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Entry inhibition of HSV-1 and-2 protects mice from viral lethal challenge

机译:HSV-1和-2的进入抑制保护小鼠免受病毒致死的攻击

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The present study focused on inhibition of HSV-1 and -2 replication and pathogenesis in vitro and in vivo, through the selective targeting of the envelope glycoprotein D. Firstly, a human monoclonal antibody (Hu-mAb#33) was identified that could neutralise both HSV-1 and -2 at nM concentrations, including clinical isolates from patients affected by different clinical manifestations and featuring different susceptibility to acyclovir in vitro. Secondly, the potency of inhibition of both infection by cell-free viruses and cell-to-cell virus transmission was also assessed. Finally, mice receiving a single systemic injection of Hu-mAb#33 were protected from death and severe clinical manifestations following both ocular and vaginal HSV-1 and -2 lethal challenge. These results pave the way for further studies reassessing the importance of HSV entry as a novel target for therapeutic intervention and inhibition of cell-to-cell virus transmission. (C) 2017 Elsevier B.V. All rights reserved.
机译:本研究专注于在体外抑制HSV-1和-2复制和发病机制,通过包膜糖蛋白D的选择性靶向,鉴定了可以中和的人单克隆抗体(HU-MAB#33) HSV-1和-2在NM浓度下,包括来自不同临床表现影响的患者的临床分离物,并在体外具有不同的敏感性易感性。 其次,还评估了无细胞病毒和细胞对细胞病毒透射感染的抑制效力。 最后,接受单一全身注射HU-MAB#33的小鼠免受眼部和阴道HSV-1和-2致命攻击后的死亡和严重的临床表现。 这些结果为进一步研究提供了重新评估HSV进入作为治疗干预的新靶点的进一步研究的方法和对细胞对细胞病毒传播的新靶点。 (c)2017 Elsevier B.v.保留所有权利。

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