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27 个注解基因与氯氮平药物遗传学的关联研究:已有研究的验证及治疗反应新候选基因 ABCB1 的鉴定。

Association study of 27 annotated genes for clozapine pharmacogenetics: validation of preexisting studies and identification of a new candidate gene, ABCB1, for treatment response.

机构信息

Department of Laboratory Medicine and Genetics, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea.

出版信息

J Clin Psychopharmacol. 2012 Aug;32(4):441-8. doi: 10.1097/JCP.0b013e31825ac35c.

DOI:10.1097/JCP.0b013e31825ac35c
PMID:22722500
Abstract

OBJECTIVE

Pharmacogenetic studies on clozapine (CLZ) have provided meaningful insights but have shown redundancies owing to wide interindividual variability and insufficient replication. The present study was designed to validate hitherto suggested candidate genes on CLZ pharmacokinetics and pharmacodynamics and explore new markers through an integrative study.

METHODS

Based on a literature review, a total of 127 variations in 27 candidate genes were selected and analyzed. Ninety-six schizophrenic patients of Korean ethnicity with constant CLZ dosing were recruited, and information on body weight and smoking habits was gathered, as well as plasma drug levels and treatment responses.

RESULTS

Among the pharmacokinetic-related single nucleotide polymorphisms, rs2069521 and rs2069522 in CYP1A2 for CLZ/(dose/weight) and norclozapine/(dose/weight) and rs1135840 in CYP2D6 for norclozapine/CLZ showed borderline associations that were insignificant after correction for multiple testing. Regarding treatment response, significant associations were exhibited in rs7787082 and rs10248420 of ABCB1 (P = 0.0005 and P = 0.0013, respectively) even after correction, and the rs7787082 G and rs10248420 A alleles in ABCB1 were more frequently observed in nonresponders. We also observed a trend in the associations of rs13064530 in HRH1 and rs4938013 in DRD2/ANKK1 with treatment response.

CONCLUSIONS

We could not convincingly replicate most of the previous studies, a result that is possibly due to modest association between the suggested genes. Rather, we found a new candidate gene, ABCB1, for treatment response, which may provide a hypothesis on the relationship between the blood-brain distribution of CLZ and its clinical efficacy.

摘要

目的

氯氮平(CLZ)的遗传药理学研究提供了有意义的见解,但由于个体间变异性大且复制不足,显示出冗余。本研究旨在通过综合研究验证迄今为止关于 CLZ 药代动力学和药效学的候选基因,并探索新的标记物。

方法

基于文献综述,选择并分析了 27 个候选基因中的 127 个变异。共招募了 96 名韩国裔精神分裂症患者,他们接受了恒定剂量的 CLZ 治疗,并收集了体重和吸烟习惯等信息,以及血浆药物水平和治疗反应。

结果

在药代动力学相关的单核苷酸多态性中,CYP1A2 中的 rs2069521 和 rs2069522 与 CLZ/(剂量/体重)和 norclozapine/(剂量/体重)以及 CYP2D6 中的 rs1135840 与 norclozapine/CLZ 呈边缘关联,但经多次检验校正后无统计学意义。关于治疗反应,ABCB1 中的 rs7787082 和 rs10248420 显示出显著的关联(P = 0.0005 和 P = 0.0013),即使经过校正后也是如此,ABCB1 中的 rs7787082 G 和 rs10248420 A 等位基因在无反应者中更为常见。我们还观察到 HRH1 中的 rs13064530 和 DRD2/ANKK1 中的 rs4938013 与治疗反应呈关联趋势。

结论

我们未能令人信服地复制大多数先前的研究,这可能是由于所建议的基因之间的关联较小。相反,我们发现了一个新的候选基因,ABCB1,用于治疗反应,这可能为 CLZ 的血脑分布与其临床疗效之间的关系提供了一个假说。

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