EPR studies of wild‐type and several mutants of cytochrome c oxidase from Rhodobacter sphaeroides: Glu286 is not a bridging ligand in the cytochrome a 3‐CuB center

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EPR studies of wild‐type and several mutants of cytochrome c oxidase from Rhodobacter sphaeroides: Glu286 is not a bridging ligand in the cytochrome a 3‐CuB center

机译：EPR研究球形红球菌野生型和几种细胞色素C氧化酶突变体：Glu286不是3–CuB中心细胞色素中的架桥配体

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>Wild-type and several mutants of cytochrome c oxidase from Rhodobacter sphaeroides were characterized by EPR spectroscopy. A pH-induced g12 signal, seen previously in mammalian cytochrome oxidase and assigned to the presence of a bridging car☐yl ligand in the bimetallic cytochrome a ₃-Cu_B site, is found also in the bacterial enzyme. Mutation of glutamate-286 to glutamine inactivates the enzyme but does not affect this signal, demonstrating that the car☐yl group of this residue is not the bridging ligand. Three mutants, M106Q, located one helix turn below a histidine ligand to cytochrome a, and T352A as well as F391Q, located close to the bimetallic center, are shown to affect dramatically the low-spin heme signal of cytochrome a. These mutants are essentially inactive, suggesting that these three mutations result in alterations to cytochrome a that render the oxidase non-functional.

机译：利用EPR光谱法鉴定了 sphaeroides 的>野生型和几种细胞色素 c 氧化酶突变体。 pH诱导的 g 12信号，先前在哺乳动物细胞色素氧化酶中观察到，并被指定为双金属细胞色素 a _{3 <在细菌酶中也发现了/ sub> -Cu _{B 位点。谷氨酸286突变为谷氨酰胺会使酶失活，但不影响该信号，表明该残基的car☐yl不是桥联配体。三个突变体M106Q位于细胞色素 a 的组氨酸配体下方一个螺旋圈处，并且位于双金属中心附近的T352A和F391Q显着影响了低血红素血红素信号。细胞色素 a 。这些突变体基本上是无活性的，表明这三个突变导致细胞色素 a 发生改变，从而使氧化酶失去功能。}} 展开▼

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《FEBS Letters》 |1995年第3期|共页

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中图分类分子生物学;

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1. Microscopic pKa Analysis of Glu286 in Cytochrome c Oxidase (Rhodobacter sphaeroides): Toward a Calibrated Molecular Model [J] . Nilanjan Ghosh Xavier Prat-Resina M. R. Gunner and Qiang Cui Biochemistry . 2009,第11期

机译：细胞色素C氧化酶（球形红球菌）中Glu286的微观pKa分析：建立校正的分子模型

2. The roles of Rhodobacter sphaeroides copper chaperones PCu AC and Sco (PrrC) in the assembly of the copper centers of the aa 3-type and the cbb 3-type cytochrome c oxidases [J] . ThompsonA.K., GrayJ., LiuA., Biochimica et biophysica acta. Bioenergetics . 2012,第6期

机译：球形球形红细菌铜伴侣PCu AC和Sco（PrrC）在aa 3型和cbb 3型细胞色素c氧化酶的铜中心组装中的作用

3. Differential effects of glutamate-286 mutations in the aa(3)-type cytochrome c oxidase from Rhodobacter sphaeroides and the cytochrome bo(3) ubiquinol oxidase from Escherichia coli. [J] . Egawa T, Ganesan K, Lin MT, Biochimica et biophysica acta. Bioenergetics . 2011,第10期

机译：球形红球菌aa（3）型细胞色素c氧化酶中的谷氨酸286突变与大肠杆菌中细胞色素bo（3）泛醇氧化酶的差异。

4. Relationship Between Coenzyme Q_(10) Synthesis and Cytochrome Accumulation in Rhodobacter sphaeroides 2.4.1 [C] . Penghao Li, Dan Gao, Junqian Gao, International conference on applied biotechnology . 2018

机译：球形红球菌中辅酶Q_（10）的合成与细胞色素积累的关系2.4.1

5. Studies on critical proton pathway residues in the AA3-type cytochrome c oxidase from Rhodobacter sphaeroides. [D] . Ganesan, Krithika. 2009

机译：球形球形红球菌AA3型细胞色素c氧化酶中关键质子途径残基的研究。

6. The roles of Rhodobacter sphaeroides copper chaperones PCuAC and Sco (PrrC) in the assembly of the copper centers of the aa3-type and the cbb3-type cytochrome c oxidases [O] . Audie K. Thompson, Jimmy Gray, Aimin Liu, -1

机译：乳头杆菌铜兼铜蛋白胶囊PCUAC和SCO（PRRC）的作用在AA3型和CBB3型细胞色素C氧化酶的组装中

7. EPR studies of wild-type and several mutants of cytochrome c oxidase from Rhodobacter sphaeroides: Glu286 is not a bridging ligand in the cytochrome a3-CuB center [O] . Mitchell David M., Aasa Roland, Ädelroth Pia, 1995

机译：EPR研究球形红球菌的野生型和几种细胞色素c氧化酶突变体：Glu286在细胞色素a3-CuB中心不是桥接配体

1. 用组氨酸取代细胞色素C中苯丙氨酸-82所得的突变体的结构和电化学性研究 [C] . 邢巍 ,郑军伟 ,陆天虹 . 第十届全国电化学会议 . 1999

2. 嗜酸氧化亚铁硫杆菌中细胞色素c氧化酶的表达纯化及IscR蛋白的定点突变研究 [A] . 张晓健 . 2009

1. Mutant type 3-hydroxybutyrate dehydrogenase from Rhodobacter sphaeroides and method for containing it [P] . 外国专利： JP6989528B2 . 2022-01-05

机译：突变体型3-羟基丁酯脱氢酶，来自乳氏菌氏菌氏菌和含它的方法

2. MUTANT CYTOCHROME OXIDASE P450CAM [P] . 外国专利： NZ294904A . 1998-09-24

机译：突变型细胞色素氧化酶P450CAM

3. Processes for detecting the presence of alzheimer's disease and mitochondrial origin in an individual and the genetic mutations that cause alzheimer's disease to inhibit the transcription or translation of genes and one or more nucleic acids encoding a mutant cytochrome c oxidase to selectively introduce a conjugated molecule in mitochondria to build a cell line to evaluate a compound for potential utility in the diagnosis of disorders in the treatment of a disorder and in the diagnosis or treatment of diabetes mellitus to prepare a cibrid animal and to determine the presence of a human disease of origin mitochondrial isolated nucleotide sequences probe kit therapeutic composition ribozyme cell line and animal hybrid [P] . 外国专利： BR9507241A . 1997-09-16

机译：用于检测个体中阿尔茨海默氏病和线粒体起源的存在的方法以及导致阿尔茨海默氏病抑制基因和一种或多种编码突变型细胞色素C氧化酶的核酸的转录或翻译的遗传突变，以选择性地将共轭分子引入线粒体建立一种细胞系，以评估该化合物在疾病诊断，疾病治疗以及糖尿病的诊断或治疗中的潜在效用，从而制备出纤巧的动物并确定是否存在人源性线粒体疾病核苷酸序列探针试剂盒治疗组合物核酶细胞系和动物杂种

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EPR studies of wild‐type and several mutants of cytochrome c oxidase from Rhodobacter sphaeroides: Glu286 is not a bridging ligand in the cytochrome a 3‐CuB center

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