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Patterns of deficits in brain function in bipolar disorder and schizophrenia: A cluster analytic study

机译:双相情感障碍和精神分裂症脑功能缺陷的模式:一项聚类分析研究

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Historically, bipolar disorder and schizophrenia have been considered distinct disorders with different etiologies. Growing evidence suggests that overlapping genetic influences contribute to risk for these disorders and that each disease is genetically heterogeneous. Using cluster analytic methods, we empirically identified homogeneous subgroups of patients, their relatives, and controls based on distinct neurophysiologic profiles. Seven phenotypes were collected from two independent cohorts at two institutions. K-means clustering was used to identify neurophysiologic profiles. In the analysis of all participants, three distinct profiles emerged: "globally impaired", "sensory processing", and "high cognitive". In a secondary analysis, restricted to patients only, we observed a similar clustering into three profiles. The neurophysiological profiles of the Schizophrenia (SZ) and Bipolar Disorder (BPD) patients did not support the Diagnostic and Statistical Manual of Mental Disorders (DSM) diagnostic distinction between these two disorders. Smokers in the globally impaired group smoked significantly more cigarettes than those in the sensory processing or high cognitive groups. Our results suggest that empirical analyses of neurophysiological phenotypes can identify potentially biologically relevant homogenous subgroups independent of diagnostic boundaries. We hypothesize that each neurophysiology subgroup may share similar genotypic profiles, which may increase statistical power to detect genetic risk factors.
机译:历史上,双相情感障碍和精神分裂症被认为是病因不同的独特疾病。越来越多的证据表明,重叠的遗传影响会增加这些疾病的风险,并且每种疾病在遗传上都是异质的。使用聚类分析方法,我们根据不同的神经生理特征凭经验确定了患者,其亲属和对照的同质亚组。从两个机构的两个独立队列中收集了七个表型。 K-均值聚类被用来识别神经生理特征。在对所有参与者的分析中,出现了三个不同的特征:“全球受损”,“感觉处理”和“高度认知”。在仅限于患者的二级分析中,我们观察到了类似的聚类为三个特征的聚类。精神分裂症(SZ)和双相情感障碍(BPD)患者的神经生理学特征不支持这两种疾病之间的精神障碍诊断和统计手册(DSM)诊断区别。与感官加工或认知能力较高的人群相比,全球有障碍的吸烟者的吸烟量明显增加。我们的结果表明,对神经生理表型的经验分析可以确定独立于诊断界限的潜在生物学相关的同质亚组。我们假设每个神经生理亚组可能共享相似的基因型谱,这可能会增加检测遗传危险因素的统计能力。

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