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病毒基因组 DNA 包装机制。

Viral Genomic DNA Packaging Machinery.

机构信息

York Structural Biology Laboratory, Department of Chemistry, University of York, York, UK.

Structural Biology, The Francis Crick Institute, London, UK.

出版信息

Subcell Biochem. 2024;104:181-205. doi: 10.1007/978-3-031-58843-3_9.

Abstract

Tailed double-stranded DNA bacteriophage employs a protein terminase motor to package their genome into a preformed protein shell-a system shared with eukaryotic dsDNA viruses such as herpesviruses. DNA packaging motor proteins represent excellent targets for antiviral therapy, with Letermovir, which binds Cytomegalovirus terminase, already licensed as an effective prophylaxis. In the realm of bacterial viruses, these DNA packaging motors comprise three protein constituents: the portal protein, small terminase and large terminase. The portal protein guards the passage of DNA into the preformed protein shell and acts as a protein interaction hub throughout viral assembly. Small terminase recognises the viral DNA and recruits large terminase, which in turn pumps DNA in an ATP-dependent manner. Large terminase also cleaves DNA at the termination of packaging. Multiple high-resolution structures of each component have been resolved for different phages, but it is only more recently that the field has moved towards cryo-EM reconstructions of protein complexes. In conjunction with highly informative single-particle studies of packaging kinetics, these structures have begun to inspire models for the packaging process and its place among other DNA machines.

摘要

有尾的双链 DNA 噬菌体利用一种蛋白终止酶马达将其基因组包装到预先形成的蛋白壳中——这种系统与疱疹病毒等真核双链 DNA 病毒共享。DNA 包装马达蛋白是抗病毒治疗的极佳靶点,已获许可的西多福韦可结合巨细胞病毒终止酶,是一种有效的预防药物。在细菌病毒领域,这些 DNA 包装马达由三种蛋白成分组成:门户蛋白、小终止酶和大终止酶。门户蛋白守护 DNA 进入预先形成的蛋白壳的通道,并在病毒组装过程中充当蛋白相互作用的枢纽。小终止酶识别病毒 DNA 并招募大终止酶,后者继而以 ATP 依赖的方式泵送 DNA。大终止酶也在包装结束时切割 DNA。不同噬菌体的每个成分的多个高分辨率结构已被解析,但直到最近,该领域才开始转向蛋白复合物的冷冻电镜重建。结合包装动力学的高信息量单颗粒研究,这些结构开始为包装过程及其在其他 DNA 机器中的位置提供模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5e04/7617512/2350c1808610/EMS203891-f001.jpg

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