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分析表达 CX3CR1 的自然杀伤细胞的表型和功能特征。

Analyses of phenotypic and functional characteristics of CX3CR1-expressing natural killer cells.

机构信息

Experimental and Clinical Research Centre, Charité-Universitätsmedizin Berlin, Berlin, Germany.

出版信息

Immunology. 2011 May;133(1):62-73. doi: 10.1111/j.1365-2567.2011.03409.x. Epub 2011 Feb 14.

DOI:10.1111/j.1365-2567.2011.03409.x
PMID:21320123
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3088968/
Abstract

We previously demonstrated a correlation between the frequency of CX3CR1-expressing human natural killer (NK) cells and disease activity in multiple sclerosis and showed that CX3CR1(high) NK cells were more cytotoxic than their CX3CR1(neg/low) counterparts. Here we aimed to determine whether human NK cell fractions defined by CX3CR1 represent distinct subtypes. Phenotypic and functional NK cell analyses revealed that, distinct from CX3CR1(high), CX3CR1(neg/low) NK cells expressed high amounts of type 2 cytokines, proliferated robustly in response to interleukin-2 and promoted a strong up-regulation of the key co-stimulatory molecule CD40 on monocytes. Co-expression analyses of CX3CR1 and CD56 demonstrated the existence of different NK cell fractions based on the surface expression of these two surface markers, the CX3CR1(neg) CD56(bright), CX3CR1(neg) CD56(dim) and CX3CR1(high) CD56(dim) fractions. Additional investigations on the expression of NK cell receptors (KIR, NKG2A, NKp30 and NKp46) and the maturation markers CD27, CD62L and CD57 indicated that CX3CR1 expression of CD56(dim) discriminated between an intermediary CX3CR1(neg)  CD56(dim) and fully mature CX3CR1(high) CD56(dim) NK cell fractions. Hence, CX3CR1 emerges as an additional differentiation marker that may link NK cell maturation with the ability to migrate to different organs including the central nervous system.

摘要

我们之前已经证明了 CX3CR1 表达的人类自然杀伤 (NK) 细胞的频率与多发性硬化症的疾病活动之间存在相关性,并表明 CX3CR1(高)NK 细胞比其 CX3CR1(neg/low)对应物更具细胞毒性。在这里,我们旨在确定通过 CX3CR1 定义的人类 NK 细胞亚群是否代表不同的亚型。表型和功能 NK 细胞分析表明,与 CX3CR1(高)不同,CX3CR1(neg/low)NK 细胞表达大量 2 型细胞因子,对白细胞介素-2 反应强烈增殖,并强烈上调单核细胞上关键共刺激分子 CD40。CX3CR1 和 CD56 的共表达分析表明,基于这两个表面标志物的表面表达,存在不同的 NK 细胞亚群,即 CX3CR1(neg)CD56(bright)、CX3CR1(neg)CD56(dim)和 CX3CR1(high)CD56(dim)亚群。对 NK 细胞受体 (KIR、NKG2A、NKp30 和 NKp46) 的表达和成熟标志物 CD27、CD62L 和 CD57 的进一步研究表明,CD56(dim)上的 CX3CR1 表达将中间 CX3CR1(neg)CD56(dim)和完全成熟的 CX3CR1(high)CD56(dim)NK 细胞亚群区分开来。因此,CX3CR1 作为一个额外的分化标志物出现,它可能将 NK 细胞成熟与迁移到包括中枢神经系统在内的不同器官的能力联系起来。

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