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Identification of a cellular receptor for subgroup E avian leukosis virus

机译:鉴定E型禽白血病病毒亚群的细胞受体

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摘要

Genetic studies in chickens and receptor interference experiments have indicated that avian leukosis virus (ALV)-E may utilize a cellular receptor related to the receptor for ALV-B and ALV-D. Recently, we cloned CAR1, a tumor necrosis factor receptor (TNFR)-related protein, that serves as a cellular receptor for ALV-B and ALV-D. To determine whether the cellular receptor for ALV-E is a CAR1-like protein, a cDNA library was made from turkey embryo fibroblasts (TEFs), which are susceptible to ALV-E infection, but not to infection by ALV-B and ALV-D. The cDNA library was screened with a radioactively labeled CAR1 cDNA probe, and clones that hybridized with the probe were isolated. A 2.3-kb cDNA clone was identified that conferred susceptibility to ALV-E infection, but not to ALV-B infection, when expressed in transfected human 293 cells. The functional cDNA clone is predicted to encode a 368 amino acid protein with significant amino acid similarity to CAR1. Like CAR1, the TEF protein is predicted to have two extracellular TNFR-like cysteine-rich domains and a putative death domain similar to those of TNFR I and Fas. Flow cytometric analysis and immunoprecipitation experiments demonstrated specific binding between the TEF CAR1-related protein and an immunoadhesin composed of the surface (SU) envelope protein of subgroup E (RAV-0) virus fused to the constant region of a rabbit immunoglobulin. These two activities of the TEF CAR1-related protein, specific binding to ALV-E SU and permitting entry only of ALV-E, have unambiguously identified this protein as a cellular receptor specific for subgroup E ALV.
机译:鸡的遗传研究和受体干扰实验表明,禽白血病病毒(ALV)-E可能利用与ALV-B和ALV-D受体相关的细胞受体。最近,我们克隆了CAR1,一种与肿瘤坏死因子受体(TNFR)相关的蛋白,可作为ALV-B和ALV-D的细胞受体。为了确定ALV-E的细胞受体是否为类CAR1蛋白,从火鸡胚胎成纤维细胞(TEFs)制备了cDNA文库,它们易受ALV-E感染,但不受ALV-B和ALV- D.用放射性标记的CAR1 cDNA探针筛选cDNA文库,并分离与探针杂交的克隆。当在转染的人293细胞中表达时,鉴定出2.3kb的cDNA克隆,其赋予ALV-E感染敏感性,但不赋予ALV-B感染敏感性。预测该功能性cDNA克隆编码与CAR1具有显着氨基酸相似性的368个氨基酸的蛋白质。像CAR1一样,预计TEF蛋白具有两个胞外TNFR样富含半胱氨酸的结构域和一个与TNFR I和Fas相似的推定死亡结构域。流式细胞仪分析和免疫沉淀实验表明,TEF CAR1相关蛋白与免疫粘附素之间具有特异性结合,该粘附素由E亚群(RAV-0)病毒的表面(SU)包膜蛋白融合到兔免疫球蛋白的恒定区组成。 TEF CAR1相关蛋白的这两种活性(与ALV-E SU特异性结合并仅允许ALV-E进入)明确地确定了该蛋白为对E ALV亚型特异的细胞受体。

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