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Binding of imidazole 1-methylimidazole and 4-nitroimidazole to yeast cytochrome c peroxidase (CcP) and the distal histidine mutant CcP(H52L)

机译：咪唑1-甲基咪唑和4-硝基咪唑与酵母细胞色素c过氧化物酶（CcP）和远端组氨酸突变体CcP（H52L）的结合

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摘要

Imidazole, 1-methylimidazole and 4-nitroimidazole bind to yeast cytochrome c peroxidase (yCcP) with apparent equilibrium dissociation constants (

K_{D}^{app}

) of 3.3 ± 0.4, 0.85 ± 0.11, and ~0.2 M, respectively, at pH 7. This is the weakest imidazole binding to a heme protein reported to date and it is about 120 times weaker than imidazole binding to metmyoglobin. Spectroscopic changes associated with imidazole and 1-methylimidazole binding to yCcP suggest partial ionization of bound imidazole to imidazolate. The pKa for ionization of bound imidazole is estimated to be 7.4 ± 0.2, about 7 units lower than that of free imidazole and about 3 units lower than imidazole bound to metmyoglobin. Equilibrium binding of imidazole to CcP(H52L) is biphasic with low- and high-affinity phases having

K_{D}^{app}

values of 9.5 ± 4.5 and 0.13 ± 0.04 M, respectively. CcP(H52L) binding of 1-methylimidazole is monophasic with an affinity similar to those of yCcP and rCcP. Binding of 1-methylimidazole to rCcP is associated with two kinetic phases, the initial binding complete within 10 s, followed by a process that is consistent with 1-methylimidazole binding to a cavity created by movement of Trp-191 from the interior of the protein to the surface. Both the equilibrium binding and kinetics of 1-methylimidazole binding to yCcP are pH dependent. yCcP has a four-fold increase in 1-methylimidazole binding affinity on decreasing the pH from 7.5 to 4.0, an observation that is unique among the many studies on binding of imidazole and imidazole derivatives to heme proteins.

机译：咪唑，1-甲基咪唑和4-硝基咪唑以明显的平衡解离常数与酵母细胞色素c过氧化物酶（yCcP）结合（ <行> K D app ）在pH 7时分别为3.3±0.4、0.85±0.11和〜0.2M。这是与咪唑结合最弱的迄今为止报道的一种血红素蛋白，它的强度比咪唑与肌红蛋白的结合弱120倍。与咪唑和1-甲基咪唑与yCcP结合相关的光谱变化表明，结合的咪唑部分电离为咪唑化物。用于结合的咪唑的离子化的pKa估计为7.4±0.2，比游离的咪唑的pKa低约7个单位，比与结合的肌红蛋白结合的咪唑的pKa低约3个单位。咪唑与CcP（H52L）的平衡结合是两相的，具有低亲和力和高亲和力相，具有

KD应用值分别为9.5±4.5和0.13±0.04M。 1-甲基咪唑的CcP（H52L）结合是单相的，其亲和力类似于yCcP和rCcP。 1-甲基咪唑与rCcP的结合与两个动力学阶段有关，初始结合在10 s内完成，随后的过程与1-甲基咪唑与Trp-191从蛋白质内部运动产生的腔相结合到表面。 1-甲基咪唑与yCcP的平衡结合和动力学均取决于pH。 yCcP在将pH从7.5降低至4.0时，1-甲基咪唑的结合亲和力增加了四倍，这一发现在许多关于咪唑和咪唑衍生物与血红素蛋白结合的研究中是独一无二的。

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期刊名称 other
作者
James E. Erman; Diana Chinchilla; Jason Studer; Lidia B. Vitello;
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年(卷),期 -1(1854),8
年度 -1
页码 869–881
总页数 43
原文格式 PDF
正文语种
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关键词
Cytochrome c Peroxidase CcP(H52L) Imidazole 1-Methylimidazole 4-Nitroimidazole;

机译：细胞色素c过氧化物酶;CcP（H52L）;咪唑;1-甲基咪唑;4-硝基咪唑;

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专利

1. Binding of imidazole, 1-methylimidazole and 4-nitroimidazole to yeast cytochrome c peroxidase (CcP) and the distal histidine mutant, CcP(H52L) [J] . Erman James E., Chinchilla Diana, Studer Jason, Biochimica et biophysica acta: BBA: International journal of biochemistry, biophysics and molecular biololgy. Proteins and Proteomics . 2015,第8期

