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视觉和躯体运动网络的功能失调为精神病产生了一种简单而可靠的生物标志物。

Functional dysconnectivity of visual and somatomotor networks yields a simple and robust biomarker for psychosis.

作者信息

Keane Brian P, Abrham Yonatan T, Cole Michael W, Johnson Brent A, Hu Boyang, Cocuzza Carrisa V

机构信息

Departments of Psychiatry and Neuroscience, University of Rochester Medical Center, 430 Elmwood Ave, Rochester, NY, 14642, USA.

Center for Visual Science, University of Rochester, 601 Elmwood Ave, P.O. Box 319, Rochester, NY, 14642, USA.

出版信息

Mol Psychiatry. 2025 Apr;30(4):1539-1547. doi: 10.1038/s41380-024-02767-3. Epub 2024 Oct 4.

Abstract

People with psychosis exhibit thalamo-cortical hyperconnectivity and cortico-cortical hypoconnectivity with sensory networks, however, it remains unclear if this applies to all sensory networks, whether it arises from other illness factors, or whether such differences could form the basis of a viable biomarker. To address the foregoing, we harnessed data from the Human Connectome Early Psychosis Project and computed resting-state functional connectivity (RSFC) matrices for 54 healthy controls and 105 psychosis patients. Primary visual, secondary visual ("visual2"), auditory, and somatomotor networks were defined via a recent brain network partition. RSFC was determined for 718 regions via regularized partial correlation. Psychosis patients-both affective and non-affective-exhibited cortico-cortical hypoconnectivity and thalamo-cortical hyperconnectivity in somatomotor and visual2 networks but not in auditory or primary visual networks. When we averaged and normalized the visual2 and somatomotor network connections, and subtracted the thalamo-cortical and cortico-cortical connectivity values, a robust psychosis biomarker emerged (p = 2e-10, Hedges' g = 1.05). This "somato-visual" biomarker was present in antipsychotic-naive patients and did not depend on confounds such as psychiatric comorbidities, substance/nicotine use, stress, anxiety, or demographics. It had moderate test-retest reliability (ICC = 0.62) and could be recovered in five-minute scans. The marker could discriminate groups in leave-one-site-out cross-validation (AUC = 0.79) and improve group classification upon being added to a well-known neurocognition task. Finally, it could differentiate later-stage psychosis patients from healthy or ADHD controls in two independent data sets. These results introduce a simple and robust RSFC biomarker that can distinguish psychosis patients from controls by the early illness stages.

摘要

患有精神病的人表现出丘脑 - 皮质的高连接性以及与感觉网络的皮质 - 皮质低连接性,然而,尚不清楚这是否适用于所有感觉网络,是否由其他疾病因素引起,或者这种差异是否可以构成一种可行生物标志物的基础。为了解决上述问题,我们利用了人类连接组早期精神病项目的数据,并计算了54名健康对照者和105名精神病患者的静息态功能连接(RSFC)矩阵。通过最近的脑网络划分定义了初级视觉、次级视觉(“视觉2”)、听觉和躯体运动网络。通过正则化偏相关确定了718个区域的RSFC。情感性和非情感性精神病患者在躯体运动和视觉2网络中表现出皮质 - 皮质低连接性和丘脑 - 皮质高连接性,但在听觉或初级视觉网络中未表现出。当我们对视觉2和躯体运动网络连接进行平均和归一化,并减去丘脑 - 皮质和皮质 - 皮质连接值时,出现了一种强大的精神病生物标志物(p = 2e - 10,Hedges' g = 1.05)。这种“躯体 - 视觉”生物标志物存在于未服用抗精神病药物的患者中,并且不依赖于诸如精神疾病共病、物质/尼古丁使用、压力、焦虑或人口统计学等混杂因素。它具有中等的重测信度(ICC = 0.62),并且可以在五分钟扫描中恢复。该标志物在留一站点交叉验证中可以区分不同组(AUC = 0.79),并且在添加到一个著名的神经认知任务后可以改善组分类。最后,它可以在两个独立数据集中区分晚期精神病患者与健康或注意力缺陷多动障碍(ADHD)对照者。这些结果引入了一种简单而强大的RSFC生物标志物,该标志物可以在疾病早期阶段将精神病患者与对照者区分开来。

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