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性别和年龄对氯氮平及其代谢产物血浆水平的影响:通过临界统计学分析

Effects of gender and age on plasma levels of clozapine and its metabolites: analyzed by critical statistics.

作者信息

Lane H Y, Chang Y C, Chang W H, Lin S K, Tseng Y T, Jann M W

机构信息

Graduate Institute of Life Sciences, National Defense Medical Center, Taipei, Taiwan.

出版信息

J Clin Psychiatry. 1999 Jan;60(1):36-40. doi: 10.4088/jcp.v60n0108.

Abstract

BACKGROUND

Previous reports concerning the effects of gender and age on steady-state plasma concentrations of clozapine and its major metabolites, norclozapine and clozapine-N-oxide, have been controversial. Since the frequency distribution of the plasma levels is asymmetrical and skewed to the right, the statistical methods (such as analysis of variance and regression analysis) used earlier are actually inappropriate for analyzing the effects of the variables on the concentrations and might contribute to the inconsistent results. The goal of the present study, with befitting statistics, is to measure the potential effect of dose, gender, age, and body weight on plasma levels of clozapine and its 2 major metabolites.

METHOD

We retrospectively analyzed data from a therapeutic drug monitoring study for steady-state plasma clozapine, norclozapine, and clozapine-N-oxide levels that was conducted in a large group of Chinese schizophrenic inpatients (male:female ratio = 83:79; age range, 33.8 +/- 9.3 years). The daily doses of clozapine had ranged from 100 to 900 mg, with a mean +/- SD value of 379.5 +/- 142.2 mg. Plasma concentrations had been measured using high-performance liquid chromatography with ultraviolet detection. Multiple linear regression was adopted to quantify the effects of various factors on the plasma levels. The natural logarithm of the plasma level was used as the dependent variable to overcome the skewness problem.

RESULTS

After adjusting the effects of gender, age, and body weight by multiple linear regression, each 1-mg increment in the daily dose could raise the clozapine level by 0.31%, norclozapine by 0.27%, and clozapine-N-oxide by 0.16%. Female patients had 34.9% higher clozapine levels and 36.3% higher norclozapine, with other variables being controlled. No sex differences were demonstrated for clozapine-N-oxide levels. Each 1-year increment in age would elevate the clozapine level by 1.1%, norclozapine by 1.0%, and clozapine-N-oxide by 1.0%. Body weight could not influence the levels of these compounds.

CONCLUSION

The present results suggest that women possess higher plasma levels (about one third higher) of clozapine and norclozapine, but not the N-oxide metabolite. Each addition of 1 year in age elevated clozapine and either metabolite's levels by about 1%. Furthermore, every 1-mg increase in the daily dose raised clozapine and norclozapine concentrations by approximately 0.3%. These findings could assist clinicians in optimizing clozapine dosing strategies.

摘要

背景

先前有关性别和年龄对氯氮平及其主要代谢物去甲氯氮平和氯氮平氮氧化物稳态血浆浓度影响的报告一直存在争议。由于血浆水平的频率分布不对称且向右偏态,早期使用的统计方法(如方差分析和回归分析)实际上不适用于分析变量对浓度的影响,可能导致结果不一致。本研究的目的是运用合适的统计方法,测量剂量、性别、年龄和体重对氯氮平及其两种主要代谢物血浆水平的潜在影响。

方法

我们回顾性分析了一项针对一大群中国精神分裂症住院患者(男:女比例 = 83:79;年龄范围,33.8 ± 9.3岁)进行的治疗药物监测研究中氯氮平、去甲氯氮平和氯氮平氮氧化物稳态血浆水平的数据。氯氮平的日剂量范围为100至900毫克,平均 ± 标准差为379.5 ± 142.2毫克。采用高效液相色谱 - 紫外检测法测量血浆浓度。采用多元线性回归来量化各种因素对血浆水平的影响。血浆水平的自然对数用作因变量以克服偏态问题。

结果

通过多元线性回归调整性别、年龄和体重的影响后,日剂量每增加1毫克,氯氮平水平可提高0.31%,去甲氯氮平提高0.27%,氯氮平氮氧化物提高0.16%。在控制其他变量的情况下,女性患者的氯氮平水平高34.9%,去甲氯氮平水平高36.3%。氯氮平氮氧化物水平未显示出性别差异。年龄每增加1岁,氯氮平水平将升高1.1%,去甲氯氮平升高1.0%,氯氮平氮氧化物升高1.0%。体重不会影响这些化合物的水平。

结论

目前的结果表明,女性的氯氮平和去甲氯氮平血浆水平较高(约高三分之一),但氮氧化物代谢物并非如此。年龄每增加1岁,氯氮平及其任何一种代谢物的水平升高约1%。此外,日剂量每增加1毫克,氯氮平和去甲氯氮平的浓度升高约0.3%。这些发现可帮助临床医生优化氯氮平给药策略。

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