alpha2c -肾上腺素能受体Del322-325多态性与精神疾病的风险:与阿片类药物滥用和依赖的显著关联

G. Rivero, I. Martín-Guerrero, Elena de Prado, A. Gabilondo, L. Callado, J. García-Sevilla, A. García-Orad, J. Meana
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引用次数: 7

摘要

目的α 2c -肾上腺素受体(α2C-AR)参与与精神障碍和自杀完成相关的行为反应。遗传多态性α2CDel322-325-AR赋予功能丧失表型。功能性人体研究发现α2CDel322-325-AR多态性与重度抑郁症病理生理相关。本研究的目的是首次分析α2CDel322-325-AR多态性与自杀完成和相关精神疾病(重度抑郁症、精神分裂症、阿片类药物和酒精滥用和依赖)的关系。方法提取516例死后脑组织DNA,采用HaeIII酶切法对PCR产物进行基因分型,并用毛细管测序仪进行DNA片段分析。对扩增产物进行测序以确认多态性的存在。结果自杀患者α2CDel322-325-AR发生率为9% (n = 236),非自杀患者为11% (n = 280)。抑郁症患者(15%,n = 39)和精神分裂症患者(18%,n = 39) α2CDel322-325-AR多态性基因型频率高于对照组(7%,n = 187),但差异无统计学意义(P = 0.125和P = 0.063)。α2CDel322-325-AR多态性与阿片类药物滥用和依赖存在选择性且显著的相关性(23%,n = 35, P = 0.011)。结论α2CDel322-325-AR可能在阿片类药物滥用和依赖的病理生理中发挥作用,值得开展更大规模的遗传关联研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Alpha2C-adrenoceptor Del322-325 polymorphism and risk of psychiatric disorders: significant association with opiate abuse and dependence
Abstract Objectives α2C-adrenoceptors (α2C-AR) are involved in behavioural responses relevant to psychiatric disorders and suicide completion. The genetic polymorphism α2CDel322-325-AR confers a loss-of-function phenotype. Functional human studies have associated α2CDel322-325-AR polymorphism with major depression pathophysiology. The aim of this study was to analyse, for the first time, the association of α2CDel322-325-AR polymorphism with suicide completion and with related psychiatric disorders: major depression, schizophrenia, opiate and alcohol abuse and dependence. Methods Post-mortem brain DNA was extracted (n = 516) and genotyping performed by HaeIII restriction endonuclease digestion of PCR products and DNA fragment analysis on capillary sequencer. Amplified products were sequenced to confirm the presence of the polymorphism. Results The frequency of α2CDel322-325-AR in suicide (9%, n = 236) and non-suicide victims (11%, n = 280) was similar. Genotype frequencies for the α2CDel322-325-AR polymorphism in depressed (15%, n = 39) and schizophrenic subjects (18%, n = 39) were higher than in controls (7%, n = 187), but these differences did not reach statistical significance (P = 0.125 and P = 0.063, respectively). A selective and significant association of α2CDel322-325-AR polymorphism with opiate abuse and dependence was found (23%, n = 35, P = 0.011). Conclusions Our results indicate that α2CDel322-325-AR may play a role in the pathophysiology of opiate abuse and dependence and raise the interest for larger genetic associative studies.
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