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双相障碍患者自杀死亡的淋巴细胞 miRNA 表达谱分析、通路分析及与尸检脑发现的整合。

MicroRNA expression profiling of lymphoblasts from bipolar disorder patients who died by suicide, pathway analysis and integration with postmortem brain findings.

机构信息

Department of Biomedical Sciences, Section of Neuroscience and Clinical Pharmacology, University of Cagliari, Italy.

Department of Biomedical Sciences, Section of Neuroscience and Clinical Pharmacology, University of Cagliari, Italy; UCL Genomics, UCL Great Ormond Street Institute of Child Health, London, United Kingdom.

出版信息

Eur Neuropsychopharmacol. 2020 May;34:39-49. doi: 10.1016/j.euroneuro.2020.03.005. Epub 2020 Mar 30.

Abstract

Post-mortem brain studies suggest that miRNAs may be involved in suicide, but their role as peripheral biomarkers or targets of preventive pharmacological treatments in suicide has yet to be elucidated. We used nCounter miRNA Expression assay to measure miRNAs expression in lymphoblastoid cell lines (LCLs) from patients with Bipolar Disorder (BD) who died by suicide (SC, n = 7) and with low risk of suicide (LR, n = 11). Five miRNAs were differentially expressed in SC compared to LR (false discovery rate p<0.05). The two most significant miRNAs were measured with RT-qPCR in the same sample and in 12 healthy controls (HC): miR-4286 was increased while miR-186-5p was decreased in SC compared to LR and HC (ANOVA F = 14.92, p = 0.000043 and F = 3.95, p = 0.032 respectively). miR-4286 was also decreased in postmortem brains from 12 patients with BD who died by suicide compared to 13 controls, even though it did not reach statistical significance (FC=0.51, p = 0.07). Treatment with lithium of human neural progenitor cells reduced the expression of miR-4286 (FC=0.30, p = 0.038). Pathway analysis on predicted miR-4286 targets showed that "insulin resistance" was significantly enriched after correction for multiple testing. This pathway comprised 17 genes involved in lipid and glucose metabolism, several of which were also dysregulated in postmortem brains from patients with BD who died by suicide from the Stanley-foundation array collection. In conclusion, our study suggests that miR-4286 could be a biomarker of suicide but further studies are warranted to investigate its targeted genes and how these could be involved in the neurobiology of suicide.

摘要

死后大脑研究表明,miRNAs 可能与自杀有关,但它们作为预防药理学治疗自杀的外周生物标志物或靶点的作用尚未阐明。我们使用 nCounter miRNA 表达分析测定了自杀死亡的双相情感障碍 (BD) 患者 (SC,n=7) 和自杀风险低的患者 (LR,n=11) 的淋巴母细胞系 (LCL) 中 miRNAs 的表达。与 LR 相比,SC 中有 5 个 miRNAs 表达差异(假发现率 p<0.05)。在同一样本和 12 个健康对照者 (HC) 中,我们用 RT-qPCR 测量了这两个最显著的 miRNAs:与 LR 和 HC 相比,SC 中 miR-4286 增加而 miR-186-5p 减少 (ANOVA F=14.92,p=0.000043 和 F=3.95,p=0.032)。与 13 个对照者相比,12 例自杀死亡的 BD 患者死后脑组织中 miR-4286 也减少,尽管没有达到统计学意义 (FC=0.51,p=0.07)。人神经祖细胞用锂处理后降低了 miR-4286 的表达 (FC=0.30,p=0.038)。对预测的 miR-4286 靶标进行途径分析显示,经多重检验校正后,“胰岛素抵抗”显著富集。该途径包含 17 个参与脂质和葡萄糖代谢的基因,其中几个基因在 Stanley-foundation 阵列收集的自杀死亡 BD 患者死后脑组织中也失调。总之,我们的研究表明,miR-4286 可能是自杀的生物标志物,但需要进一步研究来探讨其靶基因以及这些基因如何参与自杀的神经生物学。

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