首页> 外文期刊>European Journal of Immunology >Human peripheral blood and bone marrow Epstein-Barr virus-specific T-cell repertoire in latent infection reveals distinct memory T-cell subsets.
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Human peripheral blood and bone marrow Epstein-Barr virus-specific T-cell repertoire in latent infection reveals distinct memory T-cell subsets.

机译:人类外周血和骨髓巴尔病毒特异性t细胞剧目潜伏性感染了不同的记忆t细胞子集。

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摘要

EBV infection leads to life-long viral persistence. Although EBV infection can result in chronic disease and malignant transformation, most carriers remain disease-free as a result of effective control by T cells. EBV-specific IFN-gamma-producing T cells could be demonstrated in acute and chronic infection as well as during latency. Recent studies, however, provide evidence that assessing IFN-gamma alone is insufficient to assess the quantity and quality of a T-cell response. Using overlapping peptide pools of latent EBV nuclear antigen 1 and lytic BZLF-1 protein and multicolor flow cytometry, we demonstrate that the majority of ex vivo EBV-reactive T cells in healthy virus carriers are indeed IL-2- and/or TNF-producing memory cells, the latter being significantly more frequent in BM. After in vitro expansion, a substantial number of EBV-specific CD4(+) and CD8(+) T cells retained a CC-chemokine receptor 7 (CCR7)-positive memory phenotype. Based on their cytokine profiles, six different EBV-specific T-cell subsets could be distinguished with TNF-single or TNF/IL-2-double producing cells expressing the highest CCR7 levels resembling early-differentiated memory T cells. Our study delineates the memory T-cell profile of a protective immune response and provides a basis for analyzing T-cell responses in EBV-associated diseases.
机译:EBV感染会导致终身病毒持久性。慢性疾病和恶性转化,大多数携带者仍然无病的结果有效控制的T细胞。IFN-gamma-producing T细胞可以证明在急性和慢性感染延迟。证据表明IFN-gamma单独评估评估数量和质量不足t细胞的反应。的潜伏池EBV核抗原1和溶解性BZLF-1蛋白质和多色流式细胞术,我们证明大多数体外EBV-reactive T细胞在健康的病毒携带者确实是- - - - - - - 2和/或TNF-producing记忆细胞,后者更多在BM频繁。大量的EBV-specific CD4 (+)CD8 (+) T细胞保留CC-chemokine受体7(其)阳性内存表型。细胞因子资料,六种不同的EBV-specifict细胞可以子集TNF-single或TNF / IL-2-double生产细胞最高CCR7表达类似的水平early-differentiated记忆T细胞。则勾勒出记忆t细胞轮廓度保护性免疫反应和提供了一个基础在EBV-associated分析t细胞反应疾病。

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