Identification of lncRNA in circulating exosomes as potential biomarkers for MCI among the elderly

IF 4.9 2区 医学 Q1 CLINICAL NEUROLOGY Journal of affective disorders Pub Date : 2024-11-09 DOI:10.1016/j.jad.2024.11.029
Jian Gao , Peiliang Chen , Zhihao Li , Wenfang Zhong , Qingmei Huang , Xiru Zhang , Yishi Zhong , Yinru Wu , Yingjun Chen , Weiqi Song , Fangfei You , Shangjie Li , Fen Liang , Ying Nan , Jiaojiao Ren , Xiaomeng Wang , Qiaoqiao Shen , Qi Fu , Xiaoxia Zhang , Yijiang Ouyang , Chen Mao
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Abstract

Background

The abnormal expression of lncRNA in elderly patients with mild cognitive impairment (MCI), and the ability of exosomes to stably carry non-coding RNAs provide a reliable physiological basis for exosomal lncRNA in plasma as a biomarker of MCI.

Methods

This case-control study enrolled 155 patients with MCI and 155 healthy controls from a community-based population aged≥60 years. The expression profiles of lncRNA and mRNA in plasma exosomes were analyzed and validated using high-throughput RNA sequencing and qRT-PCR. Pathway enrichment analysis were performed on differentially expressed transcripts to screen for target lncRNAs and genes. Multivariate logistic regression models were used to construct clinical predictive models. The receiver operating characteristic curve was used to analyze the predictive value, with an 184-sample external database validated.

Results

132 lncRNAs and 459 mRNAs were significantly changed in plasma exosomes of MCI patients compared to healthy controls. LINC001380, ENST00000484033, and ENST00000531087 were screened as candidate exo-lncRNAs for predicting MCI. In logistic regression models, odds ratios and 95%CI for target exo-IncRNAs in MCI patients compared to healthy controls were 1.15(1.03–1.28) for LINC001380, 1.21(1.10–1.34) for ENST00000484033, and 1.23(1.08–1.40) for ENST00000531087, respectively. ROC curve analysis showed that the AUC of the combined predicted probability of target lncRNAs was 70.0 %(64.1 %–76.0 %). In the external database, the AUC for the target genes ATP2A2 and PSEN1 was 69.5 %(61.8 %–77.15 %).

Conclusion

This study provided evidence for the specific expression of plasma exosomal lncRNAs in MCI and its possible biological mechanism. The combined detection of the expression levels of lncRNA-LINC001380, lncRNA-ENST00000484033, and lncRNA-ENST00000531087 in plasma exosomes may provide early diagnosis and prevention of cognitive impairment.
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将循环外泌体中的 lncRNA 鉴定为老年人 MCI 的潜在生物标记物。
背景:lncRNA在老年轻度认知障碍(MCI)患者中的异常表达以及外泌体稳定携带非编码RNA的能力为血浆中的外泌体lncRNA作为MCI的生物标志物提供了可靠的生理基础:这项病例对照研究从年龄≥60岁的社区人群中招募了155名MCI患者和155名健康对照者。采用高通量RNA测序和qRT-PCR技术分析并验证了血浆外泌体中lncRNA和mRNA的表达谱。对差异表达的转录本进行通路富集分析,以筛选目标lncRNA和基因。多变量逻辑回归模型用于构建临床预测模型。利用接收者操作特征曲线分析预测价值,并通过184个样本的外部数据库进行验证:与健康对照组相比,MCI患者血浆外泌体中的132个lncRNA和459个mRNA发生了显著变化。LINC001380、ENST00000484033和ENST00000531087被筛选为预测MCI的候选外泌体lncRNA。在逻辑回归模型中,与健康对照组相比,MCI患者的目标外显子核糖核酸的几率比和95%CI分别为:LINC001380为1.15(1.03-1.28),ENST00000484033为1.21(1.10-1.34),ENST00000531087为1.23(1.08-1.40)。ROC曲线分析表明,目标lncRNA的综合预测概率的AUC为70.0%(64.1%-76.0%)。在外部数据库中,靶基因ATP2A2和PSEN1的AUC为69.5%(61.8%-77.15%):该研究为血浆外泌体 lncRNA 在 MCI 中的特异性表达及其可能的生物学机制提供了证据。联合检测血浆外泌体中lncRNA-LINC001380、lncRNA-ENST00000484033和lncRNA-ENST00000531087的表达水平可为认知障碍的早期诊断和预防提供依据。
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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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