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Accelerated brain aging in schizophrenia and beyond: A neuroanatomical marker of psychiatric disorders

机译:精神分裂症及其他地区加速的大脑衰老:精神疾病的神经解剖学标志

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摘要

Structural brain abnormalities are central to schizophrenia (SZ), but it remains unknown whether they are linked to dysmaturational processes crossing diagnostic boundaries, aggravating across disease stages, and driving the neurodiagnostic signature of the illness. Therefore, we investigated whether patients with SZ (N = 141), major depression (MD; N = 104), borderline personality disorder (BPD; N = 57), and individuals in at-risk mental states for psychosis (ARMS; N = 89) deviated from the trajectory of normal brain maturation. This deviation was measured as difference between chronological and the neuroanatomical age (brain age gap estimation [BrainAGE]). Neuroanatomical age was determined by a machine learning system trained to individually estimate age from the structural magnetic resonance imagings of 800 healthy controls. Group-level analyses showed that BrainAGE was highest in SZ (+5.5 y) group, followed by MD (+4.0), BPD (+3.1), and the ARMS (+1.7) groups. Earlier disease onset in MD and BPD groups correlated with more pronounced BrainAGE, reaching effect sizes of the SZ group. Second, BrainAGE increased across at-risk, recent onset, and recurrent states of SZ. Finally, BrainAGE predicted both patient status as well as negative and disorganized symptoms. These findings suggest that an individually quantifiable "accelerated aging" effect may particularly impact on the neuroanatomical signature of SZ but may extend also to other mental disorders.
机译:结构性脑异常是精神分裂症(SZ)的核心,但它们是否与跨越诊断界限,跨疾病阶段加重并推动疾病的神经诊断特征的发育不良过程有关,仍然未知。因此,我们调查了SZ患者(N = 141),重度抑郁症(MD; N = 104),边缘型人格障碍(BPD; N = 57)和处于高危精神状态的精神病患者(ARMS; N = 89)偏离了正常大脑成熟的轨迹。将该偏差测量为按时间顺序和神经解剖年龄之间的差异(脑年龄差距估计[Brainage])。神经解剖学年龄是通过机器学习系统确定的,该系统经过训练可以从800名健康对照的结构磁共振成像中分别估计年龄。小组级分析显示,SZ(+5.5 y)组的BrainAGE最高,其次是MD(+4.0),BPD(+3.1)和ARMS(+1.7)组。 MD和BPD组中较早的疾病发作与更明显的BrainAGE相关,达到SZ组的效应大小。其次,在SZ的高危,近期发作和复发状态中,BrainAGE有所增加。最终,BrainAGE可以预测患者状态以及阴性和混乱症状。这些发现表明,可单独量化的“加速衰老”效应可能特别影响SZ的神经解剖学特征,但也可能扩展到其他精神障碍。

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