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Fluvoxamine augmentation of olanzapine in chronic schizophrenia: pharmacokinetic interactions and clinical effects.

机译:氟伏沙明增加奥氮平在慢性精神分裂症中的药代动力学相互作用和临床效果。

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Olanzapine is a substrate of the cytochrome P450 enzyme (CYP) 1A2. In this study, pharmacokinetic interactions and clinical effects of adding the CYP1A2 inhibitor fluvoxamine to steady-state olanzapine was examined in patients suffering from schizophrenia. Eight patients had been treated for at least 3 months with 10 to 20 mg/day olanzapine. Fluvoxamine (100 mg/day) was added (week 0) to the olanzapine treatment and continued for 8 weeks. Concentrations of olanzapine and its metab-olite N-desmethylolanzapine and of fluvoxamine were analyzed at weeks 0, 1, 4, and 8. Addition of fluvoxamine resulted in a 12% to 112% ( < 0.01) increase of olanzapine from 31 +/- SD 15 ng/mL (week 0) to 56 +/- 31 ng/mL (week 8) in all patients. N-desmethylolanzapine concentrations were not significantly changed ( > 0.05). Fluvoxamine concentrations were 48 +/- 26 ng/mL on week 1 and 83 +/- 47 ng/mL on week 8. It is concluded that fluvoxamine affects olanzapine degradation and thus increases olanzapine concentrations. Although the combination was well tolerated in this sample and the negative symptom response appeared to be favorable in at least five patients, the combination therapy of olanzapine and fluvoxamine should be used cautiously and should be controlled by therapeutic drug monitoring to avoid olanzapine-induced side effects or intoxications.
机译:奥氮平是细胞色素P450酶(CYP)1A2的底物。在这项研究中,研究了精神分裂症患者在稳态奥氮平中添加CYP1A2抑制剂氟伏沙明的药代动力学相互作用和临床效果。八名患者接受了10至20毫克/天的奥氮平治疗至少3个月。将氟伏沙明(100毫克/天)添加到奥氮平治疗中(第0周),并持续8周。在第0、1、4和8周分析了奥氮平及其代谢物N-去甲基奥氮平和氟伏沙明的浓度。氟伏沙明的添加导致奥氮平从31 +/-增长12%至112%(<0.01)。所有患者的SD为15 ng / mL(第0周)至56 +/- 31 ng / mL(第8周)。 N-去甲基olanzapine浓度没有显着变化(> 0.05)。第1周的氟伏沙明浓度为48 +/- 26 ng / mL,第8周的氟伏沙明浓度为83 +/- 47 ng / mL。结论是氟伏沙明影响奥氮平的降解并因此增加了奥氮平的浓度。尽管该组合物耐受性良好,并且至少在五名患者中出现了不良症状反应,但奥氮平和氟伏沙明的联合治疗应谨慎使用,并应通过治疗药物监测加以控制,以避免奥氮平诱发的副作用或中毒。

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