Patterns of Immune Dysregulation in Bipolar Disorder

Benney MR Argue, Lucas G Casten, Shaylah McCool, Aysheh Alrfooh, Jenny Gringer Richards, John A Wemmie, Vincent A Magnotta, Aislinn J Williams, Jake J Michaelson, Jess G Fiedorowicz, Sabrina M Scroggins, Marie Elizabeth Gaine
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Abstract

Background: Bipolar disorder is a debilitating mood disorder associated with a high risk of suicide and characterized by immune dysregulation. In this study, we used a multi-faceted approach to better distinguish the pattern of dysregulation of immune profiles in individuals with BD. Methods: We analyzed peripheral blood mononuclear cells (bipolar disorder N=39, control N=30), serum cytokines (bipolar disorder N=86, control N=58), whole blood RNA (bipolar disorder N=25, control N=25), and whole blood DNA (bipolar disorder N=104, control N=66) to identify immune-related differences in participants diagnosed with bipolar disorder compared to controls. Results: Flow cytometry revealed a higher proportion of monocytes in participants with bipolar disorder together with a lower proportion of T helper cells. Additionally, the levels of 18 cytokines were significantly elevated, while two were reduced in participants with bipolar disorder. Most of the cytokines altered in individuals with bipolar disorder were proinflammatory. Forty-nine genes were differentially expressed in our bipolar disorder cohort and further analyses uncovered several immune-related pathways altered in these individuals. Genetic analysis indicated variants associated with inflammatory bowel disease also influences bipolar disorder risk. Discussion: Our findings indicate a significant immune component to bipolar disorder pathophysiology and genetic overlap with inflammatory bowel disease. This comprehensive study supports existing literature, whilst also highlighting novel immune targets altered in individuals with bipolar disorder. Specifically, multiple lines of evidence indicate differences in the peripheral representation of monocytes and T cells are hallmarks of bipolar disorder.
双相情感障碍的免疫失调模式
背景:躁郁症是一种使人衰弱的情绪障碍,与自杀的高风险有关,其特点是免疫失调。在本研究中,我们采用了一种多层面的方法,以更好地区分躁郁症患者免疫特征失调的模式。研究方法我们分析了外周血单核细胞(躁郁症患者39人,对照组患者30人)、血清细胞因子(躁郁症患者86人,对照组患者58人)、全血RNA(躁郁症患者25人,对照组患者25人)和全血DNA(躁郁症患者104人,对照组患者66人),以确定被诊断为躁郁症的患者与对照组患者在免疫方面的差异。结果显示流式细胞术显示,躁郁症患者的单核细胞比例较高,T辅助细胞比例较低。此外,双相情感障碍患者体内有 18 种细胞因子的水平显著升高,而有两种细胞因子的水平降低。躁郁症患者体内发生变化的细胞因子大多具有促炎作用。在我们的双相情感障碍患者队列中,有 49 个基因的表达出现了差异,进一步的分析发现,这些患者体内有几种与免疫相关的通路发生了改变。遗传分析表明,与炎症性肠病相关的变异也会影响躁郁症的风险:讨论:我们的研究结果表明,双相情感障碍的病理生理学中存在重要的免疫成分,并且与炎症性肠病存在遗传重叠。这项综合研究支持了现有的文献,同时也强调了双相情感障碍患者体内发生改变的新型免疫靶点。具体来说,多种证据表明,单核细胞和T细胞在外周表现上的差异是躁狂症的特征。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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