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核基质:细胞核内蛋白磷酸化增加的细胞周期依赖性位点。

Nuclear matrix: a cell-cycle-dependent site of increased intranuclear protein phosphorylation.

作者信息

Henry S M, Hodge L D

出版信息

Eur J Biochem. 1983 Jun 1;133(1):23-9. doi: 10.1111/j.1432-1033.1983.tb07425.x.

Abstract

Evidence is presented that the nuclear matrix is a cell-cycle-dependent site of increased intranuclear protein phosphorylation. The incorporation of radioactive phosphate (32P) is highest during the premitotic (G2) phase and 40-50% less in the postmitotic phase (G1). This is observed for both total matrix protein and for several individual polypeptides ranging in molecular mass from greater than 200 kDa to 19 kDa. The phenomenon can be demonstrated when the matrix is isolated from orthophosphate-labeled intact cells, as well as when the matrix is isolated and then incubated in vitro in a protein kinase reaction mixture. The ability of the isolated matrix to mimic the events in vivo indicates the presence of endogenous protein phosphokinase activity and physiological substrates in this isolated nuclear fraction. Further evidence for such mimicry was obtained when amino acid phosphorylation sites were determined. Phosphoserine is the most abundant phosphoamino acid in the matrix labelled both in vitro and in vivo, although phosphothreonine and phosphotyrosine are also present. On the basis of several pieces of data, the endogenous matrix activity appears to be due to multiple protein phosphokinases. Since the maximum phosphorylation coincides with premitosis, the phosphoproteins may play a role in mitotic events. These observations extend and expand the application of this fraction to the study of nuclear structure/function relationships, particularly at the time of mitosis.

摘要

有证据表明,核基质是细胞核内蛋白质磷酸化增加的细胞周期依赖性位点。放射性磷酸盐(32P)的掺入在有丝分裂前期(G2)阶段最高,在有丝分裂后期(G1)阶段则减少40-50%。对于总基质蛋白以及分子量从大于200 kDa到19 kDa的几种单个多肽来说,均观察到这种情况。当从正磷酸盐标记的完整细胞中分离出基质时,以及当分离出基质然后在体外于蛋白激酶反应混合物中孵育时,都可以证明这种现象。分离出的基质模拟体内事件的能力表明,在这个分离出的核部分中存在内源性蛋白磷酸激酶活性和生理底物。当确定氨基酸磷酸化位点时,获得了这种模拟的进一步证据。磷酸丝氨酸是体外和体内标记的基质中最丰富的磷酸氨基酸,不过也存在磷酸苏氨酸和磷酸酪氨酸。基于多项数据,内源性基质活性似乎归因于多种蛋白磷酸激酶。由于最大磷酸化与有丝分裂前期一致,磷酸化蛋白可能在有丝分裂事件中发挥作用。这些观察结果扩展并扩大了该部分在核结构/功能关系研究中的应用,特别是在有丝分裂时。

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