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Potent single-domain antibodies that arrest respiratory syncytial virus fusion protein in its prefusion state

机译:有效的单域抗体,可在其融合前状态下阻止呼吸道合胞病毒融合蛋白

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摘要

Human respiratory syncytial virus (RSV) is the main cause of lower respiratory tract infections in young children. The RSV fusion protein (F) is highly conserved and is the only viral membrane protein that is essential for infection. The prefusion conformation of RSV F is considered the most relevant target for antiviral strategies because it is the fusion-competent form of the protein and the primary target of neutralizing activity present in human serum. Here, we describe two llama-derived single-domain antibodies (VHHs) that have potent RSV-neutralizing activity and bind selectively to prefusion RSV F with picomolar affinity. Crystal structures of these VHHs in complex with prefusion F show that they recognize a conserved cavity formed by two F protomers. In addition, the VHHs prevent RSV replication and lung infiltration of inflammatory monocytes and T cells in RSV-challenged mice. These prefusion F-specific VHHs represent promising antiviral agents against RSV.
机译:人呼吸道合胞病毒(RSV)是幼儿下呼吸道感染的主要原因。 RSV融合蛋白(F)高度保守,是唯一对感染至关重要的病毒膜蛋白。 RSV F的融合前构象被认为是抗病毒策略中最相关的靶标,因为它是蛋白质的融合形式,并且是人血清中存在的中和活性的主要靶标。在这里,我们描述了两种来自美洲驼的单域抗体(VHH),它们具有强大的RSV中和活性,并以皮摩尔亲和力选择性结合预融合RSVF。这些VHHs与预融合F形成复合物的晶体结构表明,它们可以识别由两个F孕激素形成的保守腔。此外,VHH可防止RSV复制小鼠中的RSV复制以及炎性单核细胞和T细胞的肺浸润。这些融合前F特异性VHH代表了有希望的针对RSV的抗病毒药物。

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