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核定位信号和蛋白质背景均介导核输入底物的输入蛋白α特异性。

Nuclear localization signal and protein context both mediate importin alpha specificity of nuclear import substrates.

作者信息

Friedrich Beate, Quensel Christina, Sommer Thomas, Hartmann Enno, Köhler Matthias

机构信息

The Max Delbrueck Center for Molecular Medicine, Robert Roessle Strasse 10, 13125 Berlin, Germany.

出版信息

Mol Cell Biol. 2006 Dec;26(23):8697-709. doi: 10.1128/MCB.00708-06. Epub 2006 Sep 25.

Abstract

The "classical" nuclear protein import pathway depends on importin alpha and importin beta. Importin alpha binds nuclear localization signal (NLS)-bearing proteins and functions as an adapter to access the importin beta-dependent import pathway. In humans, only one importin beta is known to interact with importin alpha, while six alpha importins have been described. Various experimental approaches provided evidence that several substrates are transported specifically by particular alpha importins. Whether the NLS is sufficient to mediate importin alpha specificity is unclear. To address this question, we exchanged the NLSs of two well-characterized import substrates, the seven-bladed propeller protein RCC1, preferentially transported into the nucleus by importin alpha3, and the less specifically imported substrate nucleoplasmin. In vitro binding studies and nuclear import assays revealed that both NLS and protein context contribute to the specificity of importin alpha binding and transport.

摘要

“经典”的核蛋白导入途径依赖于输入蛋白α和输入蛋白β。输入蛋白α结合带有核定位信号(NLS)的蛋白质,并作为一种衔接子发挥作用,以进入依赖输入蛋白β的导入途径。在人类中,已知只有一种输入蛋白β与输入蛋白α相互作用,而已经描述了六种α输入蛋白。各种实验方法提供了证据,表明几种底物是由特定的α输入蛋白特异性转运的。NLS是否足以介导输入蛋白α的特异性尚不清楚。为了解决这个问题,我们交换了两种特征明确的导入底物的NLS,即七叶螺旋桨蛋白RCC1(优先由输入蛋白α3转运到细胞核中)和导入特异性较低的底物核质蛋白。体外结合研究和核导入分析表明,NLS和蛋白质背景都对输入蛋白α结合和转运的特异性有影响。

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