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乳头瘤病毒衣壳的成熟

Maturation of papillomavirus capsids.

作者信息

Buck Christopher B, Thompson Cynthia D, Pang Yuk-Ying S, Lowy Douglas R, Schiller John T

机构信息

Laboratory of Cellular Oncology, Building 37, Room 4106, 9000 Rockville Pike, Bethesda, MD 20892-4263, USA.

出版信息

J Virol. 2005 Mar;79(5):2839-46. doi: 10.1128/JVI.79.5.2839-2846.2005.

Abstract

The papillomavirus capsid is a nonenveloped icosahedral shell formed by the viral major structural protein, L1. It is known that disulfide bonds between neighboring L1 molecules help to stabilize the capsid. However, the kinetics of inter-L1 disulfide bond formation during particle morphogenesis have not previously been examined. We have recently described a system for producing high-titer papillomavirus-based gene transfer vectors (also known as pseudoviruses) in mammalian cells. Here we show that papillomavirus capsids produced using this system undergo a maturation process in which the formation of inter-L1 disulfide bonds drives condensation and stabilization of the capsid. Fully mature capsids exhibit improved regularity and resistance to proteolytic digestion. Although capsid maturation for other virus types has been reported to occur in seconds or minutes, papillomavirus capsid maturation requires overnight incubation. Maturation of the capsids of human papillomavirus types 16 and 18 proceeds through an ordered accumulation of dimeric and trimeric L1 species, whereas the capsid of bovine papillomavirus type 1 matures into more extensively cross-linked forms. The presence of encapsidated DNA or the minor capsid protein, L2, did not have major effects on the kinetics or extent of capsid maturation. Immature capsids and capsids formed from L1 mutants with impaired disulfide bond formation are infectious but physically fragile. Consequently, capsid maturation is essential for efficient purification of papillomavirus-based gene transfer vectors. Despite their obvious morphological differences, mature and immature capsids are similarly neutralizable by various L1- and L2-specific antibodies.

摘要

乳头瘤病毒衣壳是一种由病毒主要结构蛋白L1形成的无包膜二十面体壳。已知相邻L1分子之间的二硫键有助于稳定衣壳。然而,此前尚未研究颗粒形态发生过程中L1间二硫键形成的动力学。我们最近描述了一种在哺乳动物细胞中生产基于乳头瘤病毒的高滴度基因转移载体(也称为假病毒)的系统。在此我们表明,使用该系统生产的乳头瘤病毒衣壳经历一个成熟过程,其中L1间二硫键的形成驱动衣壳的凝聚和稳定。完全成熟的衣壳表现出更好的规则性和对蛋白水解消化的抗性。尽管据报道其他病毒类型的衣壳成熟在数秒或数分钟内发生,但乳头瘤病毒衣壳成熟需要过夜孵育。人乳头瘤病毒16型和18型衣壳的成熟通过二聚体和三聚体L1物种的有序积累进行,而牛乳头瘤病毒1型衣壳成熟为交联程度更高的形式。衣壳化DNA或次要衣壳蛋白L2的存在对衣壳成熟的动力学或程度没有重大影响。未成熟衣壳以及由二硫键形成受损的L1突变体形成的衣壳具有感染性,但物理上很脆弱。因此,衣壳成熟对于基于乳头瘤病毒的基因转移载体的有效纯化至关重要。尽管成熟和未成熟衣壳在形态上有明显差异,但它们同样可被各种L1和L2特异性抗体中和。

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