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CD56-negative NK cells with impaired effector function expand in CMV and EBV co-infected healthy donors with age

机译:效应子功能受损的CD56阴性NK细胞随着年龄的增长而在CMV和EBV共同感染的健康供体中扩增

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摘要

Natural killer cells lacking expression of CD56 (CD56neg NK cells) have been described in chronic HIV and hepatitis C virus infection. Features and functions of CD56neg NK cells in the context of latent infection with CMV and / or EBV with age are not known. In a cohort of healthy donors >60 years of age, we found that co-infection with CMV and EBV drives expansion of CD56neg NK cells. Functionally, CD56neg NK cells displayed reduced cytotoxic capacity and IFN-γ production, a feature that was enhanced with CMV / EBV co-infection. Further, the frequency of CD56neg NK cells correlated with accumulation of end-stage-differentiated T cells and a reduced CD4 / CD8 T cell ratio, reflecting an immune risk profile. CD56neg NK cells had a mature phenotype characterized by low CD57 and KIR expression and lacked characteristics of cell senescence. No changes in their activating NK cell receptor expression, and no upregulation of the negative co-stimulation receptors PD-1 or TIM-3 were observed. In all, our data identify expansion of dysfunctional CD56neg NK cells in CMV+EBV+ elderly individuals suggesting that these cells may function as shape-shifters of cellular immunity and argue for a previously unrecognized role of EBV in mediating immune risk in the elderly.
机译:在慢性HIV和丙型肝炎病毒感染中已经描述了缺乏CD56表达的自然杀伤细胞(CD56 neg NK细胞)。尚不知道CD56 neg NK细胞在年龄潜在感染CMV和/或EBV的情况下的特征和功能。在一群年龄超过60岁的健康供体中,我们发现CMV和EBV共同感染可驱动CD56 neg NK细胞的扩增。在功能上,CD56 neg NK细胞显示出降低的细胞毒性能力和IFN-γ的产生,这一特征可通过CMV / EBV共感染得到增强。此外,CD56 neg NK细胞的频率与终末分化T细胞的积累和CD4 / CD8 T细胞比率降低相关,反映了免疫风险状况。 CD56 neg NK细胞具有成熟的表型,其特征是CD57和KIR表达低,缺乏细胞衰老特性。没有观察到它们的活化性NK细胞受体表达的变化,也没有观察到阴性共刺激受体PD-1或TIM-3的上调。总而言之,我们的数据确定了CMV + EBV + 老年人中功能异常的CD56 neg NK细胞的扩增,提示这些细胞可能起着形状-并证明了EBV在介导老年人免疫风险中的作用是前所未有的。

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