lncLingo2及其衍生的miR-876-5p在获得阿片强化中的作用

IF 3.1 3区 医学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Hongyu Yang, Xiuning Zhang, Minglong Zhang, Yun Lu, Bing Xie, Shaoguang Sun, Hailei Yu, Bin Cong, Yixiao Luo, Chunling Ma, Di Wen
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引用次数: 0

摘要

最近的研究发现,非编码RNA(ncRNA)通过对基因表达的表观遗传调控和药物诱导的神经适应在药物成瘾中发挥着至关重要的作用。在这项研究中,我们描述了表现出吗啡条件性位置偏好(CPP)的小鼠的伏隔核(NAc)中的lncRNA转录组特征,并探索了新型差异表达的lncRNA、lncLingo2及其衍生的miR-876-5p在阿片类药物相关行为的获得中的前瞻性作用。我们发现,lncLingo2在NAc核心(NAcC)中下调,而在NAc外壳(NAcS)中没有下调。这种下调与吗啡CPP和海洛因静脉自我给药(IVSA)的发生有关。由于Mfold软件显示lncLingo2的二级结构包含前miR-876的序列,因此将LV-lncLingo2转染到HEK293细胞可显著上调miR-876的表达,而成熟miR-876的变化与吗啡CPP训练小鼠NarcC中lncLingo2的表达呈正相关。将miR-876-5p模拟物送入NAcC也能抑制吗啡CPP的获得。此外,生物信息学分析和双荧光素酶检测证实,miR-876-5p可选择性地与其靶基因Kcnn3结合,并调节吗啡CPP训练诱导的Kcnn3表达变化。最后,电生理分析表明,小电导钙激活钾通道(SK)电流增加,导致CPP训练后NAcC神经元兴奋性降低,而lncLingo2过表达可逆转这些变化。综上所述,lncLingo2可能是NAcC中miR-876-5p的前体,从而调节小鼠阿片相关行为的发展,这可能是阿片成瘾的潜在生物标志物和治疗靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Roles of lncLingo2 and its derived miR-876-5p in the acquisition of opioid reinforcement

Roles of lncLingo2 and its derived miR-876-5p in the acquisition of opioid reinforcement

Recent studies found that non-coding RNAs (ncRNAs) played crucial roles in drug addiction through epigenetic regulation of gene expression and underlying drug-induced neuroadaptations. In this study, we characterized lncRNA transcriptome profiles in the nucleus accumbens (NAc) of mice exhibiting morphine-conditioned place preference (CPP) and explored the prospective roles of novel differentially expressed lncRNA, lncLingo2 and its derived miR-876-5p in the acquisition of opioids-associated behaviours. We found that the lncLingo2 was downregulated within the NAc core (NAcC) but not in the NAc shell (NAcS). This downregulation was found to be associated with the development of morphine CPP and heroin intravenous self-administration (IVSA). As Mfold software revealed that the secondary structures of lncLingo2 contained the sequence of pre-miR-876, transfection of LV-lncLingo2 into HEK293 cells significantly upregulated miR-876 expression and the changes of mature miR-876 are positively correlated with lncLingo2 expression in NAcC of morphine CPP trained mice. Delivering miR-876-5p mimics into NAcC also inhibited the acquisition of morphine CPP. Furthermore, bioinformatics analysis and dual-luciferase assay confirmed that miR-876-5p binds to its target gene, Kcnn3, selectively and regulates morphine CPP training-induced alteration of Kcnn3 expression. Lastly, the electrophysiological analysis indicated that the currents of small conductance calcium-activated potassium (SK) channel was increased, which led to low neuronal excitability in NAcC after CPP training, and these changes were reversed by lncLingo2 overexpression. Collectively, lncLingo2 may function as a precursor of miR-876-5p in NAcC, hence modulating the development of opioid-associated behaviours in mice, which may serve as an underlying biomarker and therapeutic target of opioid addiction.

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来源期刊
Addiction Biology
Addiction Biology 生物-生化与分子生物学
CiteScore
8.10
自引率
2.90%
发文量
118
审稿时长
6-12 weeks
期刊介绍: Addiction Biology is focused on neuroscience contributions and it aims to advance our understanding of the action of drugs of abuse and addictive processes. Papers are accepted in both animal experimentation or clinical research. The content is geared towards behavioral, molecular, genetic, biochemical, neuro-biological and pharmacology aspects of these fields. Addiction Biology includes peer-reviewed original research reports and reviews. Addiction Biology is published on behalf of the Society for the Study of Addiction to Alcohol and other Drugs (SSA). Members of the Society for the Study of Addiction receive the Journal as part of their annual membership subscription.
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