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自主细小病毒小鼠微小病毒的次要衣壳蛋白VP1对于子代单链DNA的包装并非必需,但对于感染性却是必需的。

The minor capsid protein VP1 of the autonomous parvovirus minute virus of mice is dispensable for encapsidation of progeny single-stranded DNA but is required for infectivity.

作者信息

Tullis G E, Burger L R, Pintel D J

机构信息

Department of Molecular Microbiology and Immunology, School of Medicine, University of Missouri--Columbia 65212.

出版信息

J Virol. 1993 Jan;67(1):131-41. doi: 10.1128/JVI.67.1.131-141.1993.

Abstract

The two capsid proteins of minute virus of mice, VP1 and VP2, are generated from a single large open reading frame by alternate splicing of the capsid gene mRNA. Examination of the replication of a series of mutants that express only VP1, only VP2, or neither capsid protein demonstrates that VP2 is necessary for the accumulation and encapsidation of virus progeny single-stranded DNA. VP1 is dispensable for these functions but is required to produce an infectious virion. Virus that lacks VP1 binds to cells as efficiently as wild-type minute virus of mice but fails to initiate a productive infection. Because neither capsid protein is required for viral-DNA replication, these results suggest that virus lacking VP1 is blocked at a step during virus entry, subsequent to cell binding and prior to the initiation of DNA replication.

摘要

小鼠微小病毒的两种衣壳蛋白VP1和VP2,是由衣壳基因mRNA通过可变剪接从单个大的开放阅读框产生的。对一系列仅表达VP1、仅表达VP2或不表达任何衣壳蛋白的突变体的复制情况进行检测表明,VP2对于病毒子代单链DNA的积累和衣壳化是必需的。VP1对于这些功能并非必需,但产生感染性病毒粒子需要VP1。缺乏VP1的病毒与细胞结合的效率与野生型小鼠微小病毒一样,但无法引发有效感染。由于病毒DNA复制不需要任何一种衣壳蛋白,这些结果表明,缺乏VP1的病毒在病毒进入过程中,即在细胞结合之后、DNA复制起始之前的某个步骤被阻断。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/056e/237345/a2da68834a49/jvirol00022-0158-a.jpg

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