Department of Psychiatry, Icahn School of Medicine at Mount Sinai, New York, New York.
Social, Genetic & Developmental Psychiatry Centre, Institute of Psychiatry, Psychology & Neuroscience, King's College London, London, United Kingdom.
JAMA Psychiatry. 2018 Apr 1;75(4):386-395. doi: 10.1001/jamapsychiatry.2017.4741.
Alterations in multiple neuroimaging phenotypes have been reported in psychotic disorders. However, neuroimaging measures can be influenced by factors that are not directly related to psychosis and may confound the interpretation of case-control differences. Therefore, a detailed characterization of the contribution of these factors to neuroimaging phenotypes in psychosis is warranted.
To quantify the association between neuroimaging measures and behavioral, health, and demographic variables in psychosis using an integrated multivariate approach.
DESIGN, SETTING, AND PARTICIPANTS: This imaging study was conducted at a university research hospital from June 26, 2014, to March 9, 2017. High-resolution multimodal magnetic resonance imaging data were obtained from 100 patients with schizophrenia, 40 patients with bipolar disorder, and 50 healthy volunteers; computed were cortical thickness, subcortical volumes, white matter fractional anisotropy, task-related brain activation (during working memory and emotional recognition), and resting-state functional connectivity. Ascertained in all participants were nonimaging measures pertaining to clinical features, cognition, substance use, psychological trauma, physical activity, and body mass index. The association between imaging and nonimaging measures was modeled using sparse canonical correlation analysis with robust reliability testing.
Multivariate patterns of the association between nonimaging and neuroimaging measures in patients with psychosis and healthy volunteers.
The analyses were performed in 92 patients with schizophrenia (23 female [25.0%]; mean [SD] age, 27.0 [7.6] years), 37 patients with bipolar disorder (12 female [32.4%]; mean [SD] age, 27.5 [8.1] years), and 48 healthy volunteers (20 female [41.7%]; mean [SD] age, 29.8 [8.5] years). The imaging and nonimaging data sets showed significant covariation (r = 0.63, P < .001), which was independent of diagnosis. Among the nonimaging variables examined, age (r = -0.53), IQ (r = 0.36), and body mass index (r = -0.25) were associated with multiple imaging phenotypes; cannabis use (r = 0.23) and other substance use (r = 0.33) were associated with subcortical volumes, and alcohol use was associated with white matter integrity (r = -0.15). Within the multivariate models, positive symptoms retained associations with the global neuroimaging (r = -0.13), the cortical thickness (r = -0.22), and the task-related activation variates (r = -0.18); negative symptoms were mostly associated with measures of subcortical volume (r = 0.23), and depression/anxiety was associated with measures of white matter integrity (r = 0.12).
Multivariate analyses provide a more accurate characterization of the association between brain alterations and psychosis because they enable the modeling of other key factors that influence neuroimaging phenotypes.
精神障碍患者的多种神经影像学表型发生了改变。然而,神经影像学测量结果可能会受到与精神病无关的因素的影响,并且可能会干扰病例对照差异的解释。因此,详细描述这些因素对精神病神经影像学表型的贡献是有必要的。
使用综合多变量方法量化精神病患者的神经影像学测量值与行为、健康和人口统计学变量之间的关联。
设计、地点和参与者:这项影像学研究于 2014 年 6 月 26 日至 2017 年 3 月 9 日在一所大学研究医院进行。从 100 名精神分裂症患者、40 名双相情感障碍患者和 50 名健康志愿者中获取了高分辨率多模态磁共振成像数据;计算了皮质厚度、皮质下体积、白质各向异性分数、与工作记忆和情绪识别相关的大脑激活以及静息状态功能连接。所有参与者都进行了与临床特征、认知、物质使用、心理创伤、身体活动和体重指数相关的非成像测量。使用稳健可靠性测试的稀疏典型相关分析对成像和非成像测量之间的关联进行建模。
在精神病患者和健康志愿者中,非成像和神经影像学测量之间的关联的多变量模式。
在 92 名精神分裂症患者(23 名女性[25.0%];平均[标准差]年龄 27.0[7.6]岁)、37 名双相情感障碍患者(12 名女性[32.4%];平均[标准差]年龄 27.5[8.1]岁)和 48 名健康志愿者(20 名女性[41.7%];平均[标准差]年龄 29.8[8.5]岁)中进行了分析。成像和非成像数据集显示出显著的共变(r=0.63,P<.001),与诊断无关。在所检查的非成像变量中,年龄(r=-0.53)、智商(r=0.36)和体重指数(r=-0.25)与多种成像表型相关;大麻使用(r=0.23)和其他物质使用(r=0.33)与皮质下体积相关,酒精使用与白质完整性相关(r=-0.15)。在多变量模型中,阳性症状与全局神经影像学(r=-0.13)、皮质厚度(r=-0.22)和与任务相关的激活变量(r=-0.18)保留关联;阴性症状主要与皮质下体积测量值相关(r=0.23),抑郁/焦虑与白质完整性测量值相关(r=0.12)。
多变量分析通过建模影响神经影像学表型的其他关键因素,为脑改变与精神病之间的关联提供了更准确的描述。
