Fushi tarazu 因子 1 配体结合域/Fushi tarazu 肽复合物的晶体结构鉴定新型核受体。
Crystal structure of Fushi tarazu factor 1 ligand binding domain/Fushi tarazu peptide complex identifies new class of nuclear receptors.
机构信息
Department of Biology, College of Life Science and Biotechnology, Yonsei University, Shinchon-dong, Seodaemun-gu 134, Seoul 120-749, Korea.
出版信息
J Biol Chem. 2011 Sep 9;286(36):31225-31. doi: 10.1074/jbc.M111.252916. Epub 2011 Jul 20.
Abstract
The interaction between the orphan nuclear receptor FTZ-F1 (Fushi tarazu factor 1) and the segmentation gene protein FTZ is critical for specifying alternate parasegments in the Drosophila embryo. Here, we have determined the structure of the FTZ-F1 ligand-binding domain (LBD)·FTZ peptide complex using x-ray crystallography. Strikingly, the ligand-binding pocket of the FTZ-F1 LBD is completely occupied by helix 6 (H6) of the receptor, whereas the cofactor FTZ binds the co-activator cleft site of the FTZ-F1 LBD. Our findings suggest that H6 is essential for transcriptional activity of FTZ-F1; this is further supported by data from mutagenesis and activity assays. These data suggest that FTZ-F1 might belong to a novel class of ligand-independent nuclear receptors. Our findings are intriguing given that the highly homologous human steroidogenic factor-1 and liver receptor homolog-1 LBDs exhibit sizable ligand-binding pockets occupied by putative ligand molecules.
摘要
孤儿核受体 FTZ-F1(Fushi tarazu 因子 1)与分节基因蛋白 FTZ 之间的相互作用对于果蝇胚胎中指定交替副节是至关重要的。在这里,我们使用 X 射线晶体学确定了 FTZ-F1 配体结合域(LBD)·FTZ 肽复合物的结构。引人注目的是,FTZ-F1 LBD 的配体结合口袋完全被受体的螺旋 6(H6)占据,而辅因子 FTZ 结合 FTZ-F1 LBD 的共激活剂裂隙位点。我们的发现表明 H6 对于 FTZ-F1 的转录活性是必不可少的;这一观点得到了突变和活性测定数据的进一步支持。这些数据表明,FTZ-F1 可能属于一类新型的配体非依赖性核受体。我们的发现很有趣,因为高度同源的人类类固醇生成因子-1 和肝受体同源物-1 LBD 具有由假定配体分子占据的大配体结合口袋。
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