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携带DRD2 TaqIA A1等位基因的帕金森病患者在执行高要求运动任务时大脑活动增加:一种代偿机制?

Increased cerebral activity in Parkinson's disease patients carrying the DRD2 TaqIA A1 allele during a demanding motor task: a compensatory mechanism?

作者信息

Bartrés-Faz D, Martí M J, Junqué C, Solé-Padullés C, Ezquerra M, Bralten L B C, Gaig C, Campdelacreu J, Mercader J M, Tolosa E

机构信息

Department de Psiquiatria i Psicobiologia Clinica, Facultat de Medicina, Universitat de Barcelona, and Institut d'Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS), Universitat de Barcelona, Barcelona, Spain.

出版信息

Genes Brain Behav. 2007 Aug;6(6):588-92. doi: 10.1111/j.1601-183X.2006.00290.x. Epub 2006 Nov 27.

DOI:10.1111/j.1601-183X.2006.00290.x
PMID:17147698
Abstract

Previous studies suggest that neuroimaging techniques are useful for detecting the effects of functional genetic polymorphisms on brain function in healthy subjects or in patients presenting with psychiatric or neurodegenerative conditions. Former evidence showed that individuals carrying risk alleles displayed broader patterns of brain activity during behavioural and cognitive tasks, despite being clinically comparable to non-carriers. This suggests the presence of compensatory brain mechanisms. In the present study, we investigated this effect in Parkinson's disease (PD) patients carrying the DRD2 TaqIA A1 allelic variant. This variant may confer an increased risk of developing the disease and/or influence the clinical presentation. During a complex sequential motor task, we evidenced by functional magnetic resonance imaging that A1 allele carriers activated a larger network of bilateral cerebral areas than non-carriers, including cerebellar and premotor regions. Both groups had similar clinical and demographic measures. In addition, their motor performance during the functional magnetic resonance experiment was comparable. Therefore, our conclusions, pending replication in a larger sample, seem to reflect the recruitment of compensatory cerebral resources during motor processing in PD patients carrying the A1 allele.

摘要

先前的研究表明,神经影像学技术有助于检测功能基因多态性对健康受试者或患有精神疾病或神经退行性疾病患者脑功能的影响。先前的证据显示,尽管携带风险等位基因的个体在临床症状上与非携带者相当,但在行为和认知任务期间,他们表现出更广泛的脑活动模式。这表明存在代偿性脑机制。在本研究中,我们对携带DRD2 TaqIA A1等位基因变体的帕金森病(PD)患者的这种效应进行了研究。该变体可能会增加患该疾病的风险和/或影响临床表现。在一项复杂的连续运动任务中,我们通过功能磁共振成像证明,与非携带者相比,A1等位基因携带者激活了更大范围的双侧脑区网络,包括小脑和运动前区。两组患者的临床和人口统计学指标相似。此外,他们在功能磁共振实验期间的运动表现相当。因此,在更大样本中进行重复验证之前,我们的结论似乎反映了携带A1等位基因的PD患者在运动处理过程中代偿性脑资源的调动。

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