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与衣壳蛋白的结合促进了猿猴病毒40 DNA的核靶向。

Association with capsid proteins promotes nuclear targeting of simian virus 40 DNA.

作者信息

Nakanishi A, Clever J, Yamada M, Li P P, Kasamatsu H

机构信息

Department of Molecular, Cell, and Developmental Biology, University of California, Los Angeles 90095, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Jan 9;93(1):96-100. doi: 10.1073/pnas.93.1.96.

Abstract

All animal DNA viruses except pox virus utilize the cell nucleus as the site for virus reproduction. Yet, a critical viral infection process, nuclear targeting of the viral genome, is poorly understood. The role of capsid proteins in nuclear targeting of simian virus 40 (SV40) DNA, which is assessed by the nuclear accumulation of large tumor (T) antigen, the initial sign of the infectious process, was tested by two independent approaches: antibody interception experiments and reconstitution experiments. When antibody against viral capsid protein Vp1 or Vp3 was introduced into the cytoplasm, the nuclear accumulation of T antigen was not observed in cells either infected or cytoplasmically injected with virion. Nuclearly introduced anti-Vp3 IgG also showed the inhibitory effect. In the reconstitution experiments, SV40 DNA was allowed to interact with protein components of the virus, either empty particles or histones, and the resulting complexes were tested for the capability of protein components to target the DNA to the nucleus from cytoplasm as effectively as the targeting of DNA in the mature virion. In cells injected with empty particle-DNA, but not in minichromosome-injected cells, T antigen was observed as effectively as in SV40-injected cells. These results demonstrate that SV40 capsid proteins can facilitate transport of SV40 DNA into the nucleus and indicate that Vp3, one of the capsid proteins, accompanies SV40 DNA as it enters the nucleus during virus infection.

摘要

除痘病毒外,所有动物DNA病毒都利用细胞核作为病毒繁殖的场所。然而,一个关键的病毒感染过程,即病毒基因组的核靶向,却鲜为人知。衣壳蛋白在猴病毒40(SV40)DNA核靶向中的作用,通过大T抗原的核积累来评估,大T抗原是感染过程的初始迹象,采用了两种独立的方法进行测试:抗体拦截实验和重组实验。当将针对病毒衣壳蛋白Vp1或Vp3的抗体引入细胞质时,在感染或经细胞质注射病毒体的细胞中均未观察到T抗原的核积累。核内引入的抗Vp3 IgG也显示出抑制作用。在重组实验中,使SV40 DNA与病毒的蛋白质成分(空颗粒或组蛋白)相互作用,并测试所得复合物中蛋白质成分将DNA从细胞质靶向细胞核的能力,其效果与成熟病毒体中DNA的靶向效果相同。在注射了空颗粒-DNA的细胞中,而非注射了微型染色体的细胞中,观察到T抗原的效果与注射SV40的细胞中一样有效。这些结果表明,SV40衣壳蛋白可以促进SV40 DNA转运到细胞核中,并表明衣壳蛋白之一的Vp3在病毒感染期间伴随SV40 DNA进入细胞核。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0ed5/40185/235834207e32/pnas01505-0108-a.jpg

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