Exportins can inhibit major mitotic assembly events in vitro: membrane fusion, nuclear pore formation, and spindle assembly.

Matthew S Nord, Cyril Bernis, Sarah Carmona, Dennis C Garland, Anna Travesa, Douglass J Forbes
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引用次数: 2

Abstract

Xenopus: egg extracts are a powerful in vitro tool for studying complex biological processes, including nuclear reconstitution, nuclear membrane and pore assembly, and spindle assembly. Extracts have been further used to demonstrate a moonlighting regulatory role for nuclear import receptors or importins on these cell cycle assembly events. Here we show that exportins can also play a role in these events. Addition of Crm1, Exportin-t, or Exportin-5 decreased nuclear pore assembly in vitro. RanQ69L-GTP, a constitutively active form of RanGTP, ameliorated inhibition. Both Crm1 and Exportin-t inhibited fusion of nuclear membranes, again counteracted by RanQ69L-GTP. In mitotic extracts, Crm1 and Exportin-t negatively impacted spindle assembly. Pulldowns from the extracts using Crm1- or Exportin-t-beads revealed nucleoporins known to be essential for both nuclear pore and spindle assembly, with RanQ69L-GTP decreasing a subset of these target interactions. This study suggests a model where exportins, like importins, can regulate major mitotic assembly events.

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输出蛋白可以抑制体外有丝分裂的主要组装事件:膜融合、核孔形成和纺锤体组装。
爪蟾卵提取物是研究复杂生物过程的有力体外工具,包括核重构、核膜和孔组装以及纺锤体组装。提取物已进一步用于证明核输入受体或输入蛋白在这些细胞周期组装事件中的兼职调节作用。在这里,我们展示了导出也可以在这些事件中发挥作用。添加Crm1、Exportin-t或Exportin-5可减少体外核孔组装。RanGTP的组成活性形式RanQ69L-GTP改善了抑制作用。Crm1和export -t均抑制核膜融合,同样被RanQ69L-GTP抵消。在有丝分裂提取物中,Crm1和export -t对纺锤体组装产生负面影响。使用Crm1-或export -t-beads提取的下拉结果显示,已知核孔蛋白对核孔和纺锤体组装都是必不可少的,而RanQ69L-GTP减少了这些靶标相互作用的一部分。本研究提出了一个模型,其中出口蛋白和进口蛋白一样,可以调节主要的有丝分裂组装事件。
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