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人类巨细胞病毒的五聚体复合物:细胞嗜性、病毒传播、免疫反应及疫苗开发

The pentameric complex of human Cytomegalovirus: cell tropism, virus dissemination, immune response and vaccine development.

作者信息

Gerna Giuseppe, Revello Maria Grazia, Baldanti Fausto, Percivalle Elena, Lilleri Daniele

机构信息

Experimental Research Laboratories, Fondazione IRCCS Policlinico San Matteo, Pavia, Italy.

Obstetrics and Gynecology Clinics, University of Pavia, Pavia, Italy.

出版信息

J Gen Virol. 2017 Sep;98(9):2215-2234. doi: 10.1099/jgv.0.000882. Epub 2017 Aug 15.

Abstract

Between the 1980s and 1990s, three assays were developed for diagnosis of human cytomegalovirus (HCMV) infections: leuko (L)-antigenemia, l-viremia and l-DNAemia, detecting viral protein pp65, infectious virus and viral DNA, respectively, in circulating leukocytes Repeated initial attempts to reproduce the three assays in vitro using laboratory-adapted strains and infected cell cultures were consistently unsuccessful. Results were totally reversed when wild-type HCMV strains were used to infect either fibroblasts or endothelial cells. Careful analysis and sequencing of plaque-purified viruses from recent clinical isolates drew attention to the ULb' region of the HCMV genome. Using bacterial artificial chromosome technology, it was shown by both gain-of-function and loss-of-function experiments that UL131-128 genes are indispensable for virus growth in endothelial cells and virus transfer to leukocytes. In addition, a number of clinical isolates passaged in human fibroblasts had lost both properties (leuko-tropism and endothelial cell-tropism) when displaying a mutation in the UL131-128 locus (referred to as UL128L). In the following years, it was shown that pUL128L was complexed with gH and gL to form the pentameric complex (PC), which is required to infect endothelial, epithelial and myeloid cells. The immune response to PC was studied extensively, particularly its humoral component, showing that the great majority of the neutralizing antibody response is directed to PC. Although anti-HCMV antibodies may act with other mechanisms than mere neutralizing activity, these findings definitely favour their protective activity, thus paving the way to the development of a potentially protective HCMV vaccine.

摘要

在20世纪80年代至90年代期间,开发了三种用于诊断人巨细胞病毒(HCMV)感染的检测方法:白细胞(L)抗原血症、L病毒血症和L DNA血症,分别检测循环白细胞中的病毒蛋白pp65、感染性病毒和病毒DNA。最初多次尝试使用实验室适应株和感染的细胞培养物在体外重现这三种检测方法,但一直未成功。当使用野生型HCMV株感染成纤维细胞或内皮细胞时,结果完全相反。对近期临床分离株的空斑纯化病毒进行仔细分析和测序后,人们将注意力集中到了HCMV基因组的ULb'区域。利用细菌人工染色体技术,通过功能获得和功能丧失实验表明,UL131 - 128基因对于病毒在内皮细胞中的生长以及病毒向白细胞的转移是不可或缺的。此外,一些在人成纤维细胞中传代的临床分离株在UL131 - 128位点(称为UL128L)发生突变时,失去了这两种特性(嗜白细胞性和嗜内皮细胞性)。在接下来的几年里,研究表明pUL128L与gH和gL复合形成五聚体复合物(PC),这是感染内皮细胞、上皮细胞和髓样细胞所必需的。对PC的免疫反应进行了广泛研究,尤其是其体液成分,结果表明绝大多数中和抗体反应都针对PC。尽管抗HCMV抗体可能通过除单纯中和活性之外的其他机制发挥作用,但这些发现无疑有利于其保护活性,从而为开发一种潜在的保护性HCMV疫苗铺平了道路。

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