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D4476 a cell-permeant inhibitor of CK1 suppresses the site-specific phosphorylation and nuclear exclusion of FOXO1a

机译：D4476是CK1的细胞渗透抑制剂可抑制FOXO1a的位点特异性磷酸化和核排斥

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摘要

The protein kinase CK1 phosphorylates serine residues that are located close to another phosphoserine in the consensus pSer-Xaa-Xaa-Ser. This specificity generates regions in its target proteins containing two or more neighbouring phosphoserine residues, termed here multisite phosphorylation domains (MPDs). In this paper, we demonstrate that D4476 is a potent and rather selective inhibitor of CK1 in vitro and in cells. In H4IIE hepatoma cells, D4476 specifically inhibits the phosphorylation of endogenous forkhead box transcription factor O1a (FOXO1a) on Ser322 and Ser325 within its MPD, without affecting the phosphorylation of other sites. Our results indicate that these residues are targeted by CK1 in vivo and that the CK1-mediated phosphorylation of the MPD is required for accelerated nuclear exclusion of FOXO1a in response to IGF-1 and insulin. D4476 is much more potent and specific than IC261 or CKI-7, and is therefore the most useful CK1 inhibitor currently available for identifying physiological substrates of CK1.

机译：蛋白激酶CK1使位于共有pSer-Xaa-Xaa-Ser中另一个磷酸丝氨酸附近的丝氨酸残基磷酸化。这种特异性在其靶蛋白中产生包含两个或多个相邻磷酸丝氨酸残基的区域，在此称为多位磷酸化结构域（MPD）。在本文中，我们证明D4476是体外和细胞中CK1的有效且相当选择性的抑制剂。在H4IIE肝癌细胞中，D4476特异性抑制其MPD中Ser322和Ser325上的内源性叉头箱转录因子O1a（FOXO1a）的磷酸化，而不会影响其他位点的磷酸化。我们的结果表明，这些残基在体内被CK1靶向，并且CK1介导的MPD磷酸化对于响应IGF-1和胰岛素的FOXO1a加速核排斥是必需的。 D4476比IC261或CKI-7更有效和更具特异性，因此是目前可用于鉴定CK1生理底物的最有用的CK1抑制剂。

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期刊名称 EMBO Reports
作者
Graham Rena; Jenny Bain; Matthew Elliott; Philip Cohen;
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年(卷),期 2004(5),1
年度 2004
页码 60–65
总页数 6
原文格式 PDF
正文语种
中图分类分子生物学;细胞生物学;
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专利

1. Kinase activity of casein kinase 1 delta (CK1 delta) is modulated by protein kinase C alpha (PKC alpha) by site-specific phosphorylation within the kinase domain of CK1 delta [J] . Meng Zhigang, Boehm Thomas, Xu Pengfei, Biochimica et biophysica acta: BBA: International journal of biochemistry, biophysics and molecular biololgy. Proteins and Proteomics . 2019,第7a8期

机译：酪蛋白激酶1δ（CK1 delta）的激酶活性通过CK1 Delta的激酶结构域内的位点特异性磷酸化通过蛋白激酶Cα（PKCα）调节
2. Gene expression levels of Casein kinase 1 (CK1) isoforms are correlated to adiponectin levels in adipose tissue of morbid obese patients and site-specific phosphorylation mediated by CK1 influences multimerization of adiponectin [J] . Xu Pengfei, Fischer-Posovszky Pamela, Bischof Joachim, Molecular and Cellular Endocrinology . 2015,第3期

机译：酪蛋白激酶1（CK1）同工型的基因表达水平与病态肥胖患者脂肪组织中脂联素水平相关，并且由CK1介导的位点特异性磷酸化影响脂联素的多聚化
3. CK1 delta kinase activity is modulated by protein kinase C alpha (PKC alpha)-mediated site-specific phosphorylation [J] . Meng Zhigang, Bischof Joachim, Ianes Chiara, Amino acids . 2016,第5期

机译：CK1δ激酶活性受蛋白激酶Cα（PKCα）介导的位点特异性磷酸化的调节
4. Serine Phosphorylation of the Small Phosphoprotein ICAP1 Inhibits Its Nuclear Accumulation [D] . Su, Valerie Liao. 2021

机译：小磷蛋白ICAP1的丝氨酸磷酸化抑制其核积累
5. Site-specific phosphorylation of casein kinase 1 δ (CK1δ) regulates its activity towards the circadian regulator PER2 [O] . Gracie Wee Ling Eng, Edison, David M. Virshup -1

机译：酪蛋白激酶1δ（CK1δ）的位点特异性磷酸化调节其对昼夜节律调节器PER2的活性
6. D4476, a cell-permeant inhibitor of CK1, suppresses the site-specific phosphorylation and nuclear exclusion of FOXO1a [O] . Rena, Graham, Bain, Jenny, Elliott, Matthew, 2004

机译：D4476是CK1的细胞渗透抑制剂，可抑制FOXO1a的位点特异性磷酸化和核排斥

D4476 a cell-permeant inhibitor of CK1 suppresses the site-specific phosphorylation and nuclear exclusion of FOXO1a

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