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Evaluation of Mammalian Cell-free Systems of Nuclear Disassembly and Assembly

机译:哺乳动物无核核拆装系统的评价

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摘要

Mammalian cell-free systems are very useful for the biochemical and structural study of nuclear disassembly and assembly. Through experimental manipulations, the role of specific proteins in these processes can be studied. Recently, we intended to examine the involvement of integral and peripheral inner nuclear membrane proteins in nuclear disassembly and assembly. However, we could not achieve proper disassembly when isolated interphase HeLa nuclei were exposed to mitotic soluble extracts obtained from the same cell line and containing cyclin B1. Homogenates of synchronized mitotic HeLa cells left to reassemble their nuclei generated incomplete nuclear envelopes on chromatin masses. Digitonin-permeabilized mitotic cells also assembled incomplete nuclei, generating a lot of cytoplasmic inclusions of inner nuclear membrane proteins as an intermediate. These results were therefore used as a basis for a critical evaluation of mammalian cell-free systems. We present here evidence that cell synchronization itself can interfere with the progress of nuclear assembly, possibly by causing aberrant nuclear disassembly and/or by inducing the formation of an abnormal number of mitotic spindles. >(J Histochem Cytochem 56:157–173, 2008)
机译:哺乳动物无细胞系统对于核拆卸和组装的生化和结构研究非常有用。通过实验操作,可以研究特定蛋白质在这些过程中的作用。最近,我们打算检查完整的和外围的内部核膜蛋白在核拆卸和组装中的参与。但是,当分离的HeLa中间核暴露于得自同一细胞系且含有细胞周期蛋白B1的有丝分裂可溶性提取物时,我们无法实现适当的拆卸。同步有丝分裂的HeLa细胞的匀浆物会重新组装其核,从而在染色质上产生不完整的核膜。洋地黄皂通透的有丝分裂细胞也组装了不完整的核,从而产生了许多内核膜蛋白的胞质内含物作为中间体。因此,这些结果被用作对哺乳动物无细胞系统进行严格评估的基础。我们在这里提供的证据表明,细胞同步本身本身可能会干扰核组装的进程,可能会引起异常的核拆卸和/或诱导异常数量的有丝分裂纺锤体形成。 >(J Histochem Cytochem 56:157-173,2008)

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