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蛋白质向细胞核转运的调控:磷酸化的核心作用

Regulation of protein transport to the nucleus: central role of phosphorylation.

作者信息

Jans D A, Hübner S

机构信息

Nuclear Signalling Laboratory, Division for Biochemistry and Molecular Biology, John Curtin School of Medical Research, Australian National University, Canberra, Australia.

出版信息

Physiol Rev. 1996 Jul;76(3):651-85. doi: 10.1152/physrev.1996.76.3.651.

Abstract

Nuclear protein transport is integral to eukaryotic cell processes such as differentiation, transformation, and the control of gene expression. Although the targeting role of nuclear localization signals (NLSs) has been known for some time, more recent results indicate that NLS-dependent nuclear protein import is precisely regulated. Phosphorylation appears to be the main mechanism controlling the nuclear transport of a number of proteins, including transcription factors such as NFkappaB, c-rel, dorsal, and SWI5 from yeast. Cytoplasmic retention factors, intra- and intermolecular NLS masking, and NLS masking by phosphorylation are some of the mechanisms by which phosphorylation specifically regulates nuclear transport. Even nuclear localization of the archetypal NLS-containing simian virus 40 large tumor antigen (T-ag) is regulated, namely by the "CcN motif," which comprises the T-ag NLS ("N") determining ultimate subcellular destination, a casein kinase II site ("C") 13 amino acids NH2-terminal to the NLS modulating the rate of nuclear import, and a cyclin-dependent kinase site ("c") adjacent to the NLS regulating the maximal level of nuclear accumulation. The CcN motif appears to be a special form of phosphorylation-regulated NLS (prNLS), where phosphorylation at site(s) close to the NLS specifically regulates NLS function. The regulation of nuclear transport through phosphorylation and prNLSs appears to be common in eukaryotic cells from yeast and plants to higher mammals.

摘要

核蛋白转运对于真核细胞过程(如分化、转化和基因表达调控)至关重要。尽管核定位信号(NLSs)的靶向作用已为人所知一段时间,但最近的研究结果表明,依赖NLS的核蛋白导入受到精确调控。磷酸化似乎是控制许多蛋白质核转运的主要机制,包括酵母中的转录因子如NFκB、c-rel、背侧蛋白和SWI5。细胞质滞留因子、分子内和分子间NLS掩盖以及磷酸化介导的NLS掩盖是磷酸化特异性调节核转运的一些机制。甚至含有典型NLS的猿猴病毒40大肿瘤抗原(T-ag)的核定位也受到调控,即通过“CcN基序”,它由决定最终亚细胞定位的T-ag NLS(“N”)、位于NLS氨基末端13个氨基酸处调节核输入速率的酪蛋白激酶II位点(“C”)以及与NLS相邻调节核积累最大水平的细胞周期蛋白依赖性激酶位点(“c”)组成。CcN基序似乎是磷酸化调节的NLS(prNLS)的一种特殊形式,其中靠近NLS的位点磷酸化特异性调节NLS功能。通过磷酸化和prNLSs对核转运的调节在从酵母、植物到高等哺乳动物的真核细胞中似乎很常见。

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