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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Large spectrum of HLA-C recognition by killer Ig-like receptor (KIR)2DL2 and KIR2DL3 and restricted C1 specificity of KIR2DS2: Dominant impact of KIR2DL2/KIR2DS2 on KIR2D NK cell repertoire formation
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Large spectrum of HLA-C recognition by killer Ig-like receptor (KIR)2DL2 and KIR2DL3 and restricted C1 specificity of KIR2DS2: Dominant impact of KIR2DL2/KIR2DS2 on KIR2D NK cell repertoire formation

机译:杀伤性Ig样受体(KIR)2DL2和KIR2DL3的大范围HLA-C识别以及KIR2DS2的C1特异性受限:KIR2DL2 / KIR2DS2对KIR2D NK细胞库形成的主要影响

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摘要

The interactions of killer Ig-like receptor 2D (KIR2D) with HLA-C ligands contribute to functional NK cell education and regulate NK cell functions. Although simple alloreactive rules have been established for inhibitory KIR2DL, those governing activating KIR2DS function are still undefined, and those governing the formation of the KIR2D repertoire are still debated. In this study, we investigated the specificity of KIR2DL1/2/3 and KIR2DS1/2, dissected each KIR2D function, and assessed the impact of revisited specificities on the KIR2D NK cell repertoire formation from a large cohort of 159 KIR and HLA genotyped individuals. We report that KIR2DL2+ and KIR2DL3 + NK cells reacted similarly against HLA-C+ target cells, irrespective of C1 or C2 allele expression. In contrast, KIR2DL1+ NK cells specifically reacted against C2 alleles, suggesting a larger spectrum of HLA-C recognition by KIR2DL2 and KIR2DL3 than KIR2DL1. KIR2DS2+ KIR2DL2- NK cell clones were C1-reactive irrespective of their HLA-C environment. However, when KIR2DS2 and KIR2DL2 were coexpressed, NK cell inhibition via KIR2DL2 overrode NK cell activation via KIR2DS2. In contrast, KIR2DL1 and KIR2DS2 had an additive enhancing effect on NK cell responses against C1C1 target cells. KIR2DL2/3/S2 NK cells predominated within the KIR repertoire in KIR2DL2/S2+ individuals. In contrast, the KIR2DL1/S1 NK cell compartment is dominant in C2C2 KIR2DL2/S2- individuals. Moreover, our results suggest that together with KIR2DL2, activating KIR2DS1 and KIR2DS2 expression limits KIR2DL1 acquisition on NK cells. Altogether, our results suggest that the NK cell repertoire is remolded by the activating and inhibitory KIR2D and their cognate ligands.
机译:杀伤性Ig样受体2D(KIR2D)与HLA-C配体的相互作用有助于功能性NK细胞的教育和调节NK细胞的功能。尽管已经为抑制性KIR2DL建立了简单的变态反应规则,但仍未定义控制激活KIR2DS功能的规则,而仍在争论控制KIR2D组成库形成的规则。在这项研究中,我们调查了KIR2DL1 / 2/3和KIR2DS1 / 2的特异性,剖析了每个KIR2D功能,并评估了来自159个KIR和HLA基因分型个体的重新研究的特异性对KIR2D NK细胞库构成的影响。我们报告说,无论C1或C2等位基因表达,KIR2DL2 +和KIR2DL3 + NK细胞对HLA-C +目标细胞的反应相似。相反,KIR2DL1 + NK细胞与C2等位基因特异性反应,表明KIR2DL2和KIR2DL3识别的HLA-C光谱要比KIR2DL1大。无论其HLA-C环境如何,KIR2DS2 + KIR2DL2- NK细胞克隆都具有C1反应性。但是,当KIR2DS2和KIR2DL2共表达时,通过KIR2DL2抑制NK细胞将取代通过KIR2DS2激活NK细胞。相反,KIR2DL1和KIR2DS2对NK细胞针对C1C1目标细胞的反应具有加性增强作用。在KIR2DL2 / S2 +个人中,KIR2DL2 / 3 / S2 NK细胞在KIR库中占主导地位。相反,KIR2DL1 / S1 NK细胞区室在C2C2 KIR2DL2 / S2-个人中占主导地位。此外,我们的结果表明,与KIR2DL2一起激活KIR2DS1和KIR2DS2表达会限制NK细胞上KIR2DL1的获得。总而言之,我们的结果表明,NK细胞库被活化和抑制性KIR2D及其同源配体重塑。

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