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CHRM2基因rs1824024多态性与青少年早期抑郁的关系
引用本文:王美萍,张文新. CHRM2基因rs1824024多态性与青少年早期抑郁的关系[J]. 心理学报, 2010, 42(8): 853-861. DOI:  
作者姓名:王美萍  张文新
作者单位:1. 山东师范大学心理学院,济南,250014
2. 山东师范大学心理学院,济南250014;北京师范大学发展心理研究所,北京100875
基金项目:国家自然科学基金,教育部人文社科重点研究基地2008年度重大项目,全国教育科学"十一五"规划教育部青年专项课题,山东省泰山学者设岗学科、"十一五"强化建设重点学科(发展与教育心理学)建设经费资助项目
摘    要:运用问卷法与DNA分型技术,以127名高和低抑郁组初中生为被试,考察CHRM2基因rs1824024多态性与青少年早期抑郁的关系,重点探讨负性生活事件、青少年性别与年级的调节作用。结果发现,CHRM2基因rs1824024多态性与女青少年的抑郁边缘显著关联,T等位基因携带者患高抑郁的风险较低,但该位点与男青少年的抑郁无关;在那些经历低水平负性生活事件的青少年中,T等位基因携带者患高抑郁的可能性边缘显著低于GG型基因携带者;rs1824024多态性与年级对青少年早期抑郁无显著交互作用。

关 键 词:CHRM2基因  rs1824024多态性  抑郁  负性生活事件  青少年早期
收稿时间:2010-06-12

The Association Between Rs1824024 Polymorphism in the CHRM2 Gene and Early Adolescents' Depression
WANG Mei-Ping,ZHANG Wen-Xin. The Association Between Rs1824024 Polymorphism in the CHRM2 Gene and Early Adolescents' Depression[J]. Acta Psychologica Sinica, 2010, 42(8): 853-861. DOI:  
Authors:WANG Mei-Ping  ZHANG Wen-Xin
Affiliation:( School of Psychology, Shandong Normal University, Jinan 250014, China)
( Institute of Developmental Psychology, Beijing Normal University, Beijing 100875, China)
Abstract:Depression is among the top five leading causes of disability and disease burden throughout the world. It is well established that depression often has its origins in childhood, and early adolescence is associated with a sharp increase in the prevalence. The mechanism underlying depression has been studied intensively during the last few decades. With the advancement of molecular genetics, a number of studies have been conducted in recent years to identify the candidate genes and investigate the gene-environment interactions related to depression. However, the extant research has mainly focused on serotoninergic and dopaminergic systems, muscarinic–cholinergic pathways have scarcely been investigated. Although several recent studies have investigated the association between the polymorphisms in the CHRM2 gene and depression, the findings have not been always consistent. Meanwhile, no research on the effect of interaction between CHRM2 polymorphism and environment was reported. Besides, whether there is a moderating effect of age on the association between CHRM2 polymorphism and depression remains to be examined. The present study aimed to examine the association between rs1824024 polymorphism in the CHRM2 gene and depression among Chinese early adolescents, with particular focus on the moderating effect of negative life events, gender and grade on the association. The subjects of this study were 127 grade 7-9 adolescents (male = 65, female = 62) of high depression group (n= 59) and lower depression group (n= 68). The subjects’ status of depression were identified via adolescent’s self-rating on the depression questionnaire (CES-D, a = 0.87) and further validated via teacher assessment. DNA was extracted from saliva, and genotype at rs1824024 was performed for each participant in real time with MassARRAY RT software version 3.0.0.4 and analyzed using the MassARRAY Typer software version 3.4 (Sequenom). Data analysis was performed using the Statistical Package for Social Sciences 17.0 (SPSS 17.0), and chi-square and logistic regression analyses were conducted to depression distributions. A marginal moderating effect of gender on the association between depression and rs1824024 polymorphism was observed, such that female adolescents with T alleles possessed a decreased risk of depression, but no significant association was found among males. A marginal moderating effect of negative life events on the association between rs1824024 polymorphism and depression was also found. Compared with adolescents carrying GG genotype, adolescents carrying T allele had a decreased risk of depression, but this difference only existed among adolescents reporting low level of negative life events. No moderating effect of grade on the association between rs1824024 polymorphism and depression was found. The present study lends further support for the theory that acetylcholine may play an important role in depression, and thereby contributes to CHRM2 gene-depression literature by elaborating the moderating effect of negative life events and gender among healthy early adolescents.
Keywords:CHRM2 gene  rs1824024 polymorphism  depression  negative life events  early adolescence
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