Plasma concentrations of quetiapine, N-desalkylquetiapine, O-desalkylquetiapine, 7-hydroxyquetiapine, and quetiapine sulfoxide in relation to quetiapine dose, formulation, and other factors

FisherD.S.; HandleyS.A.; FlanaganR.J.; TaylorD.M.

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Plasma concentrations of quetiapine, N-desalkylquetiapine, O-desalkylquetiapine, 7-hydroxyquetiapine, and quetiapine sulfoxide in relation to quetiapine dose, formulation, and other factors

机译：与喹硫平剂量，制剂和其他因素相关的喹硫平，N-去烷基喹硫平，O-去烷基喹硫平，7-羟基喹硫平和喹硫平亚砜的血浆浓度

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BACKGROUND: N-Desalkylquetiapine may be a pharmacologically active quetiapine metabolite. However, information on plasma concentrations of N-desalkylquetiapine and other quetiapine metabolites attained during quetiapine therapy is scant. The aim of this study was to investigate plasma concentrations of quetiapine, N-desalkylquetiapine, O-desalkylquetiapine, 7-hydroxyquetiapine, and quetiapine sulfoxide attained during therapy and analyze the data with respect to prescribed dose and other variables. METHOD: Quetiapine and its metabolites were measured in plasma samples submitted for quetiapine therapeutic drug monitoring (2009-2011). Concentration, metabolic ratio, and concentration corrected for dose (C/D) were investigated against quetiapine dose, age, sex, and formulation. Sample results were excluded if nonadherence with therapy was queried. RESULTS: There were 99 samples from 59 patients. N-Desalkylquetiapine plasma concentrations showed the strongest correlation with dose of all analytes, but O-desalkylquetiapine and quetiapine sulfoxide were strongly correlated to plasma quetiapine concentrations. There was no significant difference in C/D for any analyte between males and females and no correlation to age. Quetiapine and quetiapine sulfoxide C/D were significantly different (P < 0.01) between patients prescribed immediate- and extended-release formulations. Quetiapine, 7-hydroxyquetiapine and quetiapine sulfoxide C/D showed significant variation (P < 0.02) between those samples taken 10-14 hours postdose as compared with that of 16-24 hours postdose, but there was no significant effect as regards N-desalkylquetiapine. CONCLUSIONS: Plasma quetiapine, O-desalkylquetiapine, 7-hydroxyquetiapine, and quetiapine sulfoxide concentrations were significantly affected by formulation and/or time since last dose. Plasma N-desalkylquetiapine concentrations were not affected by either factor therefore may be a better marker for quetiapine exposure than plasma quetiapine concentrations.

机译：背景：N-去烷基喹硫平可能是具有药理活性的喹硫平代谢产物。但是，有关喹硫平治疗期间获得的N-去烷基喹硫平和其他喹硫平代谢物血浆浓度的信息很少。这项研究的目的是研究在治疗过程中获得的喹硫平，N-去烷基喹硫平，O-去烷基喹硫平，7-羟基喹硫平和喹硫平亚砜的血浆浓度，并分析有关处方剂量和其他变量的数据。方法：在提交喹硫平治疗药物监测的血浆样品中测定喹硫平及其代谢产物（2009-2011年）。针对喹硫平剂量，年龄，性别和配方，研究了浓度，代谢率和校正剂量（C / D）的浓度。如果查询不坚持治疗，则排除样本结果。结果：59例患者中有99个样本。 N-去烷基喹硫平血浆浓度与所有分析物的剂量显示最强的相关性，但是O-去烷基喹硫平和喹硫平亚砜与血浆喹硫平浓度密切相关。男性和女性之间任何分析物的C / D均无显着差异，并且与年龄无关。处方速释和缓释制剂的患者之间的喹硫平和喹硫平亚砜C / D有显着差异（P <0.01）。服药后10-14小时与服药后16-24小时相比，喹硫平，7-羟基喹硫平和奎硫平亚砜C / D表现出显着差异（P <0.02），但对N-去烷基奎硫平没有明显影响。结论：血浆喹硫平，O-去烷基喹硫平，7-羟基喹硫平和喹硫平亚砜的浓度受自上次给药以来的制剂和/或时间的影响。血浆N-去烷基喹硫平浓度不受任何一个因素的影响，因此与血浆喹硫平浓度相比，它可能是喹硫平暴露的更好标志。

