Genetically Predicted Brain C4A Expression Is Associated With TSPO and Hippocampal Morphology

海马结构 形态学(生物学) 脑形态计量学 神经科学 生物 遗传学 医学 磁共振成像 放射科
作者
Tânia Maria Sarmento Silva,Elisa Guma,Sina Hafizi,Alex Koppel,Pablo Rusjan,James L. Kennedy,M. Mallar Chakravarty,Romina Mizrahi
出处
期刊:Biological Psychiatry [Elsevier]
卷期号:90 (9): 652-660 被引量:12
标识
DOI:10.1016/j.biopsych.2021.06.021
摘要

Background Alterations in the immune system, particularly C4A, have been implicated in the pathophysiology of schizophrenia. C4A promotes synapse elimination by microglia in preclinical models; however, it is unknown whether this process is also present in living humans and how it affects brain morphology. Methods Participants (N = 111; 33 patients with psychosis, 37 individuals at clinical high risk, and 41 healthy control subjects) underwent a TSPO [18F]FEPPA positron emission tomography scan and a magnetic resonance imaging scan. Brain C4A expression was genetically predicted as a function of the dosage of each of 4 structural elements (C4AL, C4BL, C4AS, C4BS). Results Higher genetically predicted brain C4A expression was associated with higher brain microglial marker (TSPO) and altered hippocampal morphology, including reduced surface area and medial displacement in the CA1 area. This study is the first to quantify genetically predicted brain C4A expression in individuals at clinical high risk, showing significantly lower C4A in individuals at clinical high risk compared with healthy control subjects. We also showed a robust effect of sex on genetically predicted brain C4A expression and effects of both sex and cannabis use on brain TSPO. Conclusions This study shows for the first time complement system (C4A) coupling with a microglial marker (TSPO) and hippocampal morphology in living human brain. These findings pave the way for future research on the interaction between C4A and glial cell function, which has the potential to inform the disease mechanism underlying psychosis and schizophrenia.

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