双相情感障碍
后代
认知
心理学
精神分裂症(面向对象编程)
临床心理学
齿轮
社会心理的
睡眠剥夺对认知功能的影响
精神科
遗传学
生物
怀孕
人工智能
计算机科学
作者
Isabel Valli,Elena de la Serna,Alex G. Segura,Jose Pariente,Angels Calvet-Mirabent,Roger Borràs,Daniel Ilzarbe,Dolores Moreno,Nuria Martín-Martínez,Inmaculada Baeza,Mireia Rosa-Justicia,Clemente García-Rizo,Covadonga M. Díaz-Caneja,Nicolas Crossley,Allan H. Young,Eduard Vieta,Sergi Mas,Josefina Castro-Fornieles,Gisela Sugranyes
标识
DOI:10.1016/j.jaac.2022.05.011
摘要
Objective Cognitive impairment is an important feature of schizophrenia (SZ) and bipolar disorder (BP) with severity across the two disorders characterized by significant heterogeneity. Youth at family risk for SZ and BP were clustered based on cognitive function and examined in terms of the clinical, genetic, and brain imaging correlates of cluster membership. Method One hundred sixty participants, 32 offspring of patients with SZ, 59 offspring of patients with BP and 69 offspring of healthy control parents underwent clinical and cognitive assessments, genotyping and structural MRI. K-means clustering was used to group family risk participants based on cognitive measures. Clusters were compared in terms of cortical and subcortical brain measures as well as polygenic risk scores. Results Participants were grouped in 3 clusters with intact, intermediate, and impaired cognitive performance. The intermediate and impaired clusters had lower total brain surface area compared with the intact cluster, with prominent localization in frontal and temporal cortices. No between-cluster differences were identified in cortical thickness and subcortical brain volumes. The impaired cluster also had poorer psychosocial functioning and worse PRS-COG compared with the other 2 clusters and with offspring of healthy control parents, while there was no significant between-cluster difference in terms of PRS-SZ and PRS-BP. PRS-COG predicted psychosocial functioning, yet this effect did not appear to be mediated by an effect of PRS-COG on brain area. Conclusion Stratification based on cognition may help to elucidate the biological underpinnings of cognitive heterogeneity across SZ and BP risk.
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