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体内MHC II类启动子上功能性调节复合物的组装。

Assembly of functional regulatory complexes on MHC class II promoters in vivo.

作者信息

Fontes J D, Jabrane-Ferrat N, Peterlin B M

机构信息

Howard Hughes Medical Institute, Department of Medicine, University of California at San Francisco, 94143-0724, USA.

出版信息

J Mol Biol. 1997 Jul 18;270(3):336-45. doi: 10.1006/jmbi.1997.1121.

Abstract

Regulatory factors that bind to the X box 1 to 5 (RFX1 to RFX5) and p36 interact with the X box in major histocompatibility class II promoters. RFX1 and RFX5 bind to DNA as a homodimer (RFX1) and heterodimer with p36 (RFX5:p36, the RFX complex), respectively. In this study, we characterized the binding of RFX1 and the RFX complex to the X box in vivo, and evaluated contributions of other proteins that bind to flanking conserved upstream sequences (CUS: S, X, X2, and Y boxes) to these protein-DNA interactions. For this purpose, an intracellular DNA-binding assay was developed. Hybrid protein effectors between RFX1 and RFX5 and the activation domain of VP16 from the herpes simplex virus were co-expressed with plasmid targets, which contained the isolated X box, X box and selected flanking CUS, or the entire DRA promoter. Whereas RFX1 bound better to isolated X boxes, the Y box selected for the binding of the RFX complex and against the binding of RFX1 to the X box. With proper spacing, S and X boxes stabilized the binding of both RFX1 and the RFX complex. The X2 box did not contribute significantly to the binding of either RFX1 or the RFX complex to the X box. Thus, complex protein-protein and protein-DNA interactions dictate the binding of functionally relevant proteins to conserved upstream sequences which regulate class II transcription.

摘要

与X盒1至5结合的调控因子(RFX1至RFX5)和p36与主要组织相容性复合体II类启动子中的X盒相互作用。RFX1和RFX5分别以同二聚体(RFX1)和与p36的异二聚体(RFX5:p36,RFX复合体)形式结合DNA。在本研究中,我们对RFX1和RFX复合体在体内与X盒的结合进行了表征,并评估了与侧翼保守上游序列(CUS:S、X、X2和Y盒)结合的其他蛋白质对这些蛋白质-DNA相互作用的贡献。为此,开发了一种细胞内DNA结合测定法。将RFX1和RFX5与单纯疱疹病毒VP16激活域之间的杂交蛋白效应物与质粒靶标共表达,质粒靶标包含分离的X盒、X盒和选定的侧翼CUS或整个DRA启动子。虽然RFX1与分离的X盒结合更好,但Y盒被选择用于RFX复合体的结合并对抗RFX1与X盒的结合。在适当的间距下,S盒和X盒稳定了RFX1和RFX复合体的结合。X2盒对RFX1或RFX复合体与X盒的结合没有显著贡献。因此,复杂的蛋白质-蛋白质和蛋白质-DNA相互作用决定了功能相关蛋白质与调控II类转录的保守上游序列的结合。

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