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首页> 外文期刊>Biochemical and Biophysical Research Communications >C-terminal tail of NADPH oxidase organizer 1 (Noxo1) mediates interaction with NADPH oxidase activator (Noxa1) in the NOX1 complex
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C-terminal tail of NADPH oxidase organizer 1 (Noxo1) mediates interaction with NADPH oxidase activator (Noxa1) in the NOX1 complex

机译:NADPH氧化酶组织机1(NOXO1)的C末端尾部介导与NOX1复合物中NADPH氧化酶活化剂(NOXA1)的相互作用

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Abstract NOX1 (NADPH oxidase) similar to phagocyte NADPH oxidase, is expressed mainly in the colon epithelium and it is responsible for host defense against microbial infections by generating ROS (reactive oxygen species). NOX1 is activated by two regulatory cytosolic proteins that form a hetero-dimer, Noxo1 (NOX organizer 1) and Noxa1 (NOX activator 1). The interaction between Noxa1 and Noxo1 is critical for activating NOX1. However no structural studies for interaction between Noxa1 and Noxo1 has not been reported till date. Here, we studied the inter-molecular interaction between the SH3 domain of Noxa1 and Noxo1 using pull-down assay and NMR spectroscopy. 15 N/ 13 C-labeled SH3 domain of Noxa1 has been purified for hetero-nuclear NMR experiments (HNCACB, CBCACONH, HNCA, HNCO, and HSQC). TALOS analysis using backbone assignment data of the Noxa1 SH3 domain showed that the structure primarily consists of β-sheets. Data from pull-down assay between the Noxo1 and Noxa1 showed that the SH3 domains (Noxa1) is responsible for interaction with Noxo1 C-terminal tail harboring proline rich region (PRR). The concentration-dependent titration of the Noxo1 C-terminal tail to Noxa1 shows that Noxo1 particularly in the RT loop: Q407*, H408, S409, A412*, G414*, E416, D417, L418, and F420; n-Src loop: C430, E431*, V432*, A435, W436, and L437; and terminal region: I447; F448*, F452* and V454 interact with Noxa1. Our results will provide a detailed understanding for interaction between Noxa1 and Noxo1 at the molecular level, providing insights into their cytoplasmic activity-mediated functioning as well as regulatory role of C-terminal tail of Noxo1 in the NOX1 complex. Highlights ? C-terminal of Noxo1 harboring PRR motif is important for Noxa1 interaction. ? Noxa1 SH3 binds C-terminal region of Noxo1with K d of 8.2?±?1.41?μM. ? Data from NMR experiments determined secondary structures of Noxa1 SH3. ? Noxa1 interacts with PRR region of Noxo1, however, binding affinity is weaker than C-terminal tail of Noxo1. ? Our results provide insights into regulatory role of C-terminal tail of Noxo1 in the NOX1 complex. ]]>
机译:摘要类似于吞噬细胞NADPH氧化酶的NOx1(NADPH氧化酶),主要在结肠上皮中表达,并通过产生ROS(反应性氧物质)对微生物感染的宿主防御负责。 NOx1由两种调节细胞溶质蛋白质激活,其形成杂二聚,NOXO1(NOx组织器1)和NOXA1(NOx活化剂1)。 NOXA1和NOXO1之间的相互作用对于激活NOx1至关重要。然而,迄今尚未报告NOXA1和NOXO1之间的相互作用的结构研究。这里,我们使用下拉测定和NMR光谱研究NOXA1和NOXO1的SH3结构域之间的分子间相互作用。已纯化15n / 13 C标记的NOxa1的SH3结构域,用于杂环NMR实验(HNCACB,CBCACONH,HNCA,HNCO和HSQC)。使用NOXA1 SH3结构域的骨干分配数据的TALOS分析表明,该结构主要由β-薄片组成。来自NOXO1和NOXA1之间的下拉测定的数据表明,SH3结构域(NOXA1)是负责与NOXO1 C末端尾部的相互作用,覆盆富含脯氨酸区(PRR)。 NOXO1 C末端尾部至NOXA1的浓度依赖性滴定表明NOXO1特别是在RT环中:Q407 *,H408,S409,A412 *,G414 *,E416,D417,L418和F420; N-SRC环:C430,E431 *,V432 *,A435,W436和L437;和终端区域:I447; F448 *,F452 *和V454与NOXA1相互作用。我们的结果将详细了解NOXA1和NOXO1之间的分子水平之间的相互作用,提供了对其细胞质活性介导的功能的见解以及NOx1复合物中NOXO1的C末端尾的调节作用。强调 ? NOXO1窝藏PRR主题的C末端对于NOXA1相互作用非常重要。还NOXA1 SH3绑定NOxo1的C末端区域,k d为8.2≤≤1.1.41≤1.41μm。还来自NMR实验的数据确定NOXA1 SH3的二次结构。还NOXA1与NOXO1的PRR区相互作用,然而,结合亲和力比NOXO1的C末端尾弱。还我们的结果提供了NOX1复合物中NOXO1的C末端尾部的监管作用的见解。 ]]>

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