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马立克氏病病毒糖蛋白 gB 和 gH 的相互作用域及具有双重功能的抗病毒肽的鉴定。

Interaction domain of glycoproteins gB and gH of Marek's disease virus and identification of an antiviral peptide with dual functions.

机构信息

Key Laboratory of Zoonosis of Ministry of Agricultrure, College of Veterinary Medicine, China Agricultural University, Beijing, People's Republic of China.

出版信息

PLoS One. 2013;8(2):e54761. doi: 10.1371/journal.pone.0054761. Epub 2013 Feb 6.

Abstract

Our previous study reported that both glycoproteins gB and gH of the herpesvirus Marek's disease virus (MDV) contain eleven potential heptad repeat domains. These domains overlap with α-helix-enriched hydrophobic regions, including the gH-derived HR1 (gHH1) and HR3 (gHH3) and gB-derived HR1 (gBH1) regions, which demonstrate effective antiviral activity, with 50% inhibitory concentrations (IC(50)) of less than 12 µM. Plaque formation and chicken embryo infection assays confirmed these results. In this study, biochemical and biophysical analyses detected potential interactions between these peptides. gHH1, gHH3, and gBH1 were found to interact with each other in pairs. The complex formed by gHH3 and gBH1 showed the most stable interaction at a molar ratio of 1:3, the binding between gHH1 and gBH1 was relatively weak, and no interaction was observed between the three HR peptides. These results indicate that gHH3 and gBH1 are likely the key contributors to the interaction between gB and gH. Furthermore, each HR peptide from herpesvirus glycoproteins did not effectively inhibit virus infection compared with peptides from a class I enveloped virus. In this report, the HR mimic peptide modified with a double glutamic acid (EE) or a double lysine (KK) at the non-interactive sites (i.e., solvent-accessible sites) did not noticeably affect the antiviral activity compared with the wild-type HR peptide, whereas tandem peptides from gH-derived gHH1 and gB-derived gBH1 (i.e., gBH1-Linker-gHH1) produced efficient antiviral effects, unlike the individual peptides. The proposed interpretation of inhibition of entry has been addressed. Our results support the hypothesis that the interaction domain between glycoproteins gH and gB is a critical target in the design of inhibitors of herpesvirus infection.

摘要

我们之前的研究报告称,疱疹病毒马立克氏病病毒(MDV)的糖蛋白 gB 和 gH 都包含十一个潜在的七肽重复结构域。这些结构域与富含α-螺旋的疏水区重叠,包括 gH 衍生的 HR1(gHH1)和 HR3(gHH3)和 gB 衍生的 HR1(gBH1)区域,这些区域表现出有效的抗病毒活性,半数抑制浓度(IC50)低于 12 µM。空斑形成和鸡胚感染实验证实了这些结果。在这项研究中,生化和生物物理分析检测到这些肽之间存在潜在的相互作用。gHH1、gHH3 和 gBH1 被发现两两相互作用。gHH3 和 gBH1 形成的复合物在摩尔比为 1:3 时表现出最稳定的相互作用,gHH1 和 gBH1 之间的结合较弱,而三个 HR 肽之间没有相互作用。这些结果表明,gHH3 和 gBH1 可能是 gB 和 gH 之间相互作用的关键因素。此外,与 I 型包膜病毒的肽相比,疱疹病毒糖蛋白的每个 HR 肽都不能有效地抑制病毒感染。在本报告中,在非相互作用位点(即溶剂可及位点)用双谷氨酸(EE)或双赖氨酸(KK)修饰的 HR 模拟肽与野生型 HR 肽相比,抗病毒活性没有明显变化,而 gH 衍生的 gHH1 和 gB 衍生的 gBH1 的串联肽(即 gBH1-Linker-gHH1)产生了有效的抗病毒作用,与单个肽不同。已经提出了对进入抑制的解释。我们的结果支持这样的假设,即糖蛋白 gH 和 gB 之间的相互作用域是设计疱疹病毒感染抑制剂的关键靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5358/3566115/7e9f4b690103/pone.0054761.g001.jpg

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