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核纤层相关蛋白2α(LAP2α)在间期细胞核中的去污剂-盐抗性以及在核组装早期与染色体的磷酸化依赖性结合暗示了其在核结构动态变化中的功能。

Detergent-salt resistance of LAP2alpha in interphase nuclei and phosphorylation-dependent association with chromosomes early in nuclear assembly implies functions in nuclear structure dynamics.

作者信息

Dechat T, Gotzmann J, Stockinger A, Harris C A, Talle M A, Siekierka J J, Foisner R

机构信息

nstitute of Biochemistry and Molecular Cell Biology, Biocenter and Institute of Tumor Biology-Cancer Research, University of Vienna, A-1030 Vienna, Austria.

出版信息

EMBO J. 1998 Aug 17;17(16):4887-902. doi: 10.1093/emboj/17.16.4887.

Abstract

Lamina-associated polypeptide (LAP) 2 of the inner nuclear membrane (now LAP2beta) and LAP2alpha are related proteins produced by alternative splicing, and contain a common 187 amino acid N-terminal domain. We show here that, unlike LAP2beta, LAP2alpha behaved like a nuclear non-membrane protein in subcellular fractionation studies and was localized throughout the nuclear interior in interphase cells. It co-fractionated with LAP2beta in nuclear lamina/matrix-enriched fractions upon extraction of nuclei with detergent, salt and nucleases. During metaphase LAP2alpha dissociated from chromosomes and became concentrated around the spindle poles. Furthermore, LAP2alpha was mitotically phosphorylated, and phosphorylation correlated with increased LAP2alpha solubility upon extraction of cells in physiological buffers. LAP2alpha relocated to distinct sites around chromosomes at early stages of nuclear reassembly and intermediarily co-localized with peripheral lamin B and intranuclear lamin A structures at telophase. During in vitro nuclear assembly LAP2alpha was dephosphorylated and assembled into insoluble chromatin-associated structures, and recombinant LAP2alpha was found to interact with chromosomes in vitro. Some LAP2alpha may also associate with membranes prior to chromatin attachment. Altogether the data suggest a role of LAP2alpha in post-mitotic nuclear assembly and in the dynamic structural organization of the nucleus.

摘要

内核膜的核纤层相关多肽(LAP)2(现称为LAP2β)和LAP2α是通过可变剪接产生的相关蛋白,它们含有一个由187个氨基酸组成的共同N端结构域。我们在此表明,与LAP2β不同,LAP2α在亚细胞分级分离研究中表现得像一种核非膜蛋白,并且在间期细胞中定位于整个核内。在用去污剂、盐和核酸酶提取细胞核后,它与LAP2β在富含核纤层/核基质的级分中共分离。在中期,LAP2α从染色体上解离并集中在纺锤体极周围。此外,LAP2α在有丝分裂过程中被磷酸化,并且磷酸化与在生理缓冲液中提取细胞时LAP2α溶解度的增加相关。在核重新组装的早期阶段,LAP2α重新定位到染色体周围的不同位点,并在末期与外周核纤层蛋白B和核内核纤层蛋白A结构中间共定位。在体外核组装过程中,LAP2α去磷酸化并组装成不溶性的染色质相关结构,并且发现重组LAP2α在体外与染色体相互作用。一些LAP2α在与染色质结合之前也可能与膜结合。总之,这些数据表明LAP2α在有丝分裂后核组装和核的动态结构组织中起作用。

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