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阿尔茨海默病中精神病发作的预测:抑郁症状严重程度和HTR2A基因T102C多态性的作用。

Prediction of psychosis onset in Alzheimer disease: the role of depression symptom severity and the HTR2A T102C polymorphism.

作者信息

Wilkosz Patricia A, Kodavali Chowdari, Weamer Elise A, Miyahara Sachiko, Lopez Oscar L, Nimgaonkar Vishwajit L, DeKosky Steven T, Sweet Robert A

机构信息

Department of Psychiatry, University of Pittsburgh, Pittsburgh, Pennsylvania, USA.

出版信息

Am J Med Genet B Neuropsychiatr Genet. 2007 Dec 5;144B(8):1054-62. doi: 10.1002/ajmg.b.30549.

Abstract

Psychotic symptoms in Alzheimer disease (AD + P) identify a heritable phenotype associated with a more severe course. We recently found an association of AD + P with depression symptom severity. Reports have shown an association of a serotonin-2A receptor (HTR2A) gene T102C polymorphism with AD + P and with depression during AD. We examined the interaction of this common genetic polymorphism with depression and increased psychosis risk. Subjects with possible or probable AD or mild cognitive impairment (MCI) without psychosis at study entry were genotyped for the HTR2A T102C polymorphism and reassessed every 6 months until psychosis onset. Psychotic and depressive symptoms were rated using the CERAD behavioral rating scale (CBRS). Cox proportional hazard models with time-dependent covariates were used to examine associations with psychosis onset. A total of 324 Caucasian subjects completed at least one follow-up exam. Depressive symptom severity was a strong predictor of psychosis onset. Neither psychosis onset nor depression severity was associated with the HTR2A genotype. Genotype interacted with depression severity to moderate the risk of AD + P onset. This did not result from an interaction of HTR2A genotype with antidepressant use. Psychosis onset in AD is strongly associated with severity of depressive symptoms, an association that may be modified by HTR2A genotype.

摘要

阿尔茨海默病的精神病性症状(AD + P)识别出一种与更严重病程相关的可遗传表型。我们最近发现AD + P与抑郁症状严重程度之间存在关联。报告显示,血清素-2A受体(HTR2A)基因T102C多态性与AD + P以及AD期间的抑郁有关。我们研究了这种常见基因多态性与抑郁及精神病风险增加之间的相互作用。研究开始时无精神病的可能或很可能患有AD或轻度认知障碍(MCI)的受试者进行了HTR2A T102C多态性基因分型,并每6个月重新评估一次,直至精神病发作。使用CERAD行为评定量表(CBRS)对精神病性和抑郁症状进行评分。采用带有时间依存性协变量的Cox比例风险模型来研究与精神病发作的关联。共有324名白人受试者完成了至少一次随访检查。抑郁症状严重程度是精神病发作的有力预测指标。精神病发作和抑郁严重程度均与HTR2A基因型无关。基因型与抑郁严重程度相互作用,可调节AD + P发作的风险。这并非由HTR2A基因型与抗抑郁药使用之间的相互作用所致。AD中的精神病发作与抑郁症状严重程度密切相关,这种关联可能会因HTR2A基因型而改变。

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