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六甲烯阿米洛利可阻断E蛋白离子通道并抑制冠状病毒复制。

Hexamethylene amiloride blocks E protein ion channels and inhibits coronavirus replication.

作者信息

Wilson Lauren, Gage Peter, Ewart Gary

机构信息

ANU Medical School, Pathology Building 10, 6th floor, The Canberra Hospital, Woden ACT 2606, Australia.

出版信息

Virology. 2006 Sep 30;353(2):294-306. doi: 10.1016/j.virol.2006.05.028. Epub 2006 Jul 3.

Abstract

All coronaviruses encode a small hydrophobic envelope (E) protein, which mediates viral assembly and morphogenesis by an unknown mechanism. We have previously shown that the E protein from Severe Acute Respiratory Syndrome coronavirus (SARS-CoV) forms cation-selective ion channels in planar lipid bilayers (Wilson, L., McKinlay, C., Gage, P., Ewart, G., 2004. SARS coronavirus E protein forms cation-selective ion channels. Virology 330(1), 322-331). We now report that three other E proteins also form cation-selective ion channels. These E proteins were from coronaviruses representative of taxonomic groups 1-3: human coronavirus 229E (HCoV-229E), mouse hepatitis virus (MHV), and infectious bronchitis virus (IBV), respectively. It appears, therefore, that coronavirus E proteins in general, belong to the virus ion channels family. Hexamethylene amiloride (HMA)--an inhibitor of the HIV-1 Vpu virus ion channel--inhibited the HCoV-229E and MHV E protein ion channel conductance in bilayers and also inhibited replication of the parent coronaviruses in cultured cells, as determined by plaque assay. Conversely, HMA had no antiviral effect on a recombinant MHV with the entire coding region of E protein deleted (MHVDeltaE). Taken together, the data provide evidence of a link between inhibition of E protein ion channel activity and the antiviral activity of HMA.

摘要

所有冠状病毒都编码一种小的疏水包膜(E)蛋白,该蛋白通过未知机制介导病毒组装和形态发生。我们之前已经表明,严重急性呼吸综合征冠状病毒(SARS-CoV)的E蛋白在平面脂质双层中形成阳离子选择性离子通道(Wilson, L., McKinlay, C., Gage, P., Ewart, G., 2004. SARS冠状病毒E蛋白形成阳离子选择性离子通道。病毒学330(1), 322 - 331)。我们现在报告,其他三种E蛋白也形成阳离子选择性离子通道。这些E蛋白分别来自分类学1 - 3组的代表性冠状病毒:人冠状病毒229E(HCoV - 229E)、小鼠肝炎病毒(MHV)和传染性支气管炎病毒(IBV)。因此,似乎冠状病毒E蛋白总体上属于病毒离子通道家族。六亚甲基amiloride(HMA)——一种HIV - 1 Vpu病毒离子通道的抑制剂——抑制了双层中HCoV - 229E和MHV E蛋白离子通道的电导,并且通过空斑试验确定,它还抑制了亲本冠状病毒在培养细胞中的复制。相反,HMA对缺失E蛋白整个编码区的重组MHV(MHVDeltaE)没有抗病毒作用。综合来看,这些数据提供了E蛋白离子通道活性抑制与HMA抗病毒活性之间存在联系的证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a4ff/7111787/d51dec154fd7/gr1.jpg

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