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腺病毒DNA结合蛋白DBP。

The adenovirus DNA-binding protein DBP.

作者信息

Bertzbach Luca D, Seddar Laura, von Stromberg Konstantin, Ip Wing-Hang, Dobner Thomas, Hidalgo Paloma

机构信息

Department of Viral Transformation, Leibniz Institute of Virology (LIV), Hamburg, Germany.

出版信息

J Virol. 2024 Feb 20;98(2):e0188523. doi: 10.1128/jvi.01885-23. Epub 2024 Jan 10.

Abstract

Adenoviruses are a group of double-stranded DNA viruses that can mainly cause respiratory, gastrointestinal, and eye infections in humans. In addition, adenoviruses are employed as vector vaccines for combatting viral infections, including SARS-CoV-2, and serve as excellent gene therapy vectors. These viruses have the ability to modulate the host cell machinery to their advantage and trigger significant restructuring of the nuclei of infected cells through the activity of viral proteins. One of those, the adenovirus DNA-binding protein (DBP), is a multifunctional non-structural protein that is integral to the reorganization processes. DBP is encoded in the E2A transcriptional unit and is highly abundant in infected cells. Its activity is unequivocally linked to the formation, structure, and integrity of virus-induced replication compartments, molecular hubs for the regulation of viral processes, and control of the infected cell. DBP also plays key roles in viral DNA replication, transcription, viral gene expression, and even host range specificity. Notably, post-translational modifications of DBP, such as SUMOylation and extensive phosphorylation, regulate its biological functions. DBP was first investigated in the 1970s, pioneering research on viral DNA-binding proteins. In this literature review, we provide an overview of DBP and specifically summarize key findings related to its complex structure, diverse functions, and significant role in the context of viral replication. Finally, we address novel insights and perspectives for future research.

摘要

腺病毒是一类双链DNA病毒,主要可引起人类呼吸道、胃肠道和眼部感染。此外,腺病毒被用作对抗包括SARS-CoV-2在内的病毒感染的载体疫苗,并作为优秀的基因治疗载体。这些病毒有能力将宿主细胞机制调节至对其有利的状态,并通过病毒蛋白的活性触发受感染细胞核的显著重组。其中之一,腺病毒DNA结合蛋白(DBP),是一种多功能非结构蛋白,对重组过程至关重要。DBP由E2A转录单元编码,在受感染细胞中高度丰富。其活性与病毒诱导的复制区室的形成、结构和完整性明确相关,复制区室是调节病毒过程和控制受感染细胞的分子中心。DBP在病毒DNA复制、转录、病毒基因表达甚至宿主范围特异性方面也发挥着关键作用。值得注意的是,DBP的翻译后修饰,如SUMO化和广泛的磷酸化,调节其生物学功能。DBP最早在20世纪70年代被研究,开创了病毒DNA结合蛋白的研究先河。在这篇文献综述中,我们概述了DBP,并特别总结了与其复杂结构、多样功能以及在病毒复制背景下的重要作用相关的关键发现。最后,我们阐述了未来研究的新见解和观点。

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