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首页> 外文期刊>Journal of Molecular Biology >Solution structure of the heterotrimeric complex between the interaction domains of RFX5 and RFXAP from the RFX gene regulatory complex.
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Solution structure of the heterotrimeric complex between the interaction domains of RFX5 and RFXAP from the RFX gene regulatory complex.

机译:RFX基因调控复合体中RFX5和RFXAP相互作用域之间的异三聚体复合体的溶液结构。

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The mammalian immune response is mediated by a heterotetrameric transcriptional control complex, called regulatory factor X (RFX), that regulates the expression of major histocompatibility complex class II genes. RFX comprises three proteins: RFX5 (two copies), RFXAP, and RFXB, and mutations and deletions that prevent the assembly of the RFX complex have been linked to a severe immunodeficiency disorder. Two RFX5 molecules and one RFXAP molecule assemble in the cytoplasm prior to nuclear localization, a process mediated by an N-terminal "dimerization domain" of RFX5 (RFX5(N)) and a C-terminal domain of RFXAP (RFXAP(C)). We previously presented evidence that RFXAP(C) is unstructured in the absence of RFX5(N) but adopts a regular structure in the RFX5(N)(2)-RFXAP(C) complex and that the RFX5(N)(2)-RFXAP(C) complex binds RFXB with high affinity. We now report the structure of the RFX5(N)(2)-RFXAP(C) complex, determined in solution by (15)N- and (13)C-edited NMR spectroscopy. RFX5(N) consists of a long central helix flanked by two shorter helices. The central helices of the two RFX5(N) molecules form an antiparallel coiled coil, and the flanking helices pack at the ends of the long helices in a perpendicular arrangement such that the RFX5(N) dimer is shaped like a staple. RFXAP(C) consists of two alpha-helices that form a V-shaped structure that packs within the RFX5(N)(2) staple. Leucine residues in the leucine-rich region of RFX5(N) (62-LYLYLQL-68) that are critical for major histocompatibility complex class II gene expression in vivo contribute to both the dimer (Leu64 and Leu68) and the RFX5(N)-RFXAP(C) interfaces (Leu62 and Leu66). The clustering of hydrophobic residues from different regions of RFXAP(C) suggests a potential binding site for RFXB.
机译:哺乳动物的免疫反应由称为调节因子X(RFX)的异四聚体转录控制复合物介导,该复合物调节主要组织相容性复合物II类基因的表达。 RFX包含三种蛋白质:RFX5(两个副本),RFXAP和RFXB,并且阻止RFX复合物装配的突变和缺失与严重的免疫缺陷疾病有关。两个RFX5分子和一个RFXAP分子在核定位之前在细胞质中组装,该过程由RFX5(RFX5(N))的N端“二聚结构域”和RFXAP(RFXAP(C))的C端结构域介导。 。我们先前提供的证据表明,在没有RFX5(N)的情况下,RFXAP(C)是非结构化的,但是在RFX5(N)(2)-RFXAP(C)复合物中采用规则结构,并且RFX5(N)(2)- RFXAP(C)复合物以高亲和力结合RFXB。现在,我们报告的RFX5(N)(2)-RFXAP(C)复杂的结构,由(15)N-和(13)C编辑的NMR光谱法在溶液中确定。 RFX5(N)由一个较长的中央螺旋线和两个较短的螺旋线组成。两个RFX5(N)分子的中心螺旋形成一个反平行的盘绕线圈,侧翼螺旋以垂直排列的方式排列在长螺旋的末端,以使RFX5(N)二聚体的形状像订书钉一样。 RFXAP(C)由两个形成V形结构的alpha螺旋组成,该结构包装在RFX5(N)(2)订书钉内。 RFX5(N)(62-LYLYLQL-68)的富含亮氨酸的区域中的亮氨酸残基对体内主要的组织相容性复合物II类基因的表达至关重要,有助于形成二聚体(Leu64和Leu68)和RFX5(N)- RFXAP(C)接口(Leu62和Leu66)。来自RFXAP(C)不同区域的疏水残基的聚集表明RFXB有潜在的结合位点。

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