MIR218 polygenic risk score is associated with cognitive function and neurochemical metabolites among patients with depressed bipolar disorders.

IF 4.9 2区 医学 Q1 CLINICAL NEUROLOGY Journal of affective disorders Pub Date : 2024-11-17 DOI:10.1016/j.jad.2024.11.046
Jianzhao Zhang, Shuming Zhong, Shunkai Lai, Yiliang Zhang, Guanmao Chen, Dong Huang, Shuya Yan, Pan Chen, Xiaodan Lu, Jie Yin, Chao Chen, Ying Wang, Yanbin Jia
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Abstract

Backgrounds: Evidence from animal and population studies has consistently revealed that microRNA 218 (MIR218) is involved in susceptibility to depression and cognitive functions. Nevertheless, few studies have evaluated the association between MIR218 and clinical features in patients with depressed bipolar disorder (BD).

Methods: A total of 66 patients with depressed BD and 49 healthy controls (HCs) were recruited for this study. MIR218 polygenic risk score (PRS) was used to assess the addictive effects of the MIR218 regulated genes. We compared the MIR218 PRS between patients with depressed BD and HCs to investigate whether it can be used to predict the risk of BD, and further explored the association between MIR218 PRS and cognitive performance as well as neurochemical metabolites among depressed BD.

Results: We found that there was a significant difference in MIR218 PRS between patients with depressed BD and HCs. The correlation analysis indicated that MIR218 PRS was negative associated with the number of disease onset (r = -0.311, P = 0.033) and choline (Cho)/creatine (Cr) in right thalamus (r = -0.285, P = 0.021). Additionally, as supported by previous findings, patients with lower MIR218 PRS presented more domains of impaired cognitive function than those with higher scores.

Conclusion: These findings suggested MIR218 PRS might be useful in differentiating patients with depressed BD from HCs. Moreover, depressed BD with lower MIR218 PRS showed more pronounced cognitive impairment than those with higher scores, which may be associated with disease recurrence and Cho metabolism in right thalamus.

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MIR218 多基因风险评分与抑郁型双相情感障碍患者的认知功能和神经化学代谢物有关。
背景:来自动物和人群研究的证据一致表明,microRNA 218(MIR218)与抑郁症易感性和认知功能有关。然而,很少有研究评估 MIR218 与抑郁性双相情感障碍(BD)患者临床特征之间的关联:方法:本研究共招募了 66 名抑郁型双相情感障碍(BD)患者和 49 名健康对照(HCs)。采用 MIR218 多基因风险评分(PRS)评估 MIR218 调控基因的成瘾效应。我们比较了 BD 抑郁症患者和 HCs 的 MIR218 PRS,以探讨其是否可用于预测 BD 的风险,并进一步探讨了 MIR218 PRS 与 BD 抑郁症患者的认知能力以及神经化学代谢物之间的关联:结果:我们发现 MIR218 PRS 在 BD 抑郁症患者和 HC 患者之间存在显著差异。相关性分析表明,MIR218 PRS与发病次数(r = -0.311,P = 0.033)和右丘脑胆碱(Cho)/肌酸(Cr)(r = -0.285,P = 0.021)呈负相关。此外,与之前的研究结果一样,MIR218 PRS较低的患者比得分较高的患者表现出更多的认知功能受损领域:这些研究结果表明,MIR218 PRS 可能有助于区分抑郁性 BD 患者和 HC 患者。此外,与得分较高者相比,MIR218 PRS较低的抑郁型BD患者表现出更明显的认知功能障碍,这可能与疾病复发和右侧丘脑的新陈代谢有关。
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来源期刊
Journal of affective disorders
Journal of affective disorders 医学-精神病学
CiteScore
10.90
自引率
6.10%
发文量
1319
审稿时长
9.3 weeks
期刊介绍: The Journal of Affective Disorders publishes papers concerned with affective disorders in the widest sense: depression, mania, mood spectrum, emotions and personality, anxiety and stress. It is interdisciplinary and aims to bring together different approaches for a diverse readership. Top quality papers will be accepted dealing with any aspect of affective disorders, including neuroimaging, cognitive neurosciences, genetics, molecular biology, experimental and clinical neurosciences, pharmacology, neuroimmunoendocrinology, intervention and treatment trials.
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