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冈比亚婴儿的巨细胞病毒感染会导致深刻的CD8 T细胞分化。

Cytomegalovirus infection in Gambian infants leads to profound CD8 T-cell differentiation.

作者信息

Miles David J C, van der Sande Marianne, Jeffries David, Kaye Steve, Ismaili Jamila, Ojuola Olubukola, Sanneh Mariama, Touray Ebrima S, Waight Pauline, Rowland-Jones Sarah, Whittle Hilton, Marchant Arnaud

机构信息

MRC Laboratories Gambia, P.O. Box 273, Banjul, The Gambia.

出版信息

J Virol. 2007 Jun;81(11):5766-76. doi: 10.1128/JVI.00052-07. Epub 2007 Mar 21.

Abstract

Cytomegalovirus (CMV) infection is endemic in Gambian infants, with 62% infected by 3 months and 85% by 12 months of age. We studied the CD8 T-cell responses of infants to CMV following primary infection. CMV-specific CD8 T cells, identified with tetramers, showed a fully differentiated phenotype (CD28(-) CD62L(-) CD95(+) perforin(+) granzyme A(+) Bcl-2(low)). Strikingly, the overall CD8 T-cell population developed a similar phenotype following CMV infection, which persisted for at least 12 months. In contrast, primary infection was accompanied by up-regulation of markers of activation (CD45R0 and HLA-D) on both CMV-specific cells and the overall CD8 T-cell population and division (Ki-67) of specific cells, but neither pattern persisted. At 12 months of age, the CD8 T-cell population of CMV-infected infants was more differentiated than that of uninfected infants. Although the subpopulation of CMV-specific cells remained constant, the CMV peptide-specific gamma interferon response was lower in younger infants and increased with age. As the CD8 T-cell phenotype induced by CMV is indicative of immune dysfunction in the elderly, the existence of a similar phenotype in large numbers of Gambian infants raises the question of whether CMV induces a similarly deleterious effect.

摘要

巨细胞病毒(CMV)感染在冈比亚婴儿中呈地方性流行,3个月龄时62%的婴儿被感染,12个月龄时85%的婴儿被感染。我们研究了婴儿初次感染CMV后CD8 T细胞的反应。用四聚体鉴定的CMV特异性CD8 T细胞表现出完全分化的表型(CD28(-) CD62L(-) CD95(+) 穿孔素(+) 颗粒酶A(+) Bcl-2(低))。令人惊讶的是,CMV感染后整个CD8 T细胞群体呈现出相似的表型,且这种表型持续至少12个月。相比之下,初次感染伴随着CMV特异性细胞和整个CD8 T细胞群体上激活标志物(CD45R0和HLA-D)的上调以及特异性细胞分裂(Ki-67),但这两种模式都没有持续下去。在12个月龄时,CMV感染婴儿的CD8 T细胞群体比未感染婴儿的更分化。虽然CMV特异性细胞亚群保持不变,但CMV肽特异性γ干扰素反应在较小婴儿中较低,并随年龄增加。由于CMV诱导的CD8 T细胞表型表明老年人存在免疫功能障碍,大量冈比亚婴儿中存在类似表型引发了CMV是否会诱导类似有害作用的问题。

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