Ran及其结合与调控蛋白在核膜装配过程中的调控作用

核膜在细胞周期中呈现高度的动态性：在细胞分裂的前中期,核膜崩解并分散到细胞质中;在细胞分裂的后期,核膜开始在染色体的表面重新装配,最终形成完整的核膜结构。近期的研究发现,Ran GTP酶、物质转运蛋白importinβ、内层核膜蛋白LBR（lamin B receptor）以及核孔复合体蛋白nucleoporins在核膜重建的过程中起关键性调控作用,并受到细胞周期调控因子p34cdc2激酶的调节。LBR是一个八次跨膜的膜蛋白,主要定位于内层核膜。在细胞分裂的早期,随着核膜崩解,LBR与核膜崩解而生成的小膜泡一起分散到细胞质中;在细胞分裂的后期,通过LBR与importinβ相互结合,含有LBR的膜泡被importinβ携带至染色质的表面参与核膜重建。目前已知p34cdc2激酶对LBR与importinβ介导的核膜重建起重要调控作用。Nucleoporins是核孔复合体主要组分。随核膜崩解,核孔复合体解聚成nucleoporins,分散到细胞质中,或结合到其他亚细胞成分上。细胞分裂后期,核孔复合体伴随核膜装配而组装。

Ran GTPase and its binding proteins regulate the nuclear envelope assembly

Ran,a Ras-like nuclear GTPase,plays a pivital role in the regulataion of the nuclear envelope assembly under the cooperation of its binding proteins RanGAP1,RCC1,importins,etc..LBR（lamin B receptor）,a chromatin and lamin B binding protein in the inner nuclear membrane,targets the membrane precursor vesicles to the chromatin mediated by importin β during the nuclear envelope（NE） assembly.It was found that the aa 69-90 of LBR sequence are required to bind importin β at aa 45-462,and the binding is essential for the NE membrane precursor vesicle targeting to the chromatin.It is also demonstrated that this binding is cell cycle-regulated and dependent on the phosphorylation of LBR S71 by p34cdc2 kinase.LBR depletion by RNAi,or perturbation of the interaction of LBR with importin β,causes the NE assembly failure and abnormal chromatin decondensation of the daughter cell nuclei,leading to the daughter cell death at early G1 phase by apoptosis.importin β also targets the nuceoporins to the chromatin regulated by Ran and its binding proteins and regulators.