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首页> 外文期刊>British Journal of Clinical Pharmacology >Time course of the increase in 4beta-hydroxycholesterol concentration during carbamazepine treatment of paediatric patients with epilepsy.
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Time course of the increase in 4beta-hydroxycholesterol concentration during carbamazepine treatment of paediatric patients with epilepsy.

机译:卡马西平治疗小儿癫痫患者中4β-羟基胆固醇浓度增加的时间过程。

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WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT: CYP3A4 converts cholesterol into 4beta-hydroxycholesterol. We have suggested that 4beta-hydroxycholesterol could be used as a clinical marker for CYP3A4 activity aiding in dose adjustments. The kinetics of 4beta-hydroxycholesterol formation is not known, however, and must be determined in order to establish under what conditions 4beta-hydroxycholesterol can be used as a CYP3A marker. WHAT THIS STUDY ADDS: The concentration of 4beta-hydroxycholesterol increases very slowly during CYP3A4/5 induction in paediatric patients. Whereas induction of CYP3A4/5 was apparently complete within 1-2 weeks of carbamazepine treatment, plasma 4beta-hydroxycholesterol levels continued to increase until at least 8 weeks of treatment. AIMS To investigate the time course of the increase in 4beta-hydroxycholesterol and carbamazepine plasma concentrations during treatment of paediatric patients with epilepsy. METHODS: Eight paediatric patients with newly diagnosed epilepsy were studied. Blood samples were drawn before and after about 1, 2, 4, 8 and 16 weeks of carbamazepine treatment. The plasma concentrations of 4beta-hydroxycholesterol were determined by gas chromatography-mass spectrometry and carbamazepine and its epoxide metabolite by high-performance liquid chromatography. RESULTS: The basal plasma concentrations of 4beta-hydroxycholesterol showed a large range of observed values between 18 and 99 ng ml(-1). Carbamazepine treatment increased mean plasma 4beta-hydroxycholesterol significantly already after 1 week of treatment (from 43 to 80 ng ml(-1), P < 0.001). 4beta-Hydroxycholesterol concentrations continued to increase until at least 8 weeks of treatment and the concentrations in the final samples (8-23 weeks of treatment) varied between 122 and 494 ng ml(-1). Plasma concentrations of carbamazepine and its epoxide metabolite reached steady state at 1-2 weeks after last dose change. CONCLUSIONS: Carbamazepine treatment of paediatric patients with epilepsy resulted in an induction of CYP3A4/5 and a concomitant increase in plasma 4beta-hydroxycholesterol. Whereas the induction of CYP3A4/5 was apparently complete after 1-2 weeks, the increase in 4beta-hydroxycholesterol continued for several weeks. Thus CYP3A4 activity is not the only determinant of the circulating level of 4beta-hydroxycholesterol. Additional factors such as transport and storage or presence of another enzyme may thus be of importance.
机译:该对象已经知道的是:CYP3A4将胆固醇转化为4beta-羟基胆固醇。我们建议将4beta-羟基胆固醇用作CYP3A4活性的临床标志物,以帮助进行剂量调整。但是,尚不知道4β-羟基胆固醇形成的动力学,以便确定在什么条件下4β-羟基胆固醇可用作CYP3A标记。该研究的结果:儿科患者在CYP3A4 / 5诱导过程中4β-羟基胆固醇的浓度增加非常缓慢。 CYP3A4 / 5的诱导在卡马西平治疗的1-2周内明显完成,而血浆4β-羟基胆固醇水平持续升高,直到治疗至少8周。目的探讨在治疗小儿癫痫患者中4β-羟基胆固醇和卡马西平血浆浓度增加的时间过程。方法:对8例新诊断为癫痫病的儿童进行研究。在卡马西平治疗前后约1、2、4、8和16周抽取血液样本。血浆4β-羟基胆固醇的含量通过气相色谱-质谱法测定,卡马西平及其环氧化物代谢产物的含量通过高效液相色谱法测定。结果:4β-羟基胆固醇的基础血浆浓度在18至99 ng ml(-1)之间显示出较大的观测值范围。卡马西平治疗在治疗1周后已经显着增加了平均血浆4β-羟基胆固醇的浓度(从43到80 ng ml(-1),P <0.001)。 4β-羟基胆固醇的浓度持续增加,直到至少治疗8周为止,最终样品(治疗8-23周)的浓度在122至494 ng ml(-1)之间变化。最后一次更改剂量后1-2周,卡马西平及其环氧化物代谢物的血浆浓度达到稳态。结论:卡马西平治疗小儿癫痫患者导致CYP3A4 / 5的诱导和血浆4β-羟基胆固醇的同时升高。 CYP3A4 / 5的诱导在1-2周后明显完成,而4beta-羟基胆固醇的增加持续了数周。因此,CYP3A4活性不是4β-羟基胆固醇循环水平的唯一决定因素。因此,其他因素,例如运输和储存或另一种酶的存在可能很重要。

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