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Filovirus proteins for antiviral drug discovery: Structure/function bases of the replication cycle

机译:用于抗病毒药物发现的泌尿病毒蛋白:复制周期的结构/功能基础

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Filoviruses are important pathogens that cause severe and often fatal hemorrhagic fever in humans, for which no approved vaccines and antiviral treatments are yet available. In an earlier article (Martin et al., Antiviral Research, 2016), we reviewed the role of the filovirus surface glycoprotein in replication and as a target for drugs and vaccines. In this review, we focus on recent findings on the filovirus replication machinery and how they could be used for the identification of new therapeutic targets and the development of new antiviral compounds. First, we summarize the recent structural and functional advances on the molecules involved in filovirus replication/transcription cycle, particularly the NP, VP30, VP35 proteins, and the "large" protein L, which harbors the RNA-dependent RNA polymerase (RdRp) and mRNA capping activities. These proteins are essential for viral mRNA synthesis and genome replication, and consequently they constitute attractive targets for drug design. We then describe how these insights into filovirus replication mechanisms and the structure function characterization of the involved proteins have led to the development of new and innovative antiviral strategies that may help reduce the filovirus disease case fatality rate through post-exposure or prophylactic treatments. (C) 2017 Elsevier B.V. All rights reserved.
机译:泌尿病毒是一种重要病原体,导致人类严重且往往致命的出血热,其尚未获得批准的疫苗和抗病毒治疗。在早先的文章中(Martin等,抗病毒研究,2016),我们审查了脲病毒表面糖蛋白在复制中的作用以及药物和疫苗的靶标。在这篇综述中,我们专注于最近关于菲病毒复制机制的结果以及它们如何用于识别新的治疗目标和新的抗病毒化合物的发展。首先,我们总结了近期涉及泌尿病毒复制/转录循环的分子的结构和功能进展,特别是NP,VP30,VP35蛋白和“大”蛋白L,其遗传RNA依赖性RNA聚合酶(RDRP)和mRNA封盖活动。这些蛋白质对于病毒mRNA合成和基因组复制至关重要,因此它们构成了药物设计的有吸引力的目标。然后,我们描述了如何对杂志复制机制的洞察力以及所涉及的蛋白质的结构功能导致了新的和创新的抗病毒策略的发展,这可能通过暴露后或预防性治疗来减少泌尿病毒病变病变率。 (c)2017 Elsevier B.v.保留所有权利。

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