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首页> 外文期刊>The Journal of Clinical Pharmacology: Official Journal of the American College of Clinical Pharmacology >Pharmacokinetics of a newly identified active metabolite of buspirone after administration of buspirone over its therapeutic dose range.
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Pharmacokinetics of a newly identified active metabolite of buspirone after administration of buspirone over its therapeutic dose range.

机译:在治疗剂量范围内给予丁螺环酮后,新发现的丁螺环酮活性代谢物的药代动力学。

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摘要

The objective of this study was to assess the pharmacokinetics of a newly identified active metabolite of buspirone, 6-hydroxybuspirone (6OHB), over the therapeutic dose range of buspirone. A 26-day, open-label, nonrandomized, single-sequence, dose-escalation study in normal healthy volunteers was conducted (N = 13). Subjects received escalating doses of buspirone with each dose administered for 5 days starting at a dose of 5 mg twice daily and increasing up to 30 mg twice daily. Plasma concentrations of 6OHB were approximately 40-fold greater than those of buspirone. 6OHB was rapidly formed following buspirone administration, and exposure increased proportionally with buspirone dose. Further research regarding the safety and efficacy of 6OHB itself is warranted.
机译:这项研究的目的是评估新确定的丁螺环酮的活性代谢产物6-羟基丁螺环酮(6OHB)在丁螺环酮的治疗剂量范围内的药代动力学。在正常健康志愿者中进行了为期26天,开放标签,非随机,单序列,剂量递增的研究(N = 13)。受试者接受递增剂量的丁螺环酮,每次给予5天,起始剂量为每日两次两次5mg,每天两次增加至30mg。 6OHB的血浆浓度约为丁螺环酮的40倍。服用丁螺环酮后6OHB迅速形成,并且暴露量与丁螺环酮剂量成比例增加。值得进一步研究6OHB本身的安全性和有效性。

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