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HLA-B signal peptide polymorphism influences the rate of HIV-1 acquisition but not viral load

机译:HLA-B信号肽多态性影响HIV-1的获取率,但不影响病毒载量

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Human leukocyte antigen alleles influence the immune response to HIV-1. Signal peptides cleaved from those alleles bind to HLA-E and mediate natural killer cell function. Signal peptides of HLA-A and HLA-C proteins carry methionine (Met) at anchor position 2 (P2); those of HLA-B carry Met or threonine (Thr). Different P2 residues alter HLA-E binding to its cognate receptors and may impact HIV-1 acquisition. Among Zambian couples (N = 566) serodiscordant for HIV-1, P2-Met accelerated acquisition in the HIV-1-negative partner (relative hazard [RH], 1.79). Among seroconverting Zambian (n = 240) and Rwandan (n = 64) partners, P2-Met also accelerated acquisition (RH, 1.47 and RH, 1.83 respectively). HLA-B alleles displaying the reportedly protective Bw4 epitope carry P2-Thr. Bw4/P2-Thr and Bw6/P2-Thr showed similar protective effects compared with Bw6/P2-Met. Neither motif was associated with viral load. The influence of HLA-B alleles on HIV/AIDS may derive from multiple motifs in and beyond the mature proteins.
机译:人白细胞抗原等位基因影响对HIV-1的免疫反应。从这些等位基因切割的信号肽与HLA-E结合并介导自然杀伤细胞功能。 HLA-A和HLA-C蛋白的信号肽在锚位2(P2)上带有蛋氨酸(Met); HLA-B的那些携带Met或苏氨酸(Thr)。不同的P2残基会改变HLA-E与其同源受体的结合,并可能影响HIV-1的获得。在赞比亚夫妇(N = 566)HIV-1血清抗粘剂中,P2-Met促进了HIV-1阴性伴侣的获取(相对危险度[RH],1.79)。在进行血清转化的赞比亚(n = 240)和卢旺达(n = 64)伙伴中,P2-Met也加快了采集速度(分别为RH,1.47和RH,1.83)。显示据报道具有保护性的Bw4表位的HLA-B等位基因携带P2-Thr。与Bw6 / P2-Met相比,Bw4 / P2-Thr和Bw6 / P2-Thr显示出相似的保护作用。两种基序均与病毒载量无关。 HLA-B等位基因对HIV / AIDS的影响可能来自成熟蛋白内外的多个基序。

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