首页> 美国卫生研究院文献>Journal of Virology >Efficient Subgroup C Avian Sarcoma and Leukosis Virus Receptor Activity Requires the IgV Domain of the Tvc Receptor and Proper Display on the Cell Membrane
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Efficient Subgroup C Avian Sarcoma and Leukosis Virus Receptor Activity Requires the IgV Domain of the Tvc Receptor and Proper Display on the Cell Membrane

机译:高效的C组禽肉瘤和白血病病毒受体活性需要Tvc受体的IgV结构域和在细胞膜上的正确显示

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摘要

We recently identified and cloned the receptor for subgroup C avian sarcoma and leukosis viruses [ASLV(C)], i.e., Tvc, a protein most closely related to mammalian butyrophilins, which are members of the immunoglobulin protein family. The extracellular domain of Tvc contains two immunoglobulin-like domains, IgV and IgC, which presumably each contain a disulfide bond important for native function of the protein. In this study, we have begun to identify the functional determinants of Tvc responsible for ASLV(C) receptor activity. We found that the IgV domain of the Tvc receptor is responsible for interacting with the glycoprotein of ASLV(C). Additional experiments demonstrated that a domain was necessary as a spacer between the IgV domain and the membrane-spanning domain for efficient Tvc receptor activity, most likely to orient the IgV domain a proper distance from the cell membrane. The effects on ASLV(C) glycoprotein binding and infection efficiency were also studied by site-directed mutagenesis of the cysteine residues of Tvc as well as conserved amino acid residues of the IgV Tvc domain compared to other IgV domains. In this initial analysis of Tvc determinants important for interacting with ASLV(C) glycoproteins, at least two aromatic amino acid residues in the IgV domain of Tvc, Trp-48 and Tyr-105, were identified as critical for efficient ASLV(C) infection. Interestingly, one or more aromatic amino acid residues have been identified as critical determinants in the other ASLV(A-E) receptors for a proper interaction with ASLV glycoproteins. This suggests that the ASLV glycoproteins may share a common mechanism of receptor interaction with an aromatic residue(s) on the receptor critical for triggering conformational changes in SU that initiate the fusion process required for efficient virus infection.
机译:最近,我们鉴定并克隆了C亚群肉瘤和白血病病毒亚组[ASLV(C)]的受体,即Tvc,Tvc是与免疫球蛋白家族的成员,但与哺乳动物嗜酪蛋白最密切相关的一种蛋白。 Tvc的胞外结构域包含两个免疫球蛋白样结构域IgV和IgC,大概每个结构域都包含一个对蛋白质天然功能重要的二硫键。在这项研究中,我们已经开始确定负责ASLV(C)受体活性的Tvc的功能决定因素。我们发现Tvc受体的IgV域负责与ASLV(C)的糖蛋白相互作用。额外的实验表明,一个域必须作为IgV域和跨膜域之间的间隔物,以实现有效的Tvc受体活性,最有可能使IgV域与细胞膜保持适当的距离。还通过定点诱变Tvc的半胱氨酸残基以及与其他IgV域相比的IgV Tvc域的保守氨基酸残基,研究了对ASLV(C)糖蛋白结合和感染效率的影响。在对与ASLV(C)糖蛋白相互作用重要的Tvc决定簇的这一初步分析中,Tvc的IgV域中至少两个芳香氨基酸残基,Trp-48和Tyr-105被确定为有效感染ASLV(C)的关键。有趣的是,一个或多个芳香族氨基酸残基已被确定为其他ASLV(A-E)受体与ASLV糖蛋白正确相互作用的关键决定因素。这表明ASLV糖蛋白可能与受体上的芳香族残基具有共同的受体相互作用机制,这对于触发SU中构象变化至关重要,而SU构象变化将启动有效病毒感染所需的融合过程。

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