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类固醇生成因子1对序列特异性脱氧核糖核酸(DNA)的识别:DNA结合结构域羧基末端的一个螺旋对于复合物稳定性是必需的。

Sequence-specific deoxyribonucleic acid (DNA) recognition by steroidogenic factor 1: a helix at the carboxy terminus of the DNA binding domain is necessary for complex stability.

作者信息

Little Tanya H, Zhang Yongbo, Matulis Christina K, Weck Jennifer, Zhang Zhipeng, Ramachandran Aparna, Mayo Kelly E, Radhakrishnan Ishwar

机构信息

Department of Biochemistry, Molecular Biology, and Cell Biology, Northwestern University, Evanston, Illinois 60208-3500, USA.

出版信息

Mol Endocrinol. 2006 Apr;20(4):831-43. doi: 10.1210/me.2005-0384. Epub 2005 Dec 8.

Abstract

Steroidogenic factor 1 (SF1) is a member of the NR5A subfamily of nuclear hormone receptors and is considered a master regulator of reproduction because it regulates a number of genes encoding reproductive hormones and enzymes involved in steroid hormone biosynthesis. Like other NR5A members, SF1 harbors a highly conserved approximately 30-residue segment called the FTZ-F1 box C-terminal to the core DNA binding domain (DBD) common to all nuclear receptors and binds to 9-bp DNA sequences as a monomer. Here we describe the solution structure of the SF1 DBD in complex with an atypical sequence in the proximal promoter region of the inhibin-alpha gene that encodes a subunit of a reproductive hormone. SF1 forms a specific complex with the DNA through a bipartite motif binding to the major and minor grooves through the core DBD and the N-terminal segment of the FTZ-F1 box, respectively, in a manner previously described for two other monomeric receptors, nerve growth factor-induced-B and estrogen-related receptor 2. However, unlike these receptors, SF1 harbors a helix in the C-terminal segment of the FTZ-F1 box that interacts with both the core DBD and DNA and serves as an important determinant of stability of the complex. We propose that the FTZ-F1 helix along with the core DBD serves as a platform for interactions with coactivators and other DNA-bound factors in the vicinity.

摘要

类固醇生成因子1(SF1)是核激素受体NR5A亚家族的成员,被认为是生殖的主要调节因子,因为它调节许多编码生殖激素和参与类固醇激素生物合成的酶的基因。与其他NR5A成员一样,SF1在所有核受体共有的核心DNA结合结构域(DBD)的C端含有一个高度保守的约30个残基的片段,称为FTZ-F1框,并以单体形式与9bp的DNA序列结合。在这里,我们描述了SF1 DBD与抑制素α基因近端启动子区域中的非典型序列形成复合物的溶液结构,该基因编码一种生殖激素的亚基。SF1通过一个二分基序与DNA形成特异性复合物,该基序分别通过核心DBD和FTZ-F1框的N端片段与大沟和小沟结合,其方式与另外两个单体受体神经生长因子诱导的B和雌激素相关受体2先前描述的方式相同。然而,与这些受体不同的是,SF1在FTZ-F1框的C端片段中含有一个螺旋,该螺旋与核心DBD和DNA相互作用,并作为复合物稳定性的重要决定因素。我们提出,FTZ-F1螺旋与核心DBD一起作为与附近的共激活因子和其他DNA结合因子相互作用的平台。

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