首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >Chromosomal Proteins HMG-14 and HMG-17 Are Released from Mitotic Chromosomes and Imported into the Nucleus by Active Transport
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Chromosomal Proteins HMG-14 and HMG-17 Are Released from Mitotic Chromosomes and Imported into the Nucleus by Active Transport

机译:染色体蛋白HMG-14和HMG-17从有丝分裂染色体上释放,并通过主动转运导入核中

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摘要

The high mobility group 14/17 (HMG-14/ -17) proteins form specific complexes with nucleosome core particles and produce distinct footprints on nucleosomal DNA. Therefore, they could be an integral part of the chromatin fiber. Here we show that during the cell cycle these proteins are transiently dissociated from chromatin. They colocalize with the nuclear DNA in interphase and prophase but not in metaphase and anaphase. They relocate into the nucleus and colocalize again with the DNA in late telophase, concomitantly with the appearance of the nuclear envelope. Thus, these nucleosomal binding proteins are not always associated with chromatin. Using reconstituted nuclei and permeabilized cells, we demonstrate that these two small proteins, with a molecular mass <10 kD, are actively imported into the nucleus. We identify the major elements involved in the nuclear import of these chromosomal proteins: HMG-14/-17 proteins contain an intrinsic bipartite nuclear localization signal, and their entry into the nucleus through nuclear pores requires energy and the participation of importin α. These findings suggest that the cell cycle–related association of HMG-14/-17 with chromatin is dependent on, and perhaps regulated by, nuclear import processes.
机译:高迁移率的14/17组(HMG-14 / -17)蛋白与核小体核心颗粒形成特定的复合物,并在核小体DNA上产生独特的印迹。因此,它们可能是染色质纤维的组成部分。在这里,我们显示了在细胞周期中,这些蛋白质从染色质中瞬时解离。它们在中期和前期与核DNA共定位,而在中期和后期不共定位。它们重新定位到细胞核中,并在末期与DNA再次共定位,并伴随着核被膜的出现。因此,这些核小体结合蛋白并不总是与染色质相关。使用重建的细胞核和通透性细胞,我们证明了这两个小分子的分子质量<10 kD,被积极地导入细胞核中。我们确定了涉及这些染色体蛋白核输入的主要元素:HMG-14 / -17蛋白包含固有的二分核定位信号,并且它们通过核孔进入核需要能量和importinα的参与。这些发现表明,HMG-14 / -17与染色质的细胞周期相关性依赖于核输入过程,并可能受其影响。

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