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Human cytomegalovirus encodes a highly specific RANTES decoy receptor.

机译:人类巨细胞病毒编码高度特异性的RANTES诱饵受体。

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摘要

The human cytomegalovirus pUL21.5 protein is a small, secreted glycoprotein whose mRNA is packaged into virions. We demonstrate that pUL21.5 protein is a soluble CC chemokine receptor that functions as a decoy to modulate the host immune response to infection. In contrast to other viral chemokine-binding proteins, which interact promiscuously with multiple chemokines, pUL21.5 selectively binds RANTES (regulated upon activation, normal T cell expressed and secreted) with high affinity. By binding RANTES, pUL21.5 blocks RANTES interaction with its cellular receptors. We propose that human cytomegalovirus directs the synthesis of a secreted, virus-coded protein that modulates the host antiviral response even before the newly infecting viral genome becomes transcriptionally active.
机译:人巨细胞病毒pUL21.5蛋白是一种分泌的小糖蛋白,其mRNA包装在病毒体中。我们证明,pUL21.5蛋白是一种可溶性CC趋化因子受体,可作为诱饵来调节宿主对感染的免疫反应。与其他病毒趋化因子结合蛋白(与多种趋化因子混杂地相互作用)相反,pUL21.5以高亲和力选择性结合RANTES(受激活后调节,正常T细胞表达和分泌)。通过结合RANTES,pUL21.5阻断了RANTES与其细胞受体的相互作用。我们建议人巨细胞病毒指导分泌的,病毒编码的蛋白质的合成,甚至在新感染的病毒基因组变得有转录活性之前,该蛋白质就能调节宿主的抗病毒反应。

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