Himisha Dixit, Vipin Upadhyay, Mahesh Kulharia and Shailender Kumar Verma*,
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引用次数: 0
摘要
金属蛋白是多种生物过程的基础,但在病毒环境中仍缺乏广泛的研究。这项研究揭示了 DNA 病毒中金属结合蛋白的普遍性和功能多样性。在 1432 个金属蛋白子集中,锌和镁结合蛋白的数量明显较多,这表明了它们在病毒生物学中的重要性。此外,还检测到大量与铁、锰、铜、镍、汞和镉结合的蛋白质。人类感染病毒的蛋白质显示出丰富的金属蛋白,其中以 MeBiPred(964 个蛋白质)和 Pfam(666 个蛋白质)的数量最多。有趣的是,许多重要的病毒蛋白都具有金属结合能力,包括聚合酶、DNA 结合蛋白、螺旋酶、dUPT 酶、胸腺嘧啶激酶以及各种结构蛋白和附属蛋白。这项研究揭示了金属蛋白的普遍存在、其功能特征、亚细胞位置和金属利用模式,为病毒生物学提供了宝贵的见解。在各种 DNA 病毒的类似功能蛋白中观察到了类似的金属利用模式。此外,这些发现为确定抗病毒感染的潜在药物靶点奠定了基础。
The Study of Metalloproteome of DNA Viruses: Identification, Functional Annotation, and Diversity Analysis of Viral Metal-Binding Proteins
Metalloproteins are fundamental to diverse biological processes but still lack extensive investigation in viral contexts. This study reveals the prevalence and functional diversity of metal-binding proteins in DNA viruses. Among a subset of 1432 metalloproteins, zinc and magnesium-binding proteins are notably abundant, indicating their importance in viral biology. Furthermore, significant numbers of proteins binding to iron, manganese, copper, nickel, mercury, and cadmium were also detected. Human-infecting viral proteins displayed a rich landscape of metalloproteins, with MeBiPred (964 proteins) and Pfam (666) yielding the highest numbers. Interestingly, many essential viral proteins exhibited metal-binding capabilities, including polymerases, DNA binding proteins, helicases, dUPTase, thymidine kinase, and various structural and accessory proteins. This study sheds light on the ubiquitous presence of metalloproteins, their functional signatures, subcellular placements, and metal-utilization patterns, providing valuable insights into viral biology. A similar metal utilization pattern was observed in similar functional proteins across the various DNA viruses. Furthermore, these findings provide a foundation for identifying potential drug targets for combating viral infections.