首页> 外文期刊>European neuropsychopharmacology: the journal of the European College of Neuropsychopharmacology >A proof of concept study of tolcapone for pathological gambling: Relationships with COMT genotype and brain activation
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A proof of concept study of tolcapone for pathological gambling: Relationships with COMT genotype and brain activation

机译:托卡朋用于病理性赌博的概念研究:与COMT基因型和大脑激活的关系

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Pathological gambling (PG) is a disabling disorder experienced by 1-3% of adults, and empirically validated treatments are lacking. Perturbations of prefrontal-dependent cognitive functions are implicated in the pathophysiology of PG. The enzyme catechol-O-methyl-transferase (COMT) is responsible for degradation of dopamine in the cortices and thereby is known to regulate such cognitive functions and their neural substrates. The objective of this study was to determine whether tolcapone, a COMT inhibitor, improves symptoms of PG and to explore whether such effects are dependent on COMT val-158-met polymorphism status and relate to concomitant changes in fronto-parietal activation. Twenty-four indviduals with PG were enrolled in an 8-week trial of oral tolcapone (100. mg/day titrated to 100. mg thrice/day) and 12 undertook pre- and post-treatment fMRI to examine brain activation during an executive planning task in a pre-defined fronto-parietal network. At baseline, patients with PG showed fronto-parietal under-activation versus controls during executive planning. Treatment was associated with statistically significant reductions on PG-Yale Brown Obsessive Compulsive Scale (PG-YBOCS), the extent of which correlated significantly with augmentation of planning-related fronto-parietal activation. Symptom improvement was also significantly more pronounced in subjects with the val/val COMT polymorphism. Tolcapone improved PG symptoms, and the extent of symptomatic improvement was significantly related to augmentation of fronto-parietal activation (fMRI probe) and COMT status. Objective genetic and fMRI markers hold promise in the search for targeting treatment and elucidating brain mechanisms associated with optimal clinical outcomes.
机译:病态赌博(PG)是1-3%的成年人经历的致残疾病,并且缺乏经过经验验证的治疗方法。前额叶依赖性认知功能的扰动与PG的病理生理有关。儿茶酚-O-甲基转移酶(COMT)负责皮质中多巴胺的降解,因此已知可调节此类认知功能及其神经基质。这项研究的目的是确定tolcapone(一种COMT抑制剂)是否可以改善PG的症状,并探讨这种作用是否取决于COMT val-158-met多态性状态并与额顶激活的伴随变化有关。 24名PG个人参加了为期8周的口服托卡酮试验(100. mg /天滴定至100. mg三次/天),其中12人进行了治疗前和治疗后fMRI检查在执行计划中的大脑激活情况预定义的额顶网络中的任务。基线时,PG患者在执行计划期间表现出额顶激活不足。治疗与PG-耶鲁布朗强迫症量表(PG-YBOCS)的统计学显着降低有关,其程度与计划相关的额顶激活的增加显着相关。 val / val COMT多态性患者的症状改善也明显更为明显。托卡朋可改善PG症状,而症状改善的程度与额顶激活(fMRI探针)和COMT状态的增加显着相关。客观的遗传和fMRI标记物有望用于寻找靶向治疗和阐明与最佳临床结果相关的脑机制。

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