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抗囊膜蛋白抑制剂对传染性支气管炎病毒(IBV)台湾分离株的抗病毒作用。

Antiviral effect of the viroporin inhibitors against Taiwan isolates of infectious bronchitis virus (IBV).

机构信息

Department of Veterinary Medicine, College of Veterinary Medicine, National Chung Hsing University, 145 Xingda Road, Taichung 402, Taiwan.

Institute of Genomics and Bioinformatics and Department of Life Sciences, College of Life Science, National Chung Hsing University, 145 Xingda Road, Taichung 402, Taiwan.

出版信息

Virus Res. 2024 Nov;349:199458. doi: 10.1016/j.virusres.2024.199458. Epub 2024 Aug 27.

Abstract

Coronaviruses (CoVs) are significant animal and human pathogens, characterized by being enveloped RNA viruses with positive-sense single-stranded RNA. The Coronaviridae family encompasses four genera, among which gammacoronaviruses pose a major threat to the poultry industry, which infectious bronchitis virus (IBV) being the most prominent of these threats. Particularly, IBV adversely affects broiler growth and egg production, causing substantial losses. The IBV strains currently circulating in Taiwan include the IBV Taiwan-I (TW-I) serotype, IBV Taiwan-II (TW-II) serotype, and vaccine strains. Therefore, ongoing efforts have focused on developing novel vaccines and discovering antiviral agents. The envelope (E) proteins of CoVs accumulate in the endoplasmic reticulum-Golgi intermediate compartment prior to virus budding. These E proteins assemble into viroporins, exhibiting ion channel activity that leads to cell membrane disruption, making them attractive targets for antiviral therapy. In this study, we investigated the E proteins of IBV H-120, as well as IBV serotypes TW-I and TW-II. E protein expression resulted in inhibited bacteria growth, increased permeability of bacteria to β-galactosidase substrates, and blocked protein synthesis of bacteria by hygromycin B (HygB). Furthermore, in the presence of E proteins, HygB also impeded protein translation in DF-1 cells and damaged their membrane integrity. Collectively, these findings confirm the viroporin activity of the E proteins from IBV H-120, IBV serotype TW-I, and IBV serotype TW-II. Next, the viroporin inhibitors, 5-(N,N-hexamethylene) amiloride (HMA) and 4,4'-diisothiocyano stilbene-2,2'-disulphonic acid (DIDS) were used to inhibit the viroporin activities of the E proteins of IBV H-120, IBV serotype TW-I, and IBV serotype TW-II. In chicken embryos and chickens infected with IBV serotypes TW-I and IBV TW-II, no survivors were observed at 6 and 11 days post-infection (dpi), respectively. However, treatments with both DIDS and HMA increased the survival rates in infected chicken embryos and chickens and mitigated histopathological lesions in the trachea and kidney. Additionally, a 3D pentameric structure of the IBV E protein was constructed via homology modeling. As expected, both inhibitors were found to bind to the lipid-facing surface within the transmembrane domain of the E protein, inhibiting ion conduction. Taken together, our findings provide comprehensive evidence supporting the use of viroporin inhibitors as promising antiviral agents against IBV Taiwan isolates.

摘要

冠状病毒(CoVs)是重要的动物和人类病原体,其特征是具有包膜的 RNA 病毒,带有正链单链 RNA。冠状病毒科包含四个属,其中γ冠状病毒对家禽业构成重大威胁,传染性支气管炎病毒(IBV)是这些威胁中最突出的一种。特别是,IBV 会对肉鸡的生长和产蛋产生不利影响,导致大量损失。目前在台湾流行的 IBV 株包括 IBV 台湾-I(TW-I)血清型、IBV 台湾-II(TW-II)血清型和疫苗株。因此,目前的研究重点是开发新型疫苗和发现抗病毒药物。CoV 的包膜(E)蛋白在病毒出芽前积累在内质网-高尔基体中间区室中。这些 E 蛋白组装成病毒孔蛋白,表现出离子通道活性,导致细胞膜破裂,使它们成为抗病毒治疗的有吸引力的靶标。在这项研究中,我们研究了 IBV H-120 的 E 蛋白以及 IBV 血清型 TW-I 和 TW-II 的 E 蛋白。E 蛋白的表达导致细菌生长受到抑制、细菌对β-半乳糖苷酶底物的通透性增加以及 HygB(潮霉素 B)阻断细菌的蛋白质合成。此外,在存在 E 蛋白的情况下,HygB 还会阻碍 DF-1 细胞中的蛋白质翻译并破坏其膜完整性。总之,这些发现证实了来自 IBV H-120、IBV 血清型 TW-I 和 IBV 血清型 TW-II 的 E 蛋白的病毒孔蛋白活性。接下来,使用病毒孔抑制剂 5-(N,N-六亚甲基)氨茴酰胺(HMA)和 4,4'-二异硫氰基二苯乙烯-2,2'-二磺酸(DIDS)抑制 IBV H-120、IBV 血清型 TW-I 和 IBV 血清型 TW-II 的 E 蛋白的病毒孔蛋白活性。在感染 IBV 血清型 TW-I 和 IBV TW-II 的鸡胚和鸡中,分别在感染后 6 天和 11 天未观察到存活者。然而,用 DIDS 和 HMA 处理感染的鸡胚和鸡可以提高存活率并减轻气管和肾脏的组织病理学损伤。此外,通过同源建模构建了 IBV E 蛋白的 3D 五聚体结构。不出所料,两种抑制剂都被发现结合在 E 蛋白跨膜结构域的脂质面向表面上,抑制离子传导。总之,我们的研究结果提供了全面的证据支持将病毒孔抑制剂用作针对台湾 IBV 分离株的有前途的抗病毒药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/13b8/11399653/f244a077a34b/gr1.jpg

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