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传染性支气管炎病毒 S2 亚基影响 Abl2 介导的合胞体形成。

The S2 Subunit of Infectious Bronchitis Virus Affects Abl2-Mediated Syncytium Formation.

机构信息

College of Veterinary Medicine, Sichuan Agricultural University, Huimin Road, Wenjiang, Chengdu 611130, China.

出版信息

Viruses. 2023 May 25;15(6):1246. doi: 10.3390/v15061246.

Abstract

The S2 subunit serves a crucial role in infectious bronchitis virus (IBV) infection, particularly in facilitating membrane fusion. Using reverse genetic techniques, mutant strains of the S2 locus exhibited substantially different syncytium-forming abilities in chick embryonic kidney cells. To determine the precise formation mechanism of syncytium, we demonstrated the co-ordinated role of Abl2 and its mediated cytoskeletal regulatory pathway within the S2 subunit. Using a combination of fluorescence quantification, RNA silencing, and protein profiling techniques, the functional role of S2 subunits in IBV-infected cells was exhaustively determined. Our findings imply that Abl2 is not the primary cytoskeletal regulator, the viral S2 component is involved in indirect regulation, and the three different viral strains activate various cytoskeletal regulatory pathways through Abl2. CRK, CRKL, ABI1, NCKAP1, and ENAH also play a role in cytoskeleton regulation. Our research provides a point of reference for the development of an intracellular regulatory network for the S2 subunit and a foundation for the rational design of antiviral drug targets against Abl2.

摘要

S2 亚基在传染性支气管炎病毒(IBV)感染中起着至关重要的作用,特别是在促进膜融合方面。使用反向遗传技术,S2 基因座的突变株在鸡胚肾细胞中表现出明显不同的合胞体形成能力。为了确定合胞体的确切形成机制,我们证明了 Abl2 的协调作用及其在 S2 亚基中的介导细胞骨架调节途径。通过荧光定量、RNA 沉默和蛋白质谱技术的组合,我们详尽地确定了 S2 亚基在 IBV 感染细胞中的功能作用。我们的研究结果表明,Abl2 不是主要的细胞骨架调节剂,病毒 S2 成分参与间接调节,三种不同的病毒株通过 Abl2 激活各种细胞骨架调节途径。CRK、CRKL、ABI1、NCKAP1 和 ENAH 也在细胞骨架调节中发挥作用。我们的研究为 S2 亚基的细胞内调节网络的发展提供了参考,并为针对 Abl2 的抗病毒药物靶点的合理设计奠定了基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b0a4/10301418/f6b70d05c7ce/viruses-15-01246-g001.jpg

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