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Strategies for development of dengue virus inhibitors.

机译:登革热病毒抑制剂开发策略。

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Antiviral drug discovery is becoming increasingly important due to the global threat of viral disease pandemics. Many members of the genus Flavivirus are significant human pathogens, among which dengue virus (DENV) alone poses a public health threat to 2.5 billion worldwide, leading to 50-100 million human infections each year. Neither vaccine nor effective therapeutics is currently available for DENV. Development of a DENV vaccine has been challenging, because of the need to simultaneously immunize and induce a long-lasting protection against all four serotypes of DENV; an incompletely immunized individual may be sensitized to life-threatening dengue hemorrhagic fever or dengue shock syndrome. The challenges associated with vaccine development have underscored the importance of development of antiviral therapies for DENV and other flaviviruses. Here we review the strategies to identify inhibitors for DENV therapy. Both viral and host proteins essential for viral replication cycle are potential targets for antiviral development. Inhibitors could be identified by multiple approaches, including enzyme-based screening, viral replication-based screening, structure-based rational design, virtual screening, and fragment-based screening. The strategies discussed in this report should be applicable to antiviral development of other viruses.
机译:由于病毒性疾病大流行的全球威胁,抗病毒药物的发现变得越来越重要。黄病毒属的许多成员都是重要的人类病原体,其中登革病毒(DENV)单独对全球25亿人构成公共健康威胁,每年导致50-100百万人感染。目前,DENV既没有疫苗也没有有效的治疗方法。 DENV疫苗的开发一直具有挑战性,因为需要同时免疫和诱导针对所有四种血清型的DENV;未完全免疫的个体可能对威胁生命的登革热出血热或登革热休克综合征敏感。与疫苗开发相关的挑战强调了开发针对DENV和其他黄病毒的抗病毒治疗的重要性。在这里,我们回顾确定DENV治疗抑制剂的策略。病毒复制周期必不可少的病毒和宿主蛋白都是抗病毒发展的潜在目标。抑制剂可以通过多种方法进行鉴定,包括基于酶的筛选,基于病毒复制的筛选,基于结构的合理设计,虚拟筛选和基于片段的筛选。本报告中讨论的策略应适用于其他病毒的抗病毒开发。

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