Mirk蛋白激酶由MKK3激活,并作为肝细胞核因子1α(HNF1α)的转录激活因子发挥作用。
Mirk protein kinase is activated by MKK3 and functions as a transcriptional activator of HNF1alpha.
作者信息
Lim Seunghwan, Jin Kideok, Friedman Eileen
机构信息
Pathology Department, Upstate Medical University, Syracuse, New York 13210, USA.
出版信息
J Biol Chem. 2002 Jul 12;277(28):25040-6. doi: 10.1074/jbc.M203257200. Epub 2002 Apr 29.
Mirk/Dyrk1B is an arginine-directed serine/threonine protein kinase that is expressed at low levels in most normal tissues but at elevated levels in many tumor cell lines and in normal skeletal muscle. Colon carcinoma cell lines stably overexpressing Mirk proliferated in serum-free medium, but the mechanism of Mirk action is unknown. DCoHm (dimerization cofactor of hepatocyte nuclear factor 1alpha ( HNF1alpha) from muscle), a novel gene of the DCoH family with 78% amino acid identity to DCoH, was identified as a Mirk-binding protein by yeast two-hybrid analysis and cloned. Mirk co-immunoprecipitated with DCoHm and bound to DCoHm in glutathione S-transferase pull-down assays. DCoH stabilizes HNF1alpha as a dimer and enhances its transcriptional activity on the beta-fibrinogen promoter reporter, and DCoHm had similar activity. Mirk enhanced HNF1alpha transcriptional activity in a dose-dependent manner, whereas two kinase-inactive Mirk mutants and a Mirk N-terminal deletion mutant did not. Mirk, DCoHm, and HNF1alpha formed a complex. Mirk bound to a specific region within the CREB-binding protein-binding region of HNF1alpha and phosphorylated HNF1alpha at a site adjacent to the Mirk-binding region. Conversely, the HNF1alpha binding domain was located within the first five conserved kinase subdomains of Mirk. Mirk co-immunoprecipitated with the MAPK kinase MKK3, an upstream activator of p38. MKK3 enhanced Mirk kinase activity and the transcriptional activation of HNF1alpha by Mirk, suggesting that Mirk, like p38, is activated by certain environmental stress agents. The Mirk-binding protein DCoH has been shown to be selectively expressed in colon carcinomas but not in normal tissue. Mirk may function as an HNF1alpha transcriptional activator in response to an MKK3-mediated stress signal, and the selective expression of DCoH could restrict the Mirk response to carcinoma cells.
Mirk/Dyrk1B是一种精氨酸定向的丝氨酸/苏氨酸蛋白激酶,在大多数正常组织中低水平表达,但在许多肿瘤细胞系和正常骨骼肌中表达升高。稳定过表达Mirk的结肠癌细胞系在无血清培养基中增殖,但其作用机制尚不清楚。通过酵母双杂交分析鉴定并克隆了DCoHm(来自肌肉的肝细胞核因子1α(HNF1α)的二聚化辅因子),它是DCoH家族的一个新基因,与DCoH有78%的氨基酸同一性。在谷胱甘肽S-转移酶下拉实验中,Mirk与DCoHm共免疫沉淀并结合。DCoH作为二聚体稳定HNF1α,并增强其对β-纤维蛋白原启动子报告基因的转录活性,DCoHm也有类似活性。Mirk以剂量依赖的方式增强HNF1α转录活性,而两个激酶失活的Mirk突变体和一个Mirk N端缺失突变体则无此作用。Mirk、DCoHm和HNF1α形成复合物。Mirk与HNF1α的CREB结合蛋白结合区域内的一个特定区域结合,并在与Mirk结合区域相邻的位点磷酸化HNF1α。相反,HNF1α结合域位于Mirk的前五个保守激酶亚结构域内。Mirk与p38的上游激活剂丝裂原活化蛋白激酶激酶MKK3共免疫沉淀。MKK3增强Mirk激酶活性以及Mirk对HNF1α的转录激活作用,表明Mirk与p38一样,可被某些环境应激因子激活。已证明Mirk结合蛋白DCoH在结肠癌中选择性表达,而在正常组织中不表达。Mirk可能作为一种HNF1α转录激活剂,响应MKK3介导的应激信号,而DCoH的选择性表达可能将Mirk的反应限制在癌细胞中。
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