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Postnatal development of hepatic oxidative, hydrolytic and conjugative drug-metabolizing enzymes in female horses

机译:雌性马肝氧化,水解和结合药物代谢酶的产后发育

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Little is known about the effects of aging on the hepatic drug metabolizing capacity of horses despite the relatively long lifespan characterizing this species. A wide array of cytochrome P450 (CYP)-dependent monooxygenases, carboxylesterases and transferases were assayed in liver microsomes from 50 female horses in an age range between less than I year to over 12 years. Rather unexpectedly, both the CYP content and the activity of NADPH cytochrome c reductase rose as a function of age. Accordingly, a general increasing trend was recorded in the rate of the in vitro metabolism of the substrates reported to be related to CYP2B-, CYP2E- or CYP3A, although, as detected by Western immunoblotting, only the levels of proteins recognized by anti-rat CYP3A- and CYP2B antibodies appeared to increase consistently. Also the carboxylesterases and uridindiphosphoglucuronyl-transferase (UGT) activity toward 1-naphthol displayed a similar trend, glutathione S-transferase accepting 3,4-dichloronitrobenzene as a substrate being the only enzyme activity showing an age-related decline. A positive correlation was also found between liver cadmium content and CYP amount as well as the activities of most monooxygenases (except for those related to CYP1A), carboxylesterases, and UGT. While confirming that a number of enzyme activities are less expressed in foals, our results contradict the general view that the drug metabolizing capacity drops in elder individuals. Although several other factors can influence the kinetics of foreign compounds in aged animals, data from this study may provide insight in understanding possible age-related differences in drug efficacy and the response to toxic substances in horses. (C) 2003 Elsevier Inc. All rights reserved. [References: 52]
机译:尽管衰老对马的肝脏药物代谢能力的影响知之甚少,但人们对此知之甚少。在年龄不超过1岁至12岁以上的50匹雌马的肝微粒体中,分析了多种细胞色素P450(CYP)依赖性单加氧酶,羧酸酯酶和转移酶。出乎意料的是,CYP含量和NADPH细胞色素C还原酶的活性均随年龄增长。因此,据报道与CYP2B-,CYP2E-或CYP3A相关的底物的体外代谢速率记录了总体上升趋势,尽管如Western blot所检测,只有抗大鼠识别的蛋白质水平CYP3A和CYP2B抗体似乎持续增加。同样,针对1-萘酚的羧酸酯酶和尿素二磷酸葡糖醛糖醛酸转移酶(UGT)活性也显示出相似的趋势,谷胱甘肽S-转移酶接受3,4-二氯硝基苯作为底物,是唯一显示与年龄相关的下降的酶活性。肝镉含量和CYP量以及大多数单加氧酶(除与CYP1A相关的酶),羧酸酯酶和UGT的活性之间也发现正相关。虽然证实了小马驹中许多酶的活性较少表达,但我们的结果与老年人的药物代谢能力下降的普遍观点相矛盾。尽管其他几个因素也可能影响年老动物中外来化合物的动力学,但这项研究的数据可能有助于了解马匹中药物功效和对有毒物质的反应中可能与年龄有关的差异。 (C)2003 Elsevier Inc.保留所有权利。 [参考:52]

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