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凋亡诱导后,FAS相关因子1在体内与蛋白激酶CK2相互作用。

FAS-associated factor 1 interacts with protein kinase CK2 in vivo upon apoptosis induction.

作者信息

Guerra B, Boldyreff B, Issinger O G

机构信息

University of Southern Denmark, Odense University, Institute for Biochemistry and Molecular Biology, DK-5230 Odense, Denmark.

出版信息

Int J Oncol. 2001 Dec;19(6):1117-26. doi: 10.3892/ijo.19.6.1117.

Abstract

We show here that in several different cell lines protein kinase CK2 and Fas-associated factor 1 (FAF1) exist together in a complex which is stable to high monovalent salt concentration. The CK2/FAF1 complex formation is significantly increased after induction of apoptosis with various DNA damaging agents. Interestingly this effect is only seen in cell lines with an embryonic origin and not when cells have entered a differentiated state. It is further shown that the CK2 specific phosphorylation sites in the FAF1 molecule, i.e. serines 289 and 291 influence this complex formation. Mutation of the CK2 phosphorylation sites in the FAF1 molecule to alanine leads to a 1.5 to 2.0-fold higher association between CK2 and FAF1. Since the CK2 activity did not increase concomitantly with the complex formation we conclude that the FAF1 becomes to the CK2 enzyme so that a normal enzyme catalysis does not take place anymore. Subcellular localization experiments involving CK2 subunits and FAF1 show a co-localization of both CK2 subunits and FAF1 in the peri-nuclear cytoplasm. The majority of CK2 subunits is found in the nucleus. FAF1 is also found in the nucleoli. The results obtained further support the view that protein kinase CK2 plays an important role in certain steps of apoptosis.

摘要

我们在此表明,在几种不同的细胞系中,蛋白激酶CK2和Fas相关因子1(FAF1)共同存在于一个对高单价盐浓度稳定的复合物中。用各种DNA损伤剂诱导细胞凋亡后,CK2/FAF1复合物的形成显著增加。有趣的是,这种效应仅在具有胚胎起源的细胞系中可见,而在细胞进入分化状态时则未观察到。进一步研究表明,FAF1分子中CK2特异性磷酸化位点,即丝氨酸289和291,影响这种复合物的形成。将FAF1分子中的CK2磷酸化位点突变为丙氨酸会导致CK2与FAF1之间的结合增加1.5至2.0倍。由于CK2活性并未随复合物的形成而相应增加,我们得出结论,FAF1与CK2酶结合,从而不再发生正常的酶催化作用。涉及CK2亚基和FAF1的亚细胞定位实验表明,CK2亚基和FAF1在核周细胞质中共定位。大多数CK2亚基存在于细胞核中。FAF1也存在于核仁中。所获得的结果进一步支持了蛋白激酶CK2在细胞凋亡的某些步骤中起重要作用的观点。

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