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吲哚醌EO9:经DT-黄递酶或黄嘌呤氧化酶还原后形成DNA链间交联。

Indoloquinone EO9: DNA interstrand cross-linking upon reduction by DT-diaphorase or xanthine oxidase.

作者信息

Maliepaard M, Wolfs A, Groot S E, de Mol N J, Janssen L H

机构信息

Department of Pharmaceutical Chemistry, Faculty of Pharmacy, Utrecht University, The Netherlands.

出版信息

Br J Cancer. 1995 Apr;71(4):836-9. doi: 10.1038/bjc.1995.161.

Abstract

We report DNA interstrand cross-linking caused by the anti-tumour indoloquinone EO9 following reductive activation with purified rat liver DT-diaphorase or xanthine oxidase. Reduction was a necessary event for cross-linking to occur. DNA cross-link formation by EO9 following DT-diaphorase reduction was completely inhibited by addition 10 microM dicoumarol, whereas only a minor effect of dicoumarol on xanthine oxidase-mediated DNA cross-linking by EO9 was observed. DNA cross-linking was pH dependent, with increasing cross-link formation from pH 5.5 to 7.0 for both DT-diaphorase and xanthine oxidase mediated reactions. Also, conversion of EO9 upon reduction was pH dependent. However, in contrast to DNA cross-linking, conversion rates of EO9 decreased at higher pH. EO9 was shown to be more efficient in DNA cross-linking than mitomycin C under identical conditions, using both DT-diaphorase and xanthine oxidase reductive activation at pH 5.5 and 7.0. This study indicates that the anti-tumour activity of EO9 may be at least partly mediated by interstrand DNA cross-link formation, and that various reducing enzymes may be important for activation of EO9 in vitro and in vivo.

摘要

我们报道了用纯化的大鼠肝脏DT-黄递酶或黄嘌呤氧化酶进行还原激活后,抗肿瘤吲哚醌EO9所引起的DNA链间交联。还原是交联发生的必要条件。在DT-黄递酶还原后,加入10微摩尔的双香豆素可完全抑制EO9引起的DNA交联形成,而双香豆素对黄嘌呤氧化酶介导的EO9 DNA交联仅产生轻微影响。DNA交联依赖于pH值,在DT-黄递酶和黄嘌呤氧化酶介导的反应中,从pH 5.5到7.0,交联形成均增加。此外,还原时EO9的转化也依赖于pH值。然而,与DNA交联不同的是,EO9的转化率在较高pH值时降低。在相同条件下,使用DT-黄递酶和黄嘌呤氧化酶在pH 5.5和7.0下进行还原激活,结果表明EO9在DNA交联方面比丝裂霉素C更有效。本研究表明,EO9的抗肿瘤活性可能至少部分是由DNA链间交联形成介导的,并且各种还原酶可能对EO9在体外和体内的激活很重要。

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