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Integrin αvβ1 Promotes Infection By Human Metapneumovirus

机译:整合素αvβ1促进人间质肺病毒感染。

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Human metapneumovirus (hMPV) is a recently described paramyxo-virus that causes lower respiratory infections in children and adults worldwide. The hMPV fusion (F) protein is a membrane-anchored glycoprotein and major protective antigen. All hMPV F protein sequences determined to date contain an Arg-Gly-Asp (RGD) sequence, suggesting that F engages RGD-binding integrins to mediate cell entry. The divalent cation chelator EDTA, which disrupts het-erodimeric integrin interactions, inhibits infectivity of hMPV but not the closely related respiratory syncytial virus (RSV), which lacks an RGD motif. Function-blocking antibodies specific for αvβ1 integrin inhibit infectivity of hMPV but not RSV. Transfection of nonpermissive cells with αv or β1 cDNAs confers hMPV infectivity, whereas reduction of αv and β1 integrin expression by siRNA inhibits hMPV infection. Recombinant hMPV F protein binds to cells, whereas Arg-Gly-Glu (RGE)-mutant F protein does not. These data suggest that αvβ1 integrin is a functional receptor for hMPV.
机译:人类间质肺病毒(hMPV)是最近描述的副粘病毒,可引起全球儿童和成人的下呼吸道感染。 hMPV融合蛋白是膜锚定的糖蛋白和主要的保护性抗原。迄今为止确定的所有hMPV F蛋白序列均包含一个Arg-Gly-Asp(RGD)序列,表明F参与RGD结合整联蛋白介导细胞进入。二价阳离子螯合剂EDTA破坏了异二聚体整联蛋白的相互作用,抑制了hMPV的感染性,但抑制了缺乏RGD母题的密切相关的呼吸道合胞病毒(RSV)。对αvβ1整联蛋白具有特异性的功能阻断抗体可抑制hMPV的感染性,但不能抑制RSV。用αv或β1cDNA转染非许可细胞可赋予hMPV感染性,而通过siRNA降低αv和β1整联蛋白表达可抑制hMPV感染。重组hMPV F蛋白与细胞结合,而Arg-Gly-Glu(RGE)突变F蛋白不结合。这些数据表明αvβ1整联蛋白是hMPV的功能性受体。

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