truncation, peptide, NTM homology, and HLA class II tetramer studies confirmed malate synthase G (encoded by gene Rv1837) as a CD4 T-cell antigen. This simple, scalable system has potential utility for the identification of candidate MTB vaccine and biomarker antigens.
机译:诱导CD4IFN-γT细胞对结核分枝杆菌(MTB)的反应是预防临床结核病的合理疫苗策略。 MTB感染的诊断基于对MTB抗原的T细胞免疫记忆。 MTB蛋白质组包含4000多个开放阅读框(ORF)。我们进行了一项试验性抗原鉴定研究,使用了164种MTB蛋白和MTB特异性T细胞,这些T细胞在体外从12名潜在MTB感染者中扩增而来。从PBMC中富集MTB反应性T细胞可用于细胞分选或与有限资源兼容的替代系统。 MTB蛋白在增殖和细胞因子分泌读数中用作单一抗原或组合基质。总体而言,我们的研究发现44种MTB蛋白具有抗原性,其中27种以前未鉴定为CD4 T细胞抗原。抗原截短,肽,NTM同源性和HLA II类四聚体研究证实苹果酸合酶G(由基因Rv1837编码)是CD4 T细胞抗原。这个简单,可扩展的系统具有潜在的用途,可用于识别候选MTB疫苗和生物标志物抗原。

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