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《Therapeutic Drug Monitoring》 |2012年第4期|共7页
作者
FisherD.S.; HandleyS.A.; FlanaganR.J.; TaylorD.M.;
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正文语种 eng
中图分类生药学（天然药物学）;
关键词
N-desalkylquetiapine; pharmacokinetics; quetiapine; quetiapine sulfoxide; therapeutic drug monitoring;

机译：N-去烷基喹硫平;药物动力学;喹硫平;喹硫平亚砜;治疗药物监测;

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1. Plasma concentrations of quetiapine, N-desalkylquetiapine, O-desalkylquetiapine, 7-hydroxyquetiapine, and quetiapine sulfoxide in relation to quetiapine dose, formulation, and other factors [J] . FisherD.S., HandleyS.A., FlanaganR.J., Therapeutic Drug Monitoring . 2012,第4期

机译：与喹硫平剂量，制剂和其他因素相关的喹硫平，N-去烷基喹硫平，O-去烷基喹硫平，7-羟基喹硫平和喹硫平亚砜的血浆浓度
2. Plasma quetiapine in relation to prescribed dose and other factors: data from a therapeutic drug monitoring service, 2000–2011 [J] . Simon A. Handley, Sally V.J. Bowskill, Maxine X. Patel, Therapeutic advances in psychopharmacology. . 2013,第3期

机译：与处方剂量和其他因素相关的喹硫平：来自治疗药物监测服务的数据，2000-2011年
3. Relationship between daily dose, plasma concentrations, dopamine receptor occupancy, and clinical response to quetiapine: a review. [J] . Sparshatt A, Taylor D, Patel MX, The journal of clinical psychiatry . 2011,第8期

机译：每日剂量，血浆浓度，多巴胺受体占用率和对喹硫平的临床反应之间的关系：综述。
4. Prevention of relapses in the bipolar I disorder: a comparative study between quetiapine monotherapy vs. quetiapine-valproate combined therapy [C] . PETRU IFTENI, VICTORIA BURTEA, CORNELIU MOSOIU WSEAS International Conferences . 2009

机译：预防双极I紊乱中的复发：喹硫代单药治疗的比较研究与喹硫氨酸 - 戊醛组合治疗
5. Determination of the Levels and Concentrations of the Most Used Autism Spectrum Disorder Medications (Olanzapine, Risperidone and Quetiapine) in Autistic Patient’s Plasma by Using Lc/Ms/Ms [D] . Fraih, Dana Fayez. 2020

机译：通过使用LC / MS / MS测定自闭症患者血浆中最常用的自闭症谱系药物（Olanzapine，Risperidone和Quetiapine）的水平和浓度
6. Plasma quetiapine in relation to prescribed dose and other factors: data from a therapeutic drug monitoring service 2000–2011 [O] . Simon A. Handley, Sally V.J. Bowskill, Maxine X. Patel, 2013

机译：血浆喹硫平与处方剂量和其他因素的关系：治疗药物监测服务提供的数据2000-2011年
7. Plasma quetiapine in relation to prescribed dose and other factors:Data from a therapeutic drug monitoring service, 2000-2011 [O] . Handley, Simon A., Bowskill, Sally V. J., Patel, Maxine X., 2013

机译：与处方剂量和其他因素相关的喹硫平血浆：治疗药物监测服务提供的数据，2000-2011年

Plasma concentrations of quetiapine, N-desalkylquetiapine, O-desalkylquetiapine, 7-hydroxyquetiapine, and quetiapine sulfoxide in relation to quetiapine dose, formulation, and other factors

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