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首页> 外文期刊>The journal of immunology >HLA-F on HLA-Null 721.221 Cells Activates Primary NK Cells Expressing the Activating Killer Ig-like Receptor KIR3DS1
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HLA-F on HLA-Null 721.221 Cells Activates Primary NK Cells Expressing the Activating Killer Ig-like Receptor KIR3DS1

机译:HLA-Null 721.221细胞上的HLA-F激活表达活化杀伤性Ig样受体KIR3DS1的原代NK细胞

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NK cells elicit important responses against transformed and virally infected cells. Carriage of the gene encoding the activating killer Ig-like receptor KIR3DS1 is associated with slower time to AIDS and protection from HIV infection. Recently, open conformers of the nonclassical MHC class Ib Ag HLA-F were identified as KIR3DS1 ligands. In this study, we investigated whether the interaction of KIR3DS1 on primary NK cells with HLA-F on the HLA-null cell line 721.221 (221) stimulated KIR3DS1sup+/sup NK cells. We used a panel of Abs to detect KIR3DS1sup+/supCD56supdim/sup NK cells that coexpressed the inhibitory NK cell receptors KIR2DL1/L2/L3, 3DL2, NKG2A, and ILT2; the activating NK cell receptors KIR2DS1/S2/S3/S5; and CCL4, IFN-γ, and CD107a functions. We showed that both untreated and acid-pulsed 221 cells induced a similar frequency of KIR3DS1sup+/sup cells to secrete CCL4/IFN-γ and express CD107a with a similar intensity. A higher percentage of KIR3DS1sup+/sup than KIR3DS1sup?/sup NK cells responded to 221 cells when either inclusive or exclusive (i.e., coexpressing none of the other inhibitory NK cell receptors and activating NK cell receptors detected by the Ab panel) gating strategies were employed to identify these NK cell populations. Blocking the interaction of HLA-F on 221 cells with KIR3DS1-Fc chimeric protein or anti–HLA-F Abs on exclusively gated KIR3DS1sup+/sup cells reduced the frequency of functional cells compared with that of unblocked conditions for stimulated KIR3DS1sup+/sup NK cells. Thus, ligation of KIR3DS1 activates primary NK cells for several antiviral functions.
机译:NK细胞引发针对转化和病毒感染细胞的重要反应。编码激活性杀伤性Ig样受体KIR3DS1的基因的携带与爱滋病时间变慢和免受HIV感染有关。最近,非经典MHC Ib Ag HLA-F的开放构象异构体被确定为KIR3DS1配体。在这项研究中,我们调查了原代NK细胞上的KIR3DS1与HLA空细胞系721.221(221)上的HLA-F的相互作用是否刺激了KIR3DS1 + NK细胞。我们使用一组Abs检测共表达抑制性NK细胞受体KIR2DL1 / L2 / L3、3DL2,NKG2A和ILT2的KIR3DS1 + CD56 dim NK细胞。活化的NK细胞受体KIR2DS1 / S2 / S3 / S5; CCL4,IFN-γ和CD107a的功能。我们发现未处理的细胞和经酸脉冲处理的221细胞均诱导相似频率的KIR3DS1 + 细胞分泌CCL4 /IFN-γ,并以相似的强度表达CD107a。当包含或排斥时,KIR3DS1 + 的百分比高于KIR3DS1 ? NK细胞对221细胞的反应(即,共表达其他抑制性NK细胞受体均不表达并激活NK细胞)通过Ab组门控策略检测到的受体被用来鉴定这些NK细胞群体。与非封闭条件刺激相比,用专门封闭的KIR3DS1 + 细胞上的KIR3DS1-Fc嵌合蛋白或抗HLA-F Abs阻断了221细胞上的HLA-F的相互作用,降低了功能细胞的频率。 KIR3DS1 + NK细胞。因此,KIR3DS1的连接激活了原代NK细胞,具有多种抗病毒功能。

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