首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Human Cytomegalovirus Infection Promotes Expansion of a Functionally Superior Cytoplasmic CD3~+ NK Cell Subset with a Bcl11b-Regulated T Cell Signature
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Human Cytomegalovirus Infection Promotes Expansion of a Functionally Superior Cytoplasmic CD3~+ NK Cell Subset with a Bcl11b-Regulated T Cell Signature

机译:人巨细胞病毒感染促进具有 Bcl11b 调节的 T 细胞特征的功能优越的细胞质 CD3~+ NK 细胞亚群的扩增

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摘要

Human CMV (HCMV) is a ubiquitous pathogen that indelibly shapes the NK cell repertoire. Using transcriptomic, epigenoimic, and proteomic approaches to evaluate peripheral blood NK cells from healthy human volunteers, we find that prior HCMV infection promotes NK cells with a T cell-like gene profile, including the canonical markers CD3ε, CD5, and CD8β, as well as the T cell lineage-commitment transcription factor Bcl11b. Although Bcl11b expression is upregulated during NK maturation from CD56~bright to CD56~dim, we find a Bcl11b-mediated signature at the protein level for FCεRIγ, PLZF, IL-2Rβ, CD3γ, CD3δ, and CD3ε in later-stage, HCMV-induced NK cells. BCL11B is targeted by Notch signaling in T cell development, and culture of NK cells with Notch ligand increases cytoplasmic CD3ε expression. The Bclllb-mediated gain of CD3ε, physically associated with CD16 signaling molecules Lck and CD247 in NK cells is correlated with increased Ab-dependent effector function, including against HCMV-infected cells, identifying a potential mechanism for their prevalence in HCMV-infected individuals and their prospective clinical use in Ab-based therapies.
机译:人巨细胞病毒(HCMV)是一种无处不在的病原体,不可磨灭地塑造了NK细胞库。使用转录组学、表观基因组学和蛋白质组学方法来评估来自健康人类志愿者的外周血 NK 细胞,我们发现先前的 HCMV 感染促进具有 T 细胞样基因谱的 NK 细胞,包括典型标记物 CD3ε、CD5 和 CD8β,以及 T 细胞谱系承诺转录因子 Bcl11b。尽管 Bcl11b 表达在 NK 成熟过程中从 CD56~明亮到 CD56~dim 上调,但在后期 HCMV 诱导的 NK 细胞中,我们发现 FCεRIγ、PLZF、IL-2Rβ、CD3γ、CD3δ 和 CD3ε 在蛋白质水平上具有 Bcl11b 介导的特征。BCL11B 在 T 细胞发育中被 Notch 信号转导靶向,用 Notch 配体培养 NK 细胞可增加细胞质 CD3ε 表达。Bclllb介导的CD3ε增益与NK细胞中的CD16信号分子Lck和CD247物理相关,与Ab依赖性效应功能增加相关,包括针对HCMV感染的细胞,确定了它们在HCMV感染个体中流行的潜在机制及其在基于Ab的治疗中的前瞻性临床应用。

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