A neuroimaging biomarker for striatal dysfunction in schizophrenia

神经影像学 精神分裂症(面向对象编程) 心理学 双相情感障碍 生物标志物 神经科学 纹状体 抗精神病药 多巴胺能 医学 精神科 多巴胺 肿瘤科 认知 生物 生物化学
作者
Ang Li,Andrew Zalesky,Weihua Yue,Oliver Howes,Hao Yan,Yong Liu,Lingzhong Fan,Kirstie Whitaker,Kaibin Xu,G. Nageswara Rao,Jin Li,Shu Liu,Meng Wang,Yuqing Sun,Ming Song,Peng Li,Jun Chen,Yunchun Chen,Huaning Wang,Wenming Liu,Zhigang Li,Yongfeng Yang,Hua Guo,Ping Wan,Luxian Lv,Lin Lü,Jun Yan,Yuqing Song,Huiling Wang,Hongxing Zhang,Huawang Wu,Yuping Ning,Yuhui Du,Yuqi Cheng,Jian Xu,Xiufeng Xu,Dai Zhang,Xiaoqun Wang,Tianzi Jiang,Bing Liu
出处
期刊:Nature Medicine [Springer Nature]
卷期号:26 (4): 558-565 被引量:185
标识
DOI:10.1038/s41591-020-0793-8
摘要

Mounting evidence suggests that function and connectivity of the striatum is disrupted in schizophrenia1–5. We have developed a new hypothesis-driven neuroimaging biomarker for schizophrenia identification, prognosis and subtyping based on functional striatal abnormalities (FSA). FSA scores provide a personalized index of striatal dysfunction, ranging from normal to highly pathological. Using inter-site cross-validation on functional magnetic resonance images acquired from seven independent scanners (n = 1,100), FSA distinguished individuals with schizophrenia from healthy controls with an accuracy exceeding 80% (sensitivity, 79.3%; specificity, 81.5%). In two longitudinal cohorts, inter-individual variation in baseline FSA scores was significantly associated with antipsychotic treatment response. FSA revealed a spectrum of severity in striatal dysfunction across neuropsychiatric disorders, where dysfunction was most severe in schizophrenia, milder in bipolar disorder, and indistinguishable from healthy individuals in depression, obsessive-compulsive disorder and attention-deficit hyperactivity disorder. Loci of striatal hyperactivity recapitulated the spatial distribution of dopaminergic function and the expression profiles of polygenic risk for schizophrenia. In conclusion, we have developed a new biomarker to index striatal dysfunction and established its utility in predicting antipsychotic treatment response, clinical stratification and elucidating striatal dysfunction in neuropsychiatric disorders. A new cross-validated neuroimaging biomarker that reflects striatal dysfunctioning can be used to distinguish patients with schizophrenia from healthy controls, and is associated with treatment response to antipsychotics.
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