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Brain‐derived subgroups of bipolar II depression associate with inflammation and choroid plexus morphology

炎症 脉络丛 萧条(经济学) 医学 内科学 大脑大小 肿瘤坏死因子α 胃肠病学 磁共振成像 中枢神经系统 放射科 经济 宏观经济学
作者
Yuan Cao,Paulo Lizano,Guohua Deng,Huan Sun,Xiaoqin Zhou,Hongsheng Xie,Yaru Zhan,Jingshi Mu,Xipeng Long,Hongqi Xiao,Shiyu Liu,Qiyong Gong,Changjian Qiu,Zhiyun Jia
出处
期刊:Psychiatry and Clinical Neurosciences [Wiley]
卷期号:77 (11): 613-621 被引量:5
标识
DOI:10.1111/pcn.13585
摘要

Elevated inflammation and larger choroid plexus (ChP) volume has been previously identified in mood disorders. Connections between inflammation, ChP, and clinical symptoms in bipolar II depression (BDII-D) are unclear. Data-driven clustering based on neuroanatomical phenotypes may help to elucidate neurobiological associations in BDII-D.Inflammatory cytokines, clinical symptoms, and neuroanatomical features were assessed in 150 BDII-D patients. Sixty-eight cortical surface area (SA) and 19 subcortical volumes were extracted using FreeSurfer. The ChP volume was segmented manually using 3D Slicer. Regularized canonical correlation analysis was used to identify significantly correlated components between cortical SA and subcortical volumes (excluding the ChP), followed by k-means clustering to define brain-derived subgroups of BDII-D. Low-grade inflammation was derived by averaging the standardized z scores of interleukin (IL)-6, IL-1β, and tumor necrosis factor-α (TNF-α), which were computed to create a composite z-value score. Partial Pearson correlations followed by multiple comparison correction were conducted to explore associations between inflammation, clinical symptoms, and ChP volume.Subgroup I demonstrated smaller subcortical volume and cortical SA, higher inflammation, and larger ChP volume compared with subgroup II. Greater ChP volume was associated with a higher low-grade inflammation (mean r = 0.289, q = 0.003), CRP (mean r = 0.249, q = 0.007), IL-6 (left r = 0.200, q = 0.03), and TNF-α (right r = 0.226, q = 0.01), while greater IL-1β was significantly associated with severe depressive symptoms in BDII-D (r = 0.218, q = 0.045).Neuroanatomically-derived subgroups of BDII-D differed in their inflammation levels and ChP volume. These findings suggest an important role of elevated peripheral inflammation and larger ChP in BDII-D.
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