Cytochrome <Emphasis Type='Italic'>b</Emphasis> <Subscript>5</Subscript> plays a dual role in the reaction cycle of cytochrome P450 3A4 during oxidation of the anticancer drug ellipticine

Marie Stiborová; Radek Indra; Eva Frei; Kate?ina Kope?ková; Heinz H. Schmeiser; Tomá? Eckschlager; Vojtěch Adam; Zbyněk Heger; Volker M. Arlt; Václav Martínek

首页> 外文期刊>Monatshefte fur Chemie >Cytochrome b 5 plays a dual role in the reaction cycle of cytochrome P450 3A4 during oxidation of the anticancer drug ellipticine

【24h】

Cytochrome b 5 plays a dual role in the reaction cycle of cytochrome P450 3A4 during oxidation of the anticancer drug ellipticine

机译：细胞色素<重点类型=“斜体”> B <下标> 5 在抗癌药物椭圆型氧化过程中在细胞色素P450 3A4的反应循环中发挥双重作用

获取原文

获取原文并翻译 | 示例

掌桥外文数据库（机构版） >>

开具论文收录证明 >>

文献代查 >>

页面导航

摘要
著录项
相似文献
相关主题

摘要

AbstractEllipticine is an anticancer agent that forms covalent DNA adducts after enzymatic activation by cytochrome P450 (CYP) enzymes, mainly by CYP3A4. This process is one of the most important ellipticine DNA-damaging mechanisms for its antitumor action. Here, we investigated the efficiencies of human hepatic microsomes and human recombinant CYP3A4 expressed with its reductase, NADPH:CYP oxidoreductase (POR), NADH:cytochromeb5reductase and/or cytochromeb5in Supersomes? to oxidize this drug. We also evaluated the effectiveness of coenzymes of two of the microsomal reductases, NADPH as a coenzyme of POR, and NADH as a coenzyme of NADH:cytochromeb5reductase, to mediate ellipticine oxidation in these enzyme systems. Using HPLC analysis we detected up to five ellipticine metabolites, which were formed by human hepatic microsomes and human CYP3A4 in the presence of NADPH or NADH. Among ellipticine metabolites, 9-hydroxy-, 12-hydroxy-, and 13-hydroxyellipticine were formed by hepatic microsomes as the major metabolites, while 7-hydroxyellipticine and the ellipticineN2-oxide were the minor ones. Human CYP3A4 in Supersomes? generated only three metabolic products, 9-hydroxy-, 12-hydroxy-, and 13-hydroxyellipticine. Using the32P-postlabeling method two ellipticine-derived DNA adducts were generated by microsomes and the CYP3A4-Supersome system, both in the presence of NADPH and NADH. These adducts were derived from the reaction of 13-hydroxy- and 12-hydroxyellipticine with deoxyguanosine in DNA. In the presence of NADPH or NADH, cytochromeb5stimulated the CYP3A4-mediated oxidation of ellipticine, but the stimulation effect differed for individual ellipticine metabolites. This heme protein also stimulated the formation of both ellipticine-DNA adducts. The results demonstrate that cytochromeb5plays a dual role in the CYP3A4-catalyzed oxidation of ellipticine: (1) cytochromeb5mediates CYP3A4 catalytic activities by donating the first and second electron to this enzyme in its catalytic cycle, indicating that NADH:cytochromeb5reductase can substitute NADPH-dependent POR in this enzymatic reaction and (2) cytochromeb5can act as an allosteric modifier of the CYP3A4 oxygenase.Graphical abstract

]]>

机译：<！[cdata [ <标题>抽象 ara id =“par1”> ellipticine是一种抗癌剂，其在通过细胞色素p450（cyp）酶酶活化后形成共价DNA加合物，主要由CYP3A44。该过程是其抗肿瘤作用最重要的烯晶型DNA损伤机制之一。在这里，我们研究了用其还原酶表达的人肝微粒体和人重组CYP3A4的效率，NADPH：CYP氧化还原酶（POR），NADH：细胞色素<重点型=“斜体”> B <下标> 5 还原酶和/或细胞色素<重点类型=“斜体”> B <下标> 5 在超镜中？氧化这种药物。我们还评估了两种微粒体还原酶的辅酶的有效性，NADPH作为POR的辅酶，以及NADH作为NADH的辅酶：细胞色素<重点型=“斜体”> B <下标> 5 还原酶，在这些酶系统中介导烯晶氧化。使用HPLC分析，我们检测到最多五种椭圆形代谢物，其在NADPH或NADH存在下由人肝微粒体和人CYP3A4形成。在椭圆形代谢物中，通过肝微粒体作为主要代谢物形成9-羟基 - ，12-羟基 - 和13-羟基晶体，而7-羟基纤维素和椭圆形<重点型=“斜体”> N <上标> 2 - 氧化物是次要的。在超级瘤中的人类CYP3A4？仅产生三种代谢产物，9-羟基，12-羟基 - 和13-羟基晶体。使用<上标> 32 p-后标记方法，通过微粒体和CYP3A4-超组系统产生两种椭圆形衍生的DNA加合在NADPH和NADH的存在下。这些加合物衍生自13-羟基和12-羟基硫胺与DNA中的脱氧核苷酸的反应。在存在NADPH或NADH的存在下，细胞色素<重点型=“斜体”> B <下标> 5 刺激CYP3A4介导的椭圆形氧化，但刺激效果不同于单个椭圆形代谢物。该血红蛋白还刺激了椭圆形-DNA加合物的形成。结果表明，细胞色素<重点型=“斜体”> B <下标> 5 在椭圆形的CYP3A4催化氧化中发挥双重作用：（1）细胞色素<重点类型=“斜体” > B <下标> 5 通过将第一和第二电子在其催化循环中向该酶送入该酶来介导CYP3A4催化活性，表明NADH：细胞色素<重点型=“斜体”> B <下标> 5 还原酶可以在该酶促反应中替代NADPH依赖性POR，（2）细胞色素<重点类型=“斜体”> B <下标> 5 可以充当CYP3A4氧酶的变构改性剂。 <标题> <标题>图形抽象 ara id =“par2”> <图类别=“标准“float =”no“id =”figa“> ]]>

