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大麻素受体 CNR1 在人类前额叶皮层、海马体和尾状核中的表达和 DNA 甲基化与大脑发育和精神分裂症有关。

Cannabinoid receptor CNR1 expression and DNA methylation in human prefrontal cortex, hippocampus and caudate in brain development and schizophrenia.

机构信息

The Lieber Institute for Brain Development, Johns Hopkins University Medical Campus, Baltimore, MD, USA.

Department of Mental Health, Johns Hopkins Bloomberg School of Public Health, Baltimore, MD, USA.

出版信息

Transl Psychiatry. 2020 May 19;10(1):158. doi: 10.1038/s41398-020-0832-8.

Abstract

Beyond being one the most widely used psychoactive drugs in the world, cannabis has been identified as an environmental risk factor for psychosis. Though the relationship between cannabis use and psychiatric disorders remains controversial, consistent association between early adolescent cannabis use and the subsequent risk of psychosis suggested adolescence may be a particularly vulnerable period. Previous findings on gene by environment interactions indicated that cannabis use may only increase the risk for psychosis in the subjects who have a specific genetic vulnerability. The type 1 cannabinoid receptor (CB1), encoded by the CNR1 gene, is a key component of the endocannabinoid system. As the primary endocannabinoid receptor in the brain, CB1 is the main molecular target of the endocannabinoid ligand, as well as tetrahydrocannabinol (THC), the principal psychoactive ingredient of cannabis. In this study, we have examined mRNA expression and DNA methylation of CNR1 in human prefrontal cortex (PFC), hippocampus, and caudate samples. The expression of CNR1 is higher in fetal PFC and hippocampus, then drops down dramatically after birth. The lifespan trajectory of CNR1 expression in the DLPFC differentially correlated with age by allelic variation at rs4680, a functional polymorphism in the COMT gene. Compared with COMT methionine carriers, Caucasian carriers of the COMT valine allele have a stronger negative correlation between the expression of CNR1 in DLPFC and age. In contrast, the methylation level of cg02498983, which is negatively correlated with the expression of CNR1 in PFC, showed the strongest positive correlation with age in PFC of Caucasian carriers of COMT valine. Additionally, we have observed decreased mRNA expression of CNR1 in the DLPFC of patients with schizophrenia. Further analysis revealed a positive eQTL SNP, rs806368, which predicted the expression of a novel transcript of CNR1 in human DLPFC, hippocampus and caudate. This SNP has been associated with addiction and other psychiatric disorders. THC or ethanol are each significantly associated with dysregulated expression of CNR1 in the PFC of patients with affective disorder, and the expression of CNR1 is significantly upