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对博尔纳病病毒p10蛋白中一种指导核输入的异常输入蛋白α结合基序的表征。

Characterization of an unusual importin alpha binding motif in the borna disease virus p10 protein that directs nuclear import.

作者信息

Wolff Thorsten, Unterstab Gunhild, Heins Gudrun, Richt Juergen A, Kann Michael

机构信息

Robert-Koch-Institut, Nordufer 20, 13353 Berlin, Germany.

出版信息

J Biol Chem. 2002 Apr 5;277(14):12151-7. doi: 10.1074/jbc.M109103200. Epub 2002 Jan 16.

Abstract

Nuclear import of many cellular and viral proteins is mediated by short nuclear localization signals (NLS) that are recognized by intracellular receptor proteins belonging to the importin/karyopherin alpha and beta families. The primary structure of NLS is not well defined, but most contain at least three basic amino acids and harbor the relative consensus sequence K(K/R)X(K/R). We have studied the nuclear import of the Borna disease virus p10 protein that lacks a canonical oligobasic NLS. It is shown that the p10 protein exhibits all characteristics of an actively transported molecule in digitonin-permeabilized cells. Import activity was found to reside in the 20 N-terminal p10 amino acids that are devoid of an NLS consensus motif. Unexpectedly, p10-dependent import was blocked by a peptide inhibitor of importin alpha-dependent nuclear translocation, and the transport activity of the p10 N-terminal domain was shown to correlate with the ability to bind to importin alpha. These findings suggest that nuclear import of the Borna disease virus p10 protein occurs through a nonconventional karyophilic signal and highlight that the cellular importin alpha NLS receptor proteins can recognize nuclear targeting signals that substantially deviate from the consensus sequence.

摘要

许多细胞和病毒蛋白的核输入是由短核定位信号(NLS)介导的,这些信号被属于输入蛋白/核转运蛋白α和β家族的细胞内受体蛋白识别。NLS的一级结构尚未明确界定,但大多数至少含有三个碱性氨基酸,并具有相对一致的序列K(K/R)X(K/R)。我们研究了缺乏典型寡聚碱性NLS的博尔纳病病毒p10蛋白的核输入。结果表明,p10蛋白在洋地黄皂苷通透细胞中表现出主动转运分子的所有特征。发现输入活性存在于20个N端p10氨基酸中,这些氨基酸缺乏NLS一致基序。出乎意料的是,p10依赖的输入被输入蛋白α依赖的核转位的肽抑制剂阻断,并且p10 N端结构域的转运活性与结合输入蛋白α的能力相关。这些发现表明,博尔纳病病毒p10蛋白的核输入通过非常规的亲核信号发生,并突出表明细胞输入蛋白α NLS受体蛋白可以识别与一致序列有很大偏差的核靶向信号。

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