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大鼠雪旺细胞细胞周期中的蛋白酶体动力学

Proteasome dynamics during cell cycle in rat Schwann cells.

作者信息

Lafarga Miguel, Fernández Rosario, Mayo Isabel, Berciano María T, Castaño José G

机构信息

Departamento de Anatomia y Biología Celular, Universidad de Cantabria, Santander, Spain.

出版信息

Glia. 2002 Jun;38(4):313-28. doi: 10.1002/glia.10075.

Abstract

The proteasome is responsible for most of the protein degradation that takes place in the cytoplasm and nucleus. Immunofluorescence and electron microscopy are used to study proteasome dynamics during the cell cycle in rat Schwann cells. During interphase, the proteasome is present in the nucleus and cytoplasm and shows no colocalization with cytoskeletal components. Some cytoplasmic proteasomes always localize in the centrosome both in interphase and in mitotic cells and only associate with microtubules during mitosis. The proteasome exits the nucleus during prophase. In anaphase, the proteasome becomes prominent in the region between the two sets of migrating chromosomes and in association with interzonal microtubules and stem bodies. In telophase, the proteasome begins to reenter the nucleus and is prominent in the midbody region until the end of cytokinesis. The proteasome does not colocalize with actin or vimentin during mitosis, except for colocalization with actin in the sheet-like lamellipodia, which serve as substrate attachments for the cell during mitosis. During S phase, nuclear proteasomes colocalize with foci of BrdU incorporation, but this association changes with time: maximal at early S phase and declining as S phase progresses to the end. These results are discussed in relation to the biochemical pathways involved in cell cycle progression.

摘要

蛋白酶体负责细胞质和细胞核中发生的大部分蛋白质降解。免疫荧光和电子显微镜用于研究大鼠雪旺细胞在细胞周期中的蛋白酶体动态。在间期,蛋白酶体存在于细胞核和细胞质中,与细胞骨架成分无共定位。一些细胞质蛋白酶体在间期和有丝分裂细胞中总是定位于中心体,仅在有丝分裂期间与微管相关联。蛋白酶体在前期退出细胞核。在后期,蛋白酶体在两组迁移染色体之间的区域以及与中间区微管和茎体相关联时变得突出。在末期,蛋白酶体开始重新进入细胞核,并在中体区域突出,直到胞质分裂结束。在有丝分裂期间,蛋白酶体除了在片状伪足中与肌动蛋白共定位外,不与肌动蛋白或波形蛋白共定位,片状伪足在有丝分裂期间作为细胞的底物附着部位。在S期,核蛋白酶体与BrdU掺入位点共定位,但这种关联随时间变化:在S期早期最大,随着S期进展到末期而下降。这些结果结合细胞周期进程中涉及的生化途径进行了讨论。

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