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首页> 外文期刊>The Journal of Experomental Medicine >Clustered Mutations in HIV-1 Gag Are Consistently Required for Escape from Hla-B27–Restricted Cytotoxic T Lymphocyte Responses
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Clustered Mutations in HIV-1 Gag Are Consistently Required for Escape from Hla-B27–Restricted Cytotoxic T Lymphocyte Responses

机译:从Hla-B27限制的细胞毒性T淋巴细胞反应中逃脱,始终需要HIV-1聚簇的突变。

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摘要

The immune response to HIV-1 in patients who carry human histocompatibility leukocyte antigen (HLA)-B27 is characterized by an immunodominant response to an epitope in p24 gag (amino acids 263–272, KRWIILGLNK). Substitution of lysine (K) or glycine (G) for arginine (R) at HIV-1 gag residue 264 (R264K and R264G) results in epitopes that bind to HLA-B27 poorly. We have detected a R264K mutation in four patients carrying HLA-B27. In three of these patients the mutation occurred late, coinciding with disease progression. In another it occurred within 1 yr of infection and was associated with a virus of syncytium-inducing phenotype. In each case, R264K was tightly associated with a leucine to methionine change at residue 268. After the loss of the cytotoxic T lymphocyte (CTL) response to this epitope and in the presence of high viral load, reversion to wild-type sequence was observed. In a fifth patient, a R264G mutation was detected when HIV-1 disease progressed. Its occurrence was associated with a glutamic acid to aspartic acid mutation at residue 260. Phylogenetic analyses indicated that these substitutions emerged under natural selection rather than by genetic drift or linkage. Outgrowth of CTL escape viruses required high viral loads and additional, possibly compensatory, mutations in the gag protein.
机译:携带人类组织相容性白细胞抗原(HLA)-B27的患者对HIV-1的免疫反应的特征是对p24 gag(氨基酸263-272,KRWIILGLNK)中一个表位的免疫反应强。在HIV-1 gag残基264(R264K和R264G)上用赖氨酸(K)或甘氨酸(G)取代精氨酸(R)会导致表位与HLA-B27的结合不良。我们在四名携带HLA-B27的患者中检测到R264K突变。其中三例患者的突变发生较晚,与疾病进展相吻合。另一种是在感染后1年内发生,并与合胞体诱导型病毒有关。在每种情况下,R264K都与残基268上的亮氨酸变为蛋氨酸紧密相关。在失去对该表位的细胞毒性T淋巴细胞(CTL)反应之后,并且在高病毒载量下,观察到回复到野生型序列。在第五名患者中,当HIV-1疾病进展时检测到R264G突变。它的出现与残基260处的谷氨酸突变为天冬氨酸有关。系统发育分析表明,这些取代是在自然选择下出现的,而不是通过遗传漂移或连锁产生的。 CTL逃逸病毒的生长需要高病毒载量和gag蛋白的额外(可能是补偿性)突变。

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