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New small-molecule drug design strategies for fighting resistant influenza A

机译:抗甲型流感的新小分子药物设计策略

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摘要

Influenza A virus is the major cause of seasonal or pandemic flu worldwide. Two main treatment strategies–vaccination and small molecule anti-influenza drugs are currently available. As an effective vaccine usually takes at least 6 months to develop, anti-influenza small molecule drugs are more effective for the first line of protection against the virus during an epidemic outbreak, especially in the early stage. Two major classes of anti-influenza drugs currently available are admantane-based M2 protein blockers (amantadine and rimantadine) and neuraminidase (NA) inhibitors (oseltamivir, zanamivir, and peramivir). However, the continuous evolvement of influenza A virus and the rapid emergence of resistance to current drugs, particularly to amantadine, rimantadine, and oseltamivir, have raised an urgent need for developing new anti-influenza drugs against resistant forms of influenza A virus. In this review, we first give a brief introduction of the molecular mechanisms behind resistance, and then discuss new strategies in small-molecule drug development to overcome influenza A virus resistance targeting mutant M2 proteins and neuraminidases, and other viral proteins not associated with current drugs.
机译:甲型流感病毒是全球季节性或大流行性流感的主要原因。目前有两种主要的治疗策略-疫苗接种和小分子抗流感药物。由于一种有效的疫苗通常需要至少6个月的研发时间,因此抗流行性感冒小分子药物在流行病爆发期间(尤其是在早期阶段)对于抵御病毒的第一道防线更为有效。当前可用的两大类抗流感药物是基于金刚烷的M2蛋白阻滞剂(金刚烷胺和金刚乙胺)和神经氨酸酶(NA)抑制剂(oseltamivir,zanamivir和peramivir)。然而,甲型流感病毒的不断发展以及对当前药物,特别是对金刚烷胺,金刚乙胺和奥司他韦的耐药性的迅速出现,迫切需要开发新的抗甲型流感病毒的抗流感药物。在这篇综述中,我们首先简要介绍了抗药性背后的分子机制,然后讨论了小分子药物开发中的新策略,以克服针对突变M2蛋白和神经氨酸酶以及与当前药物无关的其他病毒蛋白的甲型流感病毒抗药性。

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