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首页> 外文期刊>Journal of pharmaceutical sciences. >Effects of glucose on the pharmacokinetics of intravenous chlorzoxazone in rats with acute renal failure induced by uranyl nitrate.
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Effects of glucose on the pharmacokinetics of intravenous chlorzoxazone in rats with acute renal failure induced by uranyl nitrate.

机译:葡萄糖对硝酸铀酰致急性肾功能衰竭大鼠静脉内氯唑沙宗药代动力学的影响。

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The effects of glucose on CYP2E1 expression in rats with acute renal failure induced by uranyl nitrate (U-ARF) have been reported. CYP2E1 was significantly induced (2.3-fold) in rats with U-ARF compared with that in control rats. In contrast, CYP2E1 expression was significantly decreased in rats with U-ARF supplied with glucose (dissolved in tap water to make 10%, w/v) in their drinking water for 5 days (U-ARFG) compared with that in rats with U-ARF. However, CYP2E1 in rats with U-ARFG was significantly greater than that in control rats. Chlorzoxazone (CZX) primarily undergoes hydroxylation, catalyzed mainly by CYP2E1, to form 6-hydroxychlorzoxazone (OH-CZX) rats. Hence, it could be expected that in rats with U-ARFG, formation of OH-CZX could significantly decrease and increase compared with those in rats with U-ARF and control rats, respectively. This expectation is proven by the following results of a study of intravenous administration of CZX at a dose 20 mg/kg to control rats and rats with U-ARF and U-ARFG. First, the total area under the plasma concentration-time curve from time zero to 8 h (AUC(0-8 h)) of OH-CZX in rats with U-ARFG (8730 microg x min/mL) was significantly greater than that in control rats (414 microg x min/mL) and significantly smaller than that in rats with U-ARF (11500 microg x min/mL). Second, the AUC(0-8 h, OH-CZX)/AUC(CZX) ratio in rats with U-ARFG (10.0) was significantly greater than that in control rats (0.252) and significantly smaller than that in rats with U-ARF (17.5). Finally, the in vitro intrinsic OH-CZX formation clearance (CL(int)) in rats with U-ARFG (27.9 mL/min/mg protein) was significantly slower than that in rats with U-ARF (36.7 mL/min/mg protein) and significantly faster than that in control rats (17.7 mL/min/mg protein).
机译:已报道葡萄糖对硝酸铀酰(U-ARF)诱导的急性肾衰竭大鼠CYP2E1表达的影响。 CYP2E1在U-ARF大鼠中被显着诱导(2.3倍),与对照组相比。与之相反,在U-ARF中补充葡萄糖(溶解于自来水中,使其水含量为10%,w / v)的U-ARF大鼠在饮水中5天(U-ARFG),CYP2E1表达显着降低。 -ARF。但是,U-ARFG大鼠的CYP2E1明显高于对照组。氯唑沙宗(CZX)主要经过CYP2E1催化的羟基化反应,形成6-羟基氯唑沙宗(OH-CZX)大鼠。因此,可以预料,与U-ARF大鼠和对照组相比,U-ARFG大鼠中OH-CZX的形成会明显减少和增加。通过以20 mg / kg的剂量静脉注射CZX来控制大鼠和U-ARF和U-ARFG的大鼠的以下研究结果证明了这一期望。首先,U-ARFG(8730 microg x min / mL)大鼠在OH-CZX零时至8 h(AUC(0-8 h))的血浆浓度-时间曲线下的总面积明显大于在对照组大鼠中为414 microg x min / mL,而在U-ARF组为11500 microg x min / mL。其次,U-ARFG大鼠(10.0)的AUC(0-8 h,OH-CZX)/ AUC(CZX)比值显着高于对照组(0.252),并且显着小于U-ARFG大鼠ARF(17.5)。最后,U-ARFG(27.9 mL / min / mg蛋白质)大鼠的体外固有OH-CZX形成清除(CL(int))明显慢于U-ARF(36.7 mL / min / mg)大鼠蛋白质),并且比对照组大鼠(17.7毫升/分钟/毫克蛋白质)快得多。

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