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首页> 外文期刊>Brain: A journal of neurology >Individualized differential diagnosis of schizophrenia and mood disorders using neuroanatomical biomarkers
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Individualized differential diagnosis of schizophrenia and mood disorders using neuroanatomical biomarkers

机译:使用神经解剖生物标记物对精神分裂症和情绪障碍进行个体化鉴别诊断

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摘要

Magnetic resonance imaging-based markers of schizophrenia have been repeatedly shown to separate patients from healthy controls at the single-subject level, but it remains unclear whether these markers reliably distinguish schizophrenia from mood disorders across the life span and generalize to new patients as well as to early stages of these illnesses. The current study used structural MRI-based multivariate pattern classification to (i) identify and cross-validate a differential diagnostic signature separating patients with first-episode and recurrent stages of schizophrenia (n = 158) from patients with major depression (n = 104); and (ii) quantify the impact of major clinical variables, including disease stage, age of disease onset and accelerated brain ageing on the signature's classification performance. This diagnostic magnetic resonance imaging signature was then evaluated in an independent patient cohort from two different centres to test its generalizability to individuals with bipolar disorder (n = 35), first-episode psychosis (n = 23) and clinically defined at-risk mental states for psychosis (n = 89). Neuroanatomical diagnosis was correct in 80% and 72% of patients with major depression and schizophrenia, respectively, and involved a pattern of prefronto-temporo-limbic volume reductions and premotor, somatosensory and subcortical increments in schizophrenia versus major depression. Diagnostic performance was not influenced by the presence of depressive symptoms in schizophrenia or psychotic symptoms in major depression, but earlier disease onset and accelerated brain ageing promoted misclassification in major depression due to an increased neuroanatomical schizophrenia likeness of these patients. Furthermore, disease stage significantly moderated neuroanatomical diagnosis as recurrently-ill patients had higher misclassification rates (major depression: 23%; schizophrenia: 29%) than first-episode patients (major depression: 15%; schizophrenia: 12%). Finally, the trained biomarker assigned 74% of the bipolar patients to the major depression group, while 83% of the first-episode psychosis patients and 77% and 61% of the individuals with an ultra-high risk and low-risk state, respectively, were labelled with schizophrenia. Our findings suggest that neuroanatomical information may provide generalizable diagnostic tools distinguishing schizophrenia from mood disorders early in the course of psychosis. Disease course-related variables such as age of disease onset and disease stage as well alterations of structural brain maturation may strongly impact on the neuroanatomical separability of major depression and schizophrenia.
机译:反复显示基于磁共振成像的精神分裂症标志物可以使患者与健康对照在单受试者水平上分开,但是尚不清楚这些标志物是否能可靠地将精神分裂症与一生中的情绪障碍区分开来,并且可以推广到新患者以及到这些疾病的早期阶段。当前的研究使用基于MRI的结构多元模式分类来(i)识别和交叉验证将精神分裂症的首发和复发期患者(n = 158)与严重抑郁症患者(n = 104)分开的鉴别诊断特征; (ii)量化主要临床变量(包括疾病阶段,疾病发作年龄和脑部加速老化)对签名分类性能的影响。然后,在来自两个不同中心的独立患者队列中评估了这种诊断性磁共振成像签名,以测试其对双相情感障碍(n = 35),首发性精神病(n = 23)和临床定义的高危精神状态患者的普遍性用于精神病(n = 89)。神经解剖学诊断分别在80%和72%的重度抑郁症和精神分裂症患者中是正确的,并且涉及精神分裂症相对于重度抑郁症的前额颞叶边缘体积减少以及运动前,体感和皮层下增加的模式。精神分裂症患者的抑郁症状或重度抑郁症的精神病症状不会影响诊断性能,但是由于这些患者神经解剖学上的精神分裂症相似性增加,因此疾病的早期发作和脑衰老加速导致重度抑郁症的分类错误。此外,疾病阶段明显缓解了神经解剖学诊断,因为复发患者比初次发作患者(重度抑郁:15%;精神分裂症:12%)的误分类率更高(重度抑郁:23%;精神分裂症:29%)。最后,受过训练的生物标志物将74%的双相情感障碍患者分配为重度抑郁症组,而83%的首发精神病患者以及77%和61%的个体分别处于超高风险和低风险状态,被标记为精神分裂症。我们的研究结果表明,神经解剖学信息可能提供可区分精神分裂症和精神病早期情绪障碍的通用诊断工具。与疾病进程相关的变量,例如疾病的发病年龄和疾病阶段以及大脑结构的成熟改变,可能会严重影响重度抑郁症和精神分裂症的神经解剖学可分离性。

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