Lopez D, Nackley A C, Shea-Eaton W, Xue J, Schimmer B P, McLean M P
Department of Obstetrics and Gynecology, University of South Florida, Tampa, USA.
Endocrine. 2001 Apr;14(3):353-62. doi: 10.1385/ENDO:14:3:353.
The involvement of cyclic adenosine monophosphate cAMP-dependent protein kinase A (PKA) in the regulation of the steroidogenic acute regulatory protein (StAR) and the high-density lipoprotein receptor (HDL-R) genes by steroidogenic factor-1 (SF-1) and cAMP were examined. Cotransfection studies carried out in Kin 8 cells, a Y1 cell line (mouse adrenal) with a mutation in the type I PKA regulatory subunit, demonstrated that an intact PKA is required for maximal activation and that SF-1 participates in cAMP regulation of these genes. Site-directed mutational analysis was performed to examine which SF-1 regions could be involved in SF-1 transcriptional activation of the StAR and HDL-R genes. SF-1 regions protein analyzed were amino acids Thr 60, Ser 203, Ser 431, Thr 462, and the activation function-2 domain (amino acids 449-462). Plasmids encoding each of the mutated SF-1 proteins were cotransfected with the StAR and HDL-R promoter constructs into human bladder carcinoma (HTB-9) cells in the presence or absence of dibutyryl cAMP. The results of these studies suggest that although SF-1 is required for optimal promoter response to cAMP, transcriptional activation of genes by SF-1 and cAMP are promoter dependent, perhaps resulting from gene-specific interactions of this transcription factor with other regulatory proteins.
研究了环磷酸腺苷(cAMP)依赖性蛋白激酶A(PKA)在类固醇生成因子1(SF-1)和cAMP对类固醇生成急性调节蛋白(StAR)和高密度脂蛋白受体(HDL-R)基因调控中的作用。在Kin 8细胞(一种I型PKA调节亚基发生突变的Y1细胞系,来自小鼠肾上腺)中进行的共转染研究表明,完整的PKA是最大激活所必需的,且SF-1参与了这些基因的cAMP调控。进行了定点突变分析,以检查哪些SF-1区域可能参与StAR和HDL-R基因的SF-1转录激活。分析的SF-1区域蛋白包括苏氨酸60、丝氨酸203、丝氨酸431、苏氨酸462以及激活功能-2结构域(氨基酸449 - 462)。在存在或不存在二丁酰cAMP的情况下,将编码每种突变SF-1蛋白的质粒与StAR和HDL-R启动子构建体共转染到人膀胱癌细胞(HTB-9)中。这些研究结果表明,尽管SF-1是启动子对cAMP产生最佳反应所必需的,但SF-1和cAMP对基因的转录激活是启动子依赖性的,这可能是由于该转录因子与其他调节蛋白之间的基因特异性相互作用所致。
