Department of Virology, Institute of Tropical Medicine, Nagasaki University and Global COE Program, Nagasaki, Japan.
Division of Immunology, Department of Molecular Microbiology and Immunology, Graduate School of Biomedical Sciences, Nagasaki University and Global COE Program, Nagasaki, Japan.
J Gen Virol. 2012 Apr;93(Pt 4):761-770. doi: 10.1099/vir.0.037853-0. Epub 2011 Dec 14.
Dengue virus (DENV) causes fever and severe haemorrhagic symptoms in humans. The DEN2 16681 strain, derived from a dengue haemorrhagic fever patient, has been widely used in studies related to DENV pathogenesis, such as mouse and non-human primate haemorrhagic models and human vascular endothelial-cell permeability. To clarify the entry mechanism of the 16681 strain, we characterized a novel cell receptor for this strain. Our two major findings were as follows: firstly, the SDC2 membrane protein was an effective DEN2 16681 receptor in a cloned K562 cell line. Secondly, a heparan sulfate (HS) glycochain (of four glycochains in SDC2) is the specific binding site of DENV and seems to be involved in tissue-culture adaptation. Our findings present an entry mechanism that could be implicated for DENV adaptation and HS-mediated DENV infection.
登革病毒(DENV)可引起人类发热和严重出血症状。来源于登革出血热患者的 DEN2 16681 株已被广泛应用于与 DENV 发病机制相关的研究,如鼠和非人灵长类动物出血模型和人血管内皮细胞通透性。为了阐明 16681 株的进入机制,我们对该株的一种新型细胞受体进行了鉴定。我们的两项主要发现如下:首先,SDC2 膜蛋白是克隆 K562 细胞系中 DEN2 16681 株的有效受体。其次,硫酸乙酰肝素(HS)聚糖链(SDC2 中的四个糖链之一)是 DENV 的特异性结合位点,似乎参与了组织培养适应。我们的发现提出了一种进入机制,可能与 DENV 的适应和 HS 介导的 DENV 感染有关。
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