著录项

来源
《Monatshefte fur Chemie》 |2017年第11期|共9页
作者
Marie Stiborová; Radek Indra; Eva Frei; Kate?ina Kope?ková; Heinz H. Schmeiser; Tomá? Eckschlager; Vojtěch Adam; Zbyněk Heger; Volker M. Arlt; Václav Martínek;
展开▼
作者单位

Department of Biochemistry Faculty of Science Charles University;

Department of Biochemistry Faculty of Science Charles University;

Department of Biochemistry Faculty of Science Charles University;

Department of Oncology 2nd Faculty of Medicine Charles University and University Hospital Motol;

Division of Radiopharmaceutical Chemistry German Cancer Research Center (DKFZ);

Department of Pediatric Hematology and Oncology 2nd Medical Faculty Charles University and University Hospital Motol;

Laboratory of Metallomics and Nanotechnology Department of Chemistry and Biochemistry Mendel University in Brno;

Laboratory of Metallomics and Nanotechnology Department of Chemistry and Biochemistry Mendel University in Brno;

Analytical and Environmental Sciences Division MRC-PHE Centre for Environment and Health King’s College London;

Department of Biochemistry Faculty of Science Charles University;

展开▼
收录信息
原文格式 PDF
正文语种 eng
中图分类化学;
关键词
DNA; Enzymes; Coenzymes; High pressure liquid chromatography;

机译：DNA;酶;辅酶;高压液相色谱;

相似文献

外文文献
中文文献
专利

1. Cytochrome b 5 plays a dual role in the reaction cycle of cytochrome P450 3A4 during oxidation of the anticancer drug ellipticine [J] . Marie Stiborová, Radek Indra, Eva Frei, Monatshefte fur Chemie . 2017,第11期

机译：细胞色素<重点类型=“斜体”> B <下标> 5 在抗癌药物椭圆型氧化过程中在细胞色素P450 3A4的反应循环中发挥双重作用
2. One-loop γγ?→? W L + W L ? and γγ → Z L Z L from the Electroweak Chiral Lagrangian with a light Higgs-like scalar [J] . R. L. Delgado, A. Dobado, M. J. Herrero, The journal of high energy physics . 2014,第7期

机译：单环<重点类型=“斜体”>γγ？→？ <重点类型=“斜体”> W <重点类型=“斜体”> l + <重点type =“斜体”> w <重点类型=“italic”> l ？和<重点类型=“斜体”>γγ→<重点类型=“斜体”> z <重点类型=“斜体”> l z <下标> <重点类型=”斜体“> l 从Electroweak手性拉格朗日，带有轻的HIGGS样标量
3. 1 – x Ca x CoO 3 – δ Perovskites ( х = 0?1) Prepared by the Pechini Method in the Reaction of Deep Methane Oxidation]]> [J] . L. A. Isupova, N. A. Kulikovskaya, N. F. Saputina, Kinetics and catalysis . 2018,第4期

机译：<！[cdata [la 1 - x ca <重点类型=“斜体”> x COO <下标> 3 - Δ蠕动（<强调型=“斜体”>х =0≤1）在深甲烷氧化反应中由Pechini方法制备]]>
4. Molecular Mechanism of Herbicide Resistance with Special Emphasis on Cytochrome P450 Monooxygenases [C] . Hideo Ohkawa, Hiromasa Imaishi, Noriaki Shiota, 9th Japan-China Symposium on Pesticide Science October 26-28, 1998 Tian Jin China . 1998

机译：细胞色素P450单加氧酶特别强调除草剂抗性的分子机制
5. Part I. Synthesis of cytochrome P450-CAM substrate analogues towards developing cytochrome P450-CAM as an enzyme-based model system for mechanistic studies of important types of P450 reactions. Part II. Diels-Alder approach towards the synthesis of 2,3-disubstituted anthracene derivatives for luminescence spectroscopy characterization: Synthesis towards fluorescent sensors. [D] . Kemnitzer, William Edward. 1998

机译：第一部分。合成细胞色素P450-CAM底物类似物，以开发细胞色素P450-CAM作为一种基于酶的模型系统，用于重要类型P450反应的机理研究。第二部分Diels-Alder合成2,3-二取代蒽衍生物以进行发光光谱表征的方法：合成荧光传感器。
6. Cytochrome b5 plays a dual role in the reaction cycle of cytochrome P450 3A4 during oxidation of the anticancer drug ellipticine [O] . Marie Stiborová, Radek Indra, Eva Frei, -1

机译：细胞色素b5在抗癌药玫瑰树碱的氧化过程中对细胞色素P450 3A4的反应周期起双重作用
7. Cytochrome b₅ plays a dual role in the reaction cycle of cytochrome P450 3A4 during oxidation of the anticancer drug ellipticine [O] . Stiborová, Marie, Indra, Radek, Frei, Eva, 2017

机译：细胞色素b _{5 在抗癌药物玫瑰树碱氧化过程中对细胞色素P450 3A4的反应周期起双重作用}

Cytochrome b 5 plays a dual role in the reaction cycle of cytochrome P450 3A4 during oxidation of the anticancer drug ellipticine

摘要

著录项

相似文献

相关主题

期刊订阅