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HCMV triggers frequent and persistent UL40-specific unconventional HLA-E-restricted CD8 T-cell responses with potential autologous and allogeneic peptide recognition

机译:HCMV触发频繁且持续的UL40特异性非常规HLA-E限制性CD8 T细胞应答并具有潜在的自体和同种异体肽识别能力

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摘要

Immune response against human cytomegalovirus (HCMV) includes a set of persistent cytotoxic NK and CD8 T cells devoted to eliminate infected cells and to prevent reactivation. CD8 T cells against HCMV antigens (pp65, IE1) presented by HLA class-I molecules are well characterized and they associate with efficient virus control. HLA-E-restricted CD8 T cells targeting HCMV UL40 signal peptides (HLA-EUL40) have recently emerged as a non-conventional T-cell response also observed in some hosts. The occurrence, specificity and features of HLA-EUL40 CD8 T-cell responses remain mostly unknown. Here, we detected and quantified these responses in blood samples from healthy blood donors (n = 25) and kidney transplant recipients (n = 121) and we investigated the biological determinants involved in their occurrence. Longitudinal and phenotype ex vivo analyses were performed in comparison to HLA-A*02/pp65-specific CD8 T cells. Using a set of 11 HLA-E/UL40 peptide tetramers we demonstrated the presence of HLA-EUL40 CD8 αβT cells in up to 32% of seropositive HCMV+ hosts that may represent up to 38% of total circulating CD8 T-cells at a time point suggesting a strong expansion post-infection. Host’s HLA-A*02 allele, HLA-E *01:01/*01:03 genotype and sequence of the UL40 peptide from the infecting strain are major factors affecting the incidence of HLA-EUL40 CD8 T cells. These cells are effector memory CD8 (CD45RAhighROlow, CCR7-, CD27-, CD28-) characterized by a low level of PD-1 expression. HLA-EUL40 responses appear early post-infection and display a broad, unbiased, Vβ repertoire. Although induced in HCMV strain-dependent, UL4015-23-specific manner, HLA-EUL40 CD8 T cells are reactive toward a broader set of nonapeptides varying in 1–3 residues including most HLA-I signal peptides. Thus, HCMV induces strong and life-long lasting HLA-EUL40 CD8 T cells with potential allogeneic or/and autologous reactivity that take place selectively in at least a third of infections according to virus strain and host HLA concordance.
机译:针对人类巨细胞病毒(HCMV)的免疫反应包括一组持续的细胞毒性NK和CD8 T细胞,这些细胞专门用于消除感染的细胞并防止其重新激活。由HLA I类分子呈递的针对HCMV抗原(pp65,IE1)的CD8 T细胞已得到很好的表征,并且与有效的病毒控制有关。靶向HCMV UL40信号肽(HLA-EUL40)的HLA-E限制性CD8 T细胞最近作为非常规T细胞应答出现,在某些宿主中也观察到。 HLA-EUL40 CD8 T细胞反应的发生,特异性和特征仍然未知。在这里,我们检测并量化了来自健康献血者(n = 25)和肾脏移植受者(n = 121)的血液样本中的这些反应,并研究了参与其发生的生物学决定因素。与HLA-A * 02 / pp65特异性CD8 T细胞相比,进行了纵向和表型离体分析。使用一组11种HLA-E / UL40肽四聚体,我们证明了高达32%的血清阳性HCMV + 宿主中存在HLA-EUL40 CD8αβT细胞,这可能占总循环的38%在某个时间点,CD8 T细胞提示感染后会强烈扩增。宿主的HLA-A * 02等位基因,HLA-E * 01:01 / * 01:03的基因型和感染株UL40肽的序列是影响HLA-EUL40 CD8 T细胞发生率的主要因素。这些细胞是效应记忆CD8(CD45RA high RO low ,CCR7 -,CD27 -,CD28 -),其特征在于PD-1表达水平低。 HLA-EUL40反应出现在感染后的早期,并显示出广泛的,无偏见的Vβ库。尽管以依赖HCMV株系,UL4015-23的特定方式诱导,HLA-EUL40 CD8 T细胞对更广泛的一组1-3个残基(包括大多数HLA-1信号肽)中的非肽具有反应性。因此,HCMV诱导了具有潜在同种异体或/和自体反应性的强而持久的HLA-EUL40 CD8 T细胞,这些细胞根据病毒株和宿主HLA的一致性在至少三分之一的感染中选择性发生。

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