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顺二氯二氨铂处理的雄性大鼠肝和肾微粒体中细胞色素P450同工酶含量的变化

Changes in content of P450 isozymes in hepatic and renal microsomes of the male rat treated with cis-diamminedichloroplatinum.

作者信息

Ohishi N, Imaoka S, Funae Y

机构信息

Laboratory of Chemistry, Osaka City University Medical School, Japan.

出版信息

Xenobiotica. 1994 Sep;24(9):873-80. doi: 10.3109/00498259409043286.

DOI:10.3109/00498259409043286
PMID:7810169
Abstract
  1. The changes in the activity of drug-metabolizing enzymes and in the content of P450 isozymes in renal and hepatic microsomes after treatment of the male Sprague-Dawley rat with cis-diamminedichloroplatinum (Cisplatin, CDDP) were examined. 2. NADPH-P450 reductase activity in renal microsomes was significantly increased by treatment with CDDP, but lauric acid omega- and (omega-1)-hydroxylation activities of renal microsomes were not increased. 3. The level of P4502C23 was increased significantly and levels of P4504A2 and 4A8 tended to increase in renal microsomes. 4. In hepatic microsomes, lauric acid omega-hydroxylation activity was increased, but (omega-1)-hydroxylation activity was not. Levels of P4502C11 and 3A2, which are male-specific forms, were decreased, whereas levels of P4502A1, 2C7 and 2E1 were increased in hepatic microsomes. The levels of P4504A2 and 4A3 were increased by CDDP and the level of P4504A1 was not changed. Changes in the protein levels of P450 by CDDP were consistent with those in the mRNA levels reported previously (LeBlanc et al. 1992). 5. Male-specific forms in rat liver such as P4502C11 were decreased by CDDP, but those in the kidney such as P4504A2 was not. Therefore, CDDP has different influences on the regulation of hepatic and renal P450s.
摘要
  1. 研究了用顺二氨二氯铂(顺铂,CDDP)处理雄性Sprague-Dawley大鼠后,其肾和肝微粒体中药物代谢酶活性及P450同工酶含量的变化。2. 用CDDP处理后,肾微粒体中NADPH-P450还原酶活性显著增加,但肾微粒体中月桂酸ω-和(ω-1)-羟化活性未增加。3. 肾微粒体中P4502C23水平显著升高,P4504A2和4A8水平有升高趋势。4. 在肝微粒体中,月桂酸ω-羟化活性增加,但(ω-1)-羟化活性未增加。雄性特异性形式的P4502C11和3A2水平降低,而肝微粒体中P4502A1、2C7和2E1水平升高。CDDP使P4504A2和4A3水平升高,P4504A1水平未改变。CDDP引起的P450蛋白水平变化与先前报道的mRNA水平变化一致(LeBlanc等人,1992年)。5. 大鼠肝脏中的雄性特异性形式如P4502C11被CDDP降低,但肾脏中的如P4504A2未被降低。因此,CDDP对肝和肾P450的调节有不同影响。

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