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质型多角体病毒整合到多角体基质中。

Integration of Cypoviruses into polyhedrin matrix.

作者信息

Konevtsova Olga V, Golushko Ivan Yu, Podgornik Rudolf, Rochal Sergei B

机构信息

Physics Faculty, Southern Federal University Rostov-on-Don Russia

School of Physical Sciences and Kavli Institute for Theoretical Sciences, University of Chinese Academy of Sciences Beijing 100049 China

出版信息

Nanoscale Adv. 2023 Jul 16;5(16):4140-4148. doi: 10.1039/d3na00393k. eCollection 2023 Aug 8.

Abstract

Unlike in other viruses, in Cypoviruses the genome is doubly protected since their icosahedral capsids are embedded into a perfect polyhedrin crystal. Current experimental methods cannot resolve the resulting interface structure and we propose a symmetry-based approach to predict it. We reveal a remarkable match between the surfaces of Cypovirus and the outer polyhedrin matrix. The match arises due to the preservation of the common tetragonal symmetry, allowing perfect contacts of polyhedrin trimers with VP1 and VP5 capsid proteins. We highlight a crucial role of the VP5 proteins in embedding the Cypovirus into the polyhedrin matrix and discuss the relationship between the nucleoside triphosphatase activity of the proteins and their role in the superstructure formation. Additionally, we propose an electrostatic mechanism that drives the viral superstructure disassembly occurring in the alkaline environment of the insect intestines. Our study may underpin novel strategies for engineering proteinaceous nanocontainers in diverse biotechnological and chemical applications.

摘要

与其他病毒不同,在质型多角体病毒中,其基因组受到双重保护,因为它们的二十面体衣壳嵌入到完美的多角体蛋白晶体中。目前的实验方法无法解析由此产生的界面结构,因此我们提出一种基于对称性的方法来预测它。我们揭示了质型多角体病毒表面与外部多角体蛋白基质之间存在显著匹配。这种匹配是由于共同的四方对称性得以保留,使得多角体蛋白三聚体与衣壳蛋白VP1和VP5能够完美接触。我们强调了VP5蛋白在将质型多角体病毒嵌入多角体蛋白基质中的关键作用,并讨论了这些蛋白的核苷三磷酸酶活性与其在超结构形成中的作用之间的关系。此外,我们提出了一种静电机制,该机制驱动在昆虫肠道碱性环境中发生的病毒超结构解体。我们的研究可能为在各种生物技术和化学应用中设计蛋白质纳米容器提供新策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7aa0/10408579/2b4362c42bec/d3na00393k-f1.jpg

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