机译：咪唑，1-甲基咪唑和4-硝基咪唑与酵母细胞色素C过氧化物酶（CcP）和远端组氨酸突变体CcP（H52L）的结合
2. Relocation of the Distal Histidine in Cytochrome c Peroxidase: Properties of CcP(W51H), CcP(W51H/H52W), and CcP(W51H/H52L) [J] . Miriam C. Foshay Lidia B. Vitello and James E. Erman Biochemistry . 2009,第23期

机译：细胞色素c过氧化物酶中远端组氨酸的重定位：CcP（W51H），CcP（W51H / H52W）和CcP（W51H / H52L）的性质
3. Apolar distal pocket mutants of yeast cytochrome c peroxidase: Binding of imidazole, 1-methylimidazole and 4-nitroimidazole to the triAla, triVal, and triLeu variants [J] . Bidwai Anil, Ayala Caitlan, Vitello Lidia B., Biochimica et biophysica acta: BBA: International journal of biochemistry, biophysics and molecular biololgy. Proteins and Proteomics . 2015,第8期

机译：酵母细胞色素c过氧化物酶的非极性远端口袋突变体：咪唑，1-甲基咪唑和4-硝基咪唑与triAla，triVal和triLeu变体的结合
4. REDUCTION POTENTIAL SHIFTS DUE TO ACTIVE SITE AND SURFACE MUTATIONS OF YEAST CYTOCHROME C PEROXIDASE [C] . C. M. DiCarlo, L. B. Vitello, J. E. Erman Electrochemical Society(ECS) Meeting;Symposium on Organic and Biological Electrochemistry General Oral and Poster Session; 20070506-11;20070506-10; Chicago,IL(US);Chicago,IL(US) . 2007

机译：由于酵母细胞色素C过氧化物酶的活性位点和表面突变，降低了潜在的迁移
5. Part I. Magnetic circular dichroism studies of cytochrome c peroxidase from yeast: Investigations of the active site heme coordination sphere through comparison with horseradish peroxidase and myoglobin. Part II. Examination of the heme active site coordination structure of the cavity mutants of myoglobin (H93G), cytochrome c peroxidase (H175G), and heme oxygenase (H25A) and structural investigation of thiolate-ligated cytochrome c peroxidase in the H17C/D235L double mutant. [D] . Pond, Alycen Easterling. 1999

机译：第一部分。酵母中细胞色素C过氧化物酶的磁性圆二色性研究：通过与辣根过氧化物酶和肌红蛋白的比较，研究了活性部位血红素配位域。第二部分检查肌红蛋白（H93G），细胞色素c过氧化物酶（H175G）和血红素加氧酶（H25A）的空腔突变体的血红素活性位点配位结构，以及H17C / D235L双突变体中硫醇盐连接的细胞色素c过氧化物酶的结构研究。
6. Apolar distal pocket mutants of yeast cytochrome c peroxidase: Binding of imidazole 1-methylimidazole and 4-nitroimidazole to the triAla triVal and triLeu variants [O] . Anil Bidwai, Caitlan Ayala, Lidia B. Vitello, -1

机译：酵母细胞色素C过氧化物酶的非极性远端口袋突变体：咪唑1-甲基咪唑和4-硝基咪唑与triAlatriVal和triLeu变体的结合
7. Binding of imidazole, 1-methylimidazole and 4-nitroimidazole to yeast cytochrome c peroxidase (CcP) and the distal histidine mutant, CcP(H52L) [O] . James E. Erman, Diana Chinchilla, Jason Studer, 2015

机译：咪唑，1-甲基咪唑和4-硝基咪唑至酵母细胞色素C过氧化物酶（CCP）和远端组氨酸突变体，CCP（H52L）的结合
8. Production and Characterization of Yeast Cytochrome C Antibodies; Immunological Studies of Mutants with Altered Cytochrome C Synthesis [R] . Matner, R. R. 1980

机译：酵母细胞色素C抗体的制备和鉴定;改变细胞色素C合成突变体的免疫学研究

Binding of imidazole 1-methylimidazole and 4-nitroimidazole to yeast cytochrome c peroxidase (CcP) and the distal histidine mutant CcP(H52L)

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