Sex differences in the pharmacokinetics, oxidative metabolism and oral bioavailability of oxycodone in the Sprague-Dawley rat.

Chan S; Edwards SR; Wyse BD; Smith MT

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Sex differences in the pharmacokinetics, oxidative metabolism and oral bioavailability of oxycodone in the Sprague-Dawley rat.

机译：Sprague-Dawley大鼠中羟考酮的药代动力学，氧化代谢和口服生物利用度方面的性别差异。

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1. The pharmacokinetics and oxidative metabolism of oxycodone were investigated following intravenous and oral administration in male and female Sprague-Dawley (SD) rats. 2. High-performance liquid chromatography (HPLC)-electrospray ionization (ESI)-tandem mass spectrometry (MS-MS) was used to quantify plasma concentrations of oxycodone and its oxidative metabolites noroxycodone and oxymorphone following administration of single bolus intravenous (5 mg/kg) and oral (10 mg/kg) doses of oxycodone. 3. The mean (+/-SEM) clearance of intravenous oxycodone was significantly higher in male than female SD rats (4.9 +/- 0.3 vs 3.1 +/- 0.3 L/h per kg, respectively; P < 0.01). Mean areas under the plasma concentration versus time curves (AUC) for oxycodone were significantly higher in female than male SD rats following intravenous (approximately 1.6-fold; P < 0.01) and oral (approximately sevenfold; P < 0.005) administration. 4. The oral bioavailability of oxycodone was low (at 1.2 and 5.0%, respectively) in maleand female SD rats, a finding consistent with high first-pass metabolism. Noroxycodone : oxycodone AUC ratios were significantly higher in male than female SD rats after intravenous (approximately 2.4-fold; P < 0.005) and oral (approximately 12-fold; P < 0.005) administration. 5. Circulating oxymorphone concentrations remained very low following both routes of administration. Noroxycodone : oxymorphone AUC ratios were greater in male than female SD rats after intravenous (approximately 13- and fivefold, respectively) and oral (approximately 90- and sixfold, respectively) administration. 6. Sex differences were apparent in the pharmacokinetics, oxidative metabolism and oral bioavailability of oxycodone. Systemic exposure to oxycodone was greater in female compared with male SD rats, whereas systemic exposure to metabolically derived noroxycodone was higher in male than female SD rats. 7. Oral administration of oxycodone to the SD rat is a poor model of the human for the study of the pharmacodynamic effects of oxycodone.

机译：1.在静脉内和口服给药后，对雄性和雌性Sprague-Dawley（SD）大鼠进行了羟考酮的药代动力学和氧化代谢研究。 2.使用高效液相色谱（HPLC）-电喷雾电离（ESI）-串联质谱（MS-MS）定量单次静脉推注（5 mg / ml）后羟考酮及其氧化代谢产物去甲羟考酮和羟吗啡酮的血浆浓度公斤）和口服（10毫克/公斤）剂量的羟考酮。 3.雄性SD大鼠的静脉内羟考酮的平均清除率（+/- SEM）显着高于雌性SD大鼠（分别为每公斤4.9 +/- 0.3对3.1 +/- 0.3 L / h; P <0.01）。雌性大鼠在静脉注射（约1.6倍; P <0.01）和口服（约7倍; P <0.005）后，羟考酮的血浆浓度-时间曲线下平均面积（AUC）明显高于雄性SD大鼠。 4.雄性和雌性SD大鼠中羟考酮的口服生物利用度较低（分别为1.2％和5.0％），这一发现与首过代谢较高有关。静脉（约2.4倍; P <0.005）和口服（约12倍; P <0.005）给药后，雄性SD大鼠中的去甲羟可待酮：羟考酮的AUC比率明显高于雌性SD大鼠。 5.两种给药途径中循环羟吗啡酮的浓度仍然很低。静脉（分别约为13和5倍）和口服（分别约为90和6倍）给药后，雄性SD大鼠中的去甲羟可待酮：羟吗啡酮的AUC比率大于雌性SD大鼠。 6.羟考酮的药代动力学，氧化代谢和口服生物利用度方面存在明显的性别差异。与雄性SD大鼠相比，雌性对羟考酮的全身暴露量更大，而雄性SD大鼠中对代谢衍生的去甲羟可待酮的全身暴露量更高。 7.将羟考酮口服给予SD大鼠对于研究羟考酮的药效学研究而言是一个不良的人类模型。

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《Clinical and experimental pharmacology & physiology 》 |2008年第3期| 共8页
作者
Chan S; Edwards SR; Wyse BD; Smith MT;
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正文语种 eng
中图分类药理学 ;
关键词
Oxycodone; Oral; Suspected diagnosis; Rattus norvegicus; Male gender; 羟可酮;

机译：羟考酮;口服;疑似诊断;北att;男性;羟可酮;

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1. Sex differences in the pharmacokinetics, oxidative metabolism and oral bioavailability of oxycodone in the Sprague-Dawley rat. [J] . Chan S, Edwards SR, Wyse BD, Clinical and experimental pharmacology & physiology . 2008 ,第3期

机译：Sprague-Dawley大鼠中羟考酮的药代动力学，氧化代谢和口服生物利用度方面的性别差异。
2. Metabolism of Cyanox in rat. II. Sex-related differences in oxidative dearylation and desulphuration. [J] . Tomigahara Y, Onogi M, Saito K, Xenobiotica: the fate of foreign compounds in biological systems . 2000 ,第4期

机译：Cyanox在大鼠中的代谢。二。氧化脱芳基和脱硫中与性别有关的差异。
3. Pharmacokinetics and metabolism of the reactive oxygen scavenger alpha-phenyl-N-tert-butylnitrone in the male Sprague-Dawley rat. [J] . Trudeau Lame ME, Kalgutkar AS, LaFontaine M Drug Metabolism and Disposition: The Biological Fate of Chemicals . 2003 ,第2期

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4. Improving the Oral Bioavailability of Raloxifene HCl and Atenolol in Male Sprague-Dawley Rats Using Novel Self-Correcting Amino Acid Tablet Formulations [C] . Wu, Y., Brunelle, Annual meeting exposition of the Controlled Release Society . 2005

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5. Sex differences in movement organization - II: The organization of sex differences in movement during food protection, contact righting, skilled reaching and vertical exploration in the rat. The role of gonadal steroids, body morphology, and the central nervous system. [D] . Field, Evelyn F. 2006

机译：运动组织中的性别差异-II：在食物保护，接触扶正，熟练触及和垂直探索过程中，大鼠运动性别差异的组织。性腺类固醇的作用，身体形态和中枢神经系统。
6. Inhibitory effects of centrally acting drugs on the neonatal imprinting of sex differences in the hepatic metabolism of a dimethylated epoxide in the rat. [O] . M. J. Finnen, K. A. Hassall 1984

机译：中枢作用药物对二甲基化环氧化物的肝脏代谢中性别差异的新生儿印迹的抑制作用。
7. Inhibitory effects of centrally acting drugs on the neonatal imprinting of sex differences in the hepatic metabolism of a dimethylated epoxide in the rat. [O] . Finnen, M. J., Hassall, K. A. 1984

机译：中枢作用药物对二甲基化环氧化物的肝脏代谢中性别差异的新生儿印迹的抑制作用。

Sex differences in the pharmacokinetics, oxidative metabolism and oral bioavailability of oxycodone in the Sprague-Dawley rat.

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