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N-丁基脱氧野尻霉素对牛病毒性腹泻病毒的抗病毒作用与E2包膜蛋白的错误折叠及其形成E1-E2异二聚体的能力受损有关。

Antiviral effect of N-butyldeoxynojirimycin against bovine viral diarrhea virus correlates with misfolding of E2 envelope proteins and impairment of their association into E1-E2 heterodimers.

作者信息

Branza-Nichita N, Durantel D, Carrouée-Durantel S, Dwek R A, Zitzmann N

机构信息

Oxford Glycobiology Institute, Department of Biochemistry, University of Oxford, Oxford OX1 3QU, United Kingdom.

出版信息

J Virol. 2001 Apr;75(8):3527-36. doi: 10.1128/JVI.75.8.3527-3536.2001.

Abstract

The iminosugar N-butyldeoxynojirimycin (NB-DNJ), an endoplasmic reticulum alpha-glucosidase inhibitor, has an antiviral effect against bovine viral diarrhea virus (BVDV). In this report, we investigate the molecular mechanism of this inhibition by studying the folding pathway of BVDV envelope glycoproteins in the presence and absence of NB-DNJ. Our results show that, while the disulfide-dependent folding of E2 glycoprotein occurs rapidly (2.5 min), the folding of E1 occurs slowly (30 min). Both BVDV envelope glycoproteins associate rapidly with calnexin and dissociate with different kinetics. The release of E1 from the interaction with calnexin coincides with the beginning of E1 and E2 association into disulfide-linked heterodimers. In the presence of NB-DNJ, the interaction of E1 and E2 with calnexin is prevented, leading to misfolding of the envelope glycoproteins and inefficient formation of E1-E2 heterodimers. The degree of misfolding and the lack of association of E1 and E2 into disulfide-linked complexes in the presence of NB-DNJ correlate with the dose-dependent antiviral effect observed for this iminosugar.

摘要

亚氨基糖N-丁基脱氧野尻霉素(NB-DNJ)是一种内质网α-葡萄糖苷酶抑制剂,对牛病毒性腹泻病毒(BVDV)具有抗病毒作用。在本报告中,我们通过研究在有和没有NB-DNJ的情况下BVDV包膜糖蛋白的折叠途径,来探究这种抑制作用的分子机制。我们的结果表明,虽然E2糖蛋白依赖二硫键的折叠迅速发生(2.5分钟),但E1的折叠则较为缓慢(30分钟)。两种BVDV包膜糖蛋白都能迅速与钙连蛋白结合,并以不同的动力学解离。E1从与钙连蛋白的相互作用中释放出来,与E1和E2缔合成二硫键连接的异二聚体的开始时间一致。在NB-DNJ存在的情况下,E1和E2与钙连蛋白的相互作用受到阻碍,导致包膜糖蛋白错误折叠,E1-E2异二聚体的形成效率低下。在NB-DNJ存在的情况下,错误折叠的程度以及E1和E2无法缔合成二硫键连接的复合物,与该亚氨基糖所观察到的剂量依赖性抗病毒作用相关。

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