Enhancement of the Binding of O-Ethyl O-p-Nitrophenyl Phenylphosphonate (EPNoxon) to Microsomal Carboxylesterase by NAD in vitro

Haruo KITAGAWA; Koichi UENO; Masakiyo HOSOKAWA; Seiyu SUGIYAMA; Takashi IGARASHI; Tetsuo SATOH

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Enhancement of the Binding of O-Ethyl O-p-Nitrophenyl Phenylphosphonate (EPNoxon) to Microsomal Carboxylesterase by NAD in vitro

机译：NAD增强O-乙基O-对硝基苯基苯基膦酸酯（EPNoxon）与微粒体羧酯酶的结合

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References(10) Cited-By(1) Inhibition of rat liver microsomal carboxylesterase(CEase) by O-ethyl O-p-nitrophenyl phenylphosphonothioate (EPN) and binding of EPN oxygen analog to microsomal CEase were enhanced by addition of NAD or NADP. This was more prominent in addition of NAD than NADP. No potentiation of anti-CEase action of EPN by NAD was seen when pure esterase (E.C. 3.1.1.1) instead of liver microsomes was used as an enzyme source. This effect of NAD in microsomal CEase was significantly decreased when N-ethylmaleimide or p-chloromercuribenzoic acid was added. From these findings, it is strongly suggested that NAD-mediated potentiation of the anti-CEase action of EPN might be attributed to the increase in formation of NADH from NAD by microsomal dehydrogenase(s) containing a sulfhydryl group, leading to a subsequent increase in formation of the EPN oxygen analog from EPN, and in turn, CEase inhibition was enhanced.

机译：参考文献（10）（1）通过添加NAD或NADP增强了O-乙基-对硝基苯基苯基硫代磷酸酯（EPN）对大鼠肝微粒体羧酸酯酶（CEase）的抑制作用以及EPN氧类似物与微粒体CEase的结合。除NAD外，这比NADP更突出。当使用纯酯酶（E.C. 3.1.1.1）代替肝微粒体作为酶源时，没有发现NAD增强EPN的抗CEase作用。当添加N-乙基马来酰亚胺或对氯巯基苯甲酸时，NAD在微粒体CEase中的作用显着降低。从这些发现中，强烈建议NAD介导的EPN的抗CEase作用增强可能归因于含有巯基的微粒体脱氢酶从NAD形成NADH的增加，从而导致NDH的增加。由EPN形成EPN氧类似物，进而增强了CEase抑制作用。

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《Japanese Journal of Pharmacology》 |1985年第1期|共页
作者
Haruo KITAGAWA; Koichi UENO; Masakiyo HOSOKAWA; Seiyu SUGIYAMA; Takashi IGARASHI; Tetsuo SATOH;
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1. NAD-Coupled Enzymatic Oxidation of O-Ethyl O-p-Nitrophenyl Phenylphosphonothioate (EPN) to Its Oxygen Analog with Liver Microsomes of Rats [J] . Haruo KITAGAWA, Koichi UENO, Seiyu SUGIYAMA, Japanese Journal of Pharmacology . 1985,第3期

机译：大鼠肝脏微粒体的NAD偶联O-乙基O-对硝基硝基苯苯基硫代磷酸酯（EPN）的酶氧化
2. Identification of the NADP(H) binding site of rat liver microsomal 5 alpha-reductase (isozyme-1): purification of a photolabeled peptide corresponding to the adenine binding domain. [J] . Bhattacharyya AK, Chavan AJ, Haley BE, Biochemistry . 1995,第11期

机译：大鼠肝微粒体5α-还原酶（isozyme-1）的NADP（H）结合位点的鉴定：对应于腺嘌呤结合域的光标记肽的纯化。
3. Addressing in silico-in vitro-in vivo correlation (ISIVIVC) gaps for intrinsic clearance: in silico and in vitro assessment of microsomal binding (FUMIC) to improve prediction of in vivo pharmacokinetics [J] . Joshi Elizabeth M., Katwaru Ravi, Harradine Paul, Drug Metabolism Reviews . 2016,第1a4期

机译：解决内部固有清除的计算机模拟-体外-体内相关性（ISIVIVC）差距：微粒子结合（FUMIC）的计算机模拟和体外评估，以改善对体内药代动力学的预测
4. In vitro DNA-binding studies of cyclic AMP responsive element binding protein and CCAAT/enhancer binding protein beta. [D] . Popova, Katerina. 2004

机译：环状AMP响应元件结合蛋白和CCAAT /增强子结合蛋白β的体外DNA结合研究。
5. Binding of diethylstilboestrol to deoxyribonucleic acid by rat liver microsomal fractions in vitro and in mouse foetal cells in culture. [O] . G M Blackburn, M H Thompson, H W King 1976

机译：在体外和培养的小鼠胎儿细胞中大鼠肝脏微粒体组分使二乙基雌二醇与脱氧核糖核酸结合。
6. The Hydrolysis of O-ethyl O-p-nitrophenyl Phenylphosphonates [O] . Yasukazu URA, Yoshiharu MORI, Gozyo SAKATA 1973

机译：O-乙基O-P-硝基苯基苯膦酸盐的水解

Enhancement of the Binding of O-Ethyl O-p-Nitrophenyl Phenylphosphonate (EPNoxon) to Microsomal Carboxylesterase by NAD in vitro

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