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Natural Killer Cells in Human Immunodeficiency Virus-1 Infection: Spotlight on the Impact of Human Cytomegalovirus

机译:人类免疫缺陷病毒-1感染中的自然杀伤细胞:对人类巨细胞病毒影响的关注。

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摘要

Human cytomegalovirus (HCMV) has been closely associated with the human race across evolutionary time. HCMV co-infection is nearly universal in human immunodeficiency virus-1 (HIV-1)-infected individuals and remains an important cofactor in HIV-1 disease progression even in the era of effective antiretroviral treatment. HCMV infection has been shown to have a broad and potent influence on the human immune system and has been linked with the discovery and characterization of adaptive natural killer (NK) cells. Distinct NK-cell subsets, predominately expressing the activating receptor NKG2C and the marker of terminal differentiation CD57, expand in response to HCMV. These NK-cell populations engaged in the long-lasting interaction with HCMV, in addition to characteristic but variable expression of surface receptors, exhibit reduced expression of signaling proteins and transcription factors expressed by canonical NK cells. Broad epigenetic modifications drive the emergence and persistence of HCMV-adapted NK cells that have distinct functional characteristics. NKG2C+ NK-cell expansions have been observed in HIV-1 infected patients and other acute and chronic viral infections being systematically associated with HCMV seropositivity. The latter is potentially an important confounding variable in studies focused on the cellular NK-cell receptor repertoire and functional capacity. Here, focusing on HIV-1 infection we review the evidence in favor of “adaptive” changes likely induced by HCMV co-infection in NK-cell subsets. We highlight a number of key questions and how insights into the adaptive behavior of NK cells will inform new strategies exploiting their unique properties in the fight against HIV-1.
机译:人类巨细胞病毒(HCMV)与人类在整个进化时期都息息相关。 HCMV合并感染在感染人类免疫缺陷病毒1(HIV-1)的个体中几乎普遍存在,即使在有效的抗逆转录病毒治疗时代,HCMV合并感染仍是HIV-1疾病进展的重要辅助因素。 HCMV感染已显示对人体免疫系统具有广泛而有效的影响,并已与适应性自然杀伤(NK)细胞的发现和表征有关。分别表达激活受体NKG2C和终末分化CD57标记的不同NK细胞亚群在响应HCMV时会扩展。这些NK细胞群体与HCMV长期相互作用,除了表面受体的特征性表达不同外,还表现出规范性NK细胞表达的信号蛋白和转录因子表达降低。广泛的表观遗传修饰驱动具有独特功能特征的HCMV适应性NK细胞的出现和持久性。在HIV-1感染的患者以及其他与HCMV血清阳性系统相关的急性和慢性病毒感染中,已观察到NKG2C + NK细胞扩增。在专注于细胞NK细胞受体库和功能能力的研究中,后者可能是一个重要的混淆变量。在这里,我们以HIV-1感染为重点,回顾了支持NK细胞亚群中HCMV共感染可能引起的“适应性”变化的证据。我们重点介绍了一些关键问题,以及对NK细胞适应行为的见识将如何为在对抗HIV-1的斗争中利用其独特特性的新策略提供信息。

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