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并且其成分能够抑制甲型流感病毒诱导的自噬和复制。

and its Components Inhibit Influenza A Virus-Induced Autophagy and Replication.

机构信息

Korean Medicine (KM) Application Center, Korea Institute of Oriental Medicine (KIOM), Dong-gu, Daegu 701-300, Republic of Korea.

出版信息

Am J Chin Med. 2019;47(6):1307-1324. doi: 10.1142/S0192415X19500678. Epub 2019 Sep 10.

Abstract

ethanol extract (AVE) reportedly has significant anti-influenza virus activity, but its underlying mechanisms of action and constituents have not yet been completely elucidated. Previously, we have confirmed that AVE treatment significantly reduces the viral replication of green fluorescent protein-labeled influenza A virus in Madin-Darby canine kidney (MDCK) cells. In addition, post-treatment with AVE inhibited viral matrix protein 1 (M1), matrix protein 2 (M2), and hemagglutinin (HA) mRNA synthesis and viral protein (M1, M2, and HA) expressions. In this study, we demonstrated that AVE inhibited autophagy induced by influenza A virus in MDCK cells and also identified quercetin, catechin hydrate, and kaempferol as the active antiviral components of AVE. We also found that post-treatment with quercetin, catechin hydrate, and kaempferol markedly inhibited M2 viral mRNA synthesis and M2 protein expression. A docking simulation suggested that the binding affinity of quercetin, catechin hydrate, and kaempferol for the M2 protein may be higher than that of known M2 protein inhibitors. Thus, the inhibition of autophagy induced by influenza virus may explain the antiviral activity of AVE against H1N1 or H3N2. extract and its constituents may, therefore, be potentially useful for the development of anti-influenza agents.

摘要

乙醇提取物(AVE)据称具有显著的抗流感病毒活性,但作用机制和成分尚未完全阐明。此前,我们已证实 AVE 处理可显著减少绿色荧光蛋白标记的流感 A 病毒在 Madin-Darby 犬肾(MDCK)细胞中的复制。此外,AVE 的后期处理抑制了病毒基质蛋白 1(M1)、基质蛋白 2(M2)和血凝素(HA)mRNA 的合成以及病毒蛋白(M1、M2 和 HA)的表达。在这项研究中,我们证明了 AVE 抑制了 MDCK 细胞中流感 A 病毒诱导的自噬,还确定了槲皮素、儿茶素和山奈酚是 AVE 的抗病毒活性成分。我们还发现,槲皮素、儿茶素和山奈酚的后期处理显著抑制了 M2 病毒 mRNA 的合成和 M2 蛋白的表达。对接模拟表明,槲皮素、儿茶素和山奈酚与 M2 蛋白的结合亲和力可能高于已知的 M2 蛋白抑制剂。因此,流感病毒诱导的自噬抑制可能解释了 AVE 对 H1N1 或 H3N2 的抗病毒活性。因此,AVE 及其成分可能对开发抗流感药物具有潜在用途。

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