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在昆虫细胞中产生的SV40衣壳蛋白之间的自组装和蛋白质-蛋白质相互作用。

Self-assembly and protein-protein interactions between the SV40 capsid proteins produced in insect cells.

作者信息

Sandalon Z, Oppenheim A

机构信息

Department of Hematology, The Hebrew University-Hadassah Medical School, Jerusalem, 91120, Israel.

出版信息

Virology. 1997 Oct 27;237(2):414-21. doi: 10.1006/viro.1997.8796.

Abstract

Soluble SV40 capsid proteins were obtained by expression of the three late genes, VP1, VP2, and VP3, in Sf9 cells using baculovirus expression vectors. Coproduction of the capsid proteins VP1, VP2, and VP3 was achieved by infecting Sf9 cells with the three recombinant baculovirus species at equal multiplicities. All three proteins were found to be localized in the nuclear fraction. Electron microscopy of nuclear extracts of the infected cells showed an abundance of SV40-like capsid structures and heterogeneous aggregates of variable size, mostly 20-45 nm. Under the same staining conditions wild-type SV40 virions are 45 nm. The capsid-like particles sedimented in glycerol gradients similarly to authentic wild-type SV40 virions. Pentamers of the major capsid protein VP1 were also seen. Protein analysis on sucrose gradients demonstrated that the capsid-like particles can be disrupted by treatment with the reducing agent dithiothreitol and the calcium chelator EGTA. The capsid-like particles were found to be significantly less stable than SV40 virions and were partially stabilized by calcium ions. Understanding the complex interactions between the capsid proteins is important for the development of an efficient in vitro packaging system for SV40 virions and pseudovirions.

摘要

通过使用杆状病毒表达载体在Sf9细胞中表达三个晚期基因VP1、VP2和VP3,获得了可溶性SV40衣壳蛋白。通过用三种重组杆状病毒以相等的感染复数感染Sf9细胞,实现了衣壳蛋白VP1、VP2和VP3的共表达。发现所有这三种蛋白都定位于细胞核部分。对感染细胞的核提取物进行电子显微镜观察,发现大量类似SV40的衣壳结构以及大小不一的异质聚集体,多数为20 - 45纳米。在相同的染色条件下,野生型SV40病毒粒子为45纳米。类似衣壳的颗粒在甘油梯度中的沉降情况与正宗的野生型SV40病毒粒子相似。还观察到主要衣壳蛋白VP1的五聚体。在蔗糖梯度上进行的蛋白质分析表明,类似衣壳的颗粒可以通过用还原剂二硫苏糖醇和钙螯合剂EGTA处理而被破坏。发现类似衣壳的颗粒比SV40病毒粒子的稳定性明显更低,并且可被钙离子部分稳定。了解衣壳蛋白之间的复杂相互作用对于开发高效的SV40病毒粒子和假病毒体外包装系统很重要。

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