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CD56 明亮型自然杀伤细胞亚群:对白细胞介素-2和c-kit配体不同功能反应的特征

CD56bright natural killer cell subsets: characterization of distinct functional responses to interleukin-2 and the c-kit ligand.

作者信息

Carson W E, Fehniger T A, Caligiuri M A

机构信息

Department of Surgery, Roswell Park Cancer Institute, Buffalo, NY 14263, USA.

出版信息

Eur J Immunol. 1997 Feb;27(2):354-60. doi: 10.1002/eji.1830270203.

Abstract

Natural killer (NK) cells are bone marrow-derived large granular lymphocytes that express the CD56 surface antigen. The CD56bright NK subset represents approximately 10% of all NK cells and is thought to be the least differentiated NK cell component in blood. The most mature NK cell expresses CD56 at low density and CD16 (FcR gammaIII) at high density, whereas CD56bright NK cells either lack CD16 (CD56bright CD16-) or express it at low density (CD56bright CD16dim). c-kit is a tyrosine kinase receptor which is expressed on both CD34+ hematopoietic precursor cells and CD56bright NK cells. In the current study, we characterize interleukin (IL)-2 receptor (IL-2R) and c-kit expression in each of the CD56bright subsets. Both the CD56bright CD16- and CD56bright CD16dim NK subsets express the high-affinity IL-2R and the c-kit receptor when isolated from fresh blood. However, each CD56bright NK cell subset has distinct functional responses to IL-2, the c-kit ligand (KL), or both. Activation of the high-affinity IL-2R on CD56bright CD16- NK cells induces a proliferative response that is significantly weaker than that observed in the CD56bright CD16dim NK cell subset. Incubation of the CD56bright CD16 NK cell subset with KL significantly enhances IL-2-induced proliferation, while KL has no such effect on the CD56bright CD16dim NK subset. Activation of the high-affinity IL-2R in both CD56bright subsets induces lymphokine-activated killer (LAK) activity, but the addition of KL has no effect on LAK activity. Co-stimulation of either CD56bright subset with IL-12 and concentrations of IL-2 that only saturate the high-affinity IL-2R induces substantial interferon (IFN)-gamma production. The addition of KL to this co-stimulatory signal enhances IFN-gamma production in both CD56bright NK subsets. The distinct functional responses to IL-2 and KL seen in the CD56bright CD16- and CD56bright CD16dim NK subsets provide insight into IL-2R signaling and suggest that each phenotype identifies a discrete stage of NK cell differentiation.

摘要

自然杀伤(NK)细胞是源自骨髓的大颗粒淋巴细胞,表达CD56表面抗原。CD56bright NK亚群约占所有NK细胞的10%,被认为是血液中分化程度最低的NK细胞成分。最成熟的NK细胞低密度表达CD56,高密度表达CD16(FcRγIII),而CD56bright NK细胞要么缺乏CD16(CD56bright CD16-),要么低密度表达CD16(CD56bright CD16dim)。c-kit是一种酪氨酸激酶受体,在CD34+造血前体细胞和CD56bright NK细胞上均有表达。在本研究中,我们对每个CD56bright亚群中的白细胞介素(IL)-2受体(IL-2R)和c-kit表达进行了表征。从新鲜血液中分离出来时,CD56bright CD16-和CD56bright CD16dim NK亚群均表达高亲和力IL-2R和c-kit受体。然而,每个CD56bright NK细胞亚群对IL-2、c-kit配体(KL)或两者都有不同的功能反应。CD56bright CD16- NK细胞上高亲和力IL-2R的激活诱导的增殖反应明显弱于CD56bright CD16dim NK细胞亚群中观察到的增殖反应。用KL孵育CD56bright CD16 NK细胞亚群可显著增强IL-2诱导的增殖,而KL对CD56bright CD16dim NK亚群没有这种作用。两个CD56bright亚群中高亲和力IL-2R的激活均诱导淋巴因子激活的杀伤(LAK)活性,但添加KL对LAK活性没有影响。用IL-12和仅使高亲和力IL-2R饱和的IL-2浓度对任一CD56bright亚群进行共刺激可诱导大量干扰素(IFN)-γ产生。向该共刺激信号中添加KL可增强两个CD56bright NK亚群中的IFN-γ产生。在CD56bright CD16-和CD56bright CD16dim NK亚群中观察到的对IL-2和KL的不同功能反应为IL-2R信号传导提供了见解,并表明每种表型都识别NK细胞分化的一个离散阶段。

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