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多巴胺D2受体基因变异与儿童及青少年中利培酮所致高催乳素血症

Variants of the dopamine D2 receptor gene and risperidone-induced hyperprolactinemia in children and adolescents.

作者信息

Calarge Chadi A, Ellingrod Vicki L, Acion Laura, Miller Del D, Moline Jessica, Tansey Michael J, Schlechte Janet A

机构信息

The University of Iowa Carver College of Medicine, Iowa, USA.

出版信息

Pharmacogenet Genomics. 2009 May;19(5):373-82. doi: 10.1097/FPC.0b013e328329a60f.

Abstract

OBJECTIVE

To investigate the association between hyperprolactinemia and variants of the dopamine D2 receptor (DRD2) gene in children and adolescents in long-term treatment with risperidone.

METHODS

Medically healthy 7 to 17-year-old patients chronically treated with risperidone but receiving no other antipsychotics were recruited in a cross-sectional study. Four DRD2 variants were genotyped and prolactin concentration was measured. Medication history was obtained from the medical records. The effect of the TaqIA variants of the DRD2 on the risk of risperidone-induced hyperprolactinemia was the primary outcome measure.

RESULTS

Hyperprolactinemia was present in 50% of 107 patients (87% males) treated with risperidone for an average of 2.9 years. Age, stage of sexual development, and the dose of risperidone independently predicted a higher prolactin concentration, whereas the dose of psychostimulants was negatively correlated with it. However, these four predictors became nonsignificant when risperidone serum concentration was entered into the model. Adverse events potentially related to hyperprolactinemia were more common in participants with elevated prolactin concentration and in girls (45%) compared with boys (10%). After controlling for risperidone concentration and the dose of psychostimulants, the TaqIA A1 and the A-241G alleles were associated with higher prolactin concentration, whereas the -141C Ins/Del and C957T variants had no significant effect. In addition, adverse events potentially related to hyperprolactinemia were four times more common in TaqIA A1 allele carriers.

CONCLUSION

Prolactin concentration is closely related to central DRD2 blockade, as reflected by risperidone serum concentration. Furthermore, the TaqIA and A-241G variants of the DRD2 gene could be useful in predicting the emergence of hyperprolactinemia and its potential adverse events.

摘要

目的

探讨长期使用利培酮治疗的儿童和青少年高催乳素血症与多巴胺D2受体(DRD2)基因变异之间的关联。

方法

在一项横断面研究中招募了7至17岁长期接受利培酮治疗但未使用其他抗精神病药物的身体健康的患者。对四个DRD2变异进行基因分型,并测量催乳素浓度。从病历中获取用药史。DRD2的TaqIA变异对利培酮所致高催乳素血症风险的影响是主要结局指标。

结果

107例接受利培酮治疗平均2.9年的患者中,50%存在高催乳素血症(87%为男性)。年龄、性发育阶段和利培酮剂量独立预测催乳素浓度较高,而精神兴奋剂剂量与之呈负相关。然而,当将利培酮血清浓度纳入模型时,这四个预测因素变得无统计学意义。与高催乳素血症潜在相关的不良事件在催乳素浓度升高的参与者和女孩(45%)中比男孩(10%)更常见。在控制利培酮浓度和精神兴奋剂剂量后,TaqIA A1和A - 241G等位基因与较高的催乳素浓度相关,而 - 141C Ins/Del和C957T变异无显著影响。此外,TaqIA A1等位基因携带者中与高催乳素血症潜在相关的不良事件常见四倍。

结论

催乳素浓度与中枢DRD2阻断密切相关,如利培酮血清浓度所反映。此外,DRD2基因的TaqIA和A - 241G变异可用于预测高催乳素血症及其潜在不良事件的发生。

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