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HIV-1 Control by NK Cells via Reduced Interaction between KIR2DL2 and HLA-C^*12:02/C^*14:03

机译:通过降低Kir2DL2和HLA-C ^ * 12:02 / C ^ * 14:03,通过降低kir2dl2和hla-c ^ * 14:03的互相控制来控制NK细胞的控制

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Natural killer (NK) cells control viral infection in part through the interaction between killer cell immunoglobulin-like receptors (KIRs) and their human leukocyte antigen (HLA) ligands. We investigated 504 anti-retroviral (ART)-free Japanese patients chronically infected with HIV-1 and identified two KIR/HLA combinations, KIR2DL2/HLA-C^*12:02 and KIR2DL2/HLA-C^*14:03, that impact suppression of HIV-1 replication. KIR2DL2^+ NK cells suppressed viral replication in HLA-C^*14:03^+ or HLA-C^*12:02^+ cells to a significantly greater extent than did KIR2DL2^- NK cells in vitro. Functional analysis showed that the binding between HIV-1-derived peptide and HLA-C^*14:03 or HLA-C^*12:02 influenced KIR2DL2^+ NK cell activity through reduced expression of the peptide-HLA (pHLA) complex on the cell surface (i.e., reduced KIR2DL2 ligand expression), rather than through reduced binding affinity of KIR2DL2 to the respective pHLA complexes. Thus, KIR2DL2/HLA-C^*12:02 and KIR2DL2/HLA-C^*14:03 compound genotypes have protective effects on control of HIV-1 through a mechanism involving KIR2DL2-mediated NK cell recognition of virus-infected cells, providing additional understanding of NK cells in HIV-1 infection.
机译:自然杀伤(NK)细胞通过杀手细胞免疫球蛋白样受体(KIRS)与其人白细胞抗原(HLA)配体的相互作用来控制病毒感染。我们调查了504次抗逆转录病毒(ART) - 免费日本患者慢性感染HIV-1并确定了两种KIR / HLA组合,KIR2DL2 / HLA-C ^ * 12:02和KIR2DL2 / HLA-C ^ * 14:03,即HIV-1复制的影响抑制。 Kir2DL2 ^ + NK细胞在HLA-C ^ * 14:03 ^ +或HLA-C ^ * 12中抑制了病毒复制,比体外kir2dl2 ^-nk细胞显着更大的程度。功能分析表明,HIV-1衍生的肽和HLA-C ^ * 14:03或HLA-C ^ * 12之间的结合通过减少肽-HLA(PHLA)复合物的表达来影响KIR2DL2 ^ + NK细胞活性在细胞表面(即,降低Kir2Dl2配体表达),而不是通过降低Kir2DL2的结合亲和力至相应的Phla络合物。因此,Kir2DL2 / HLA-C ^ * 12:02和Kir2DL2 / HLA-C ^ * 14:03化合物基因型对HIV-1控制的保护作用通过涉及Kir2DL2介导的病毒感染细胞的NK细胞识别的机制,提供对HIV-1感染中NK细胞的额外理解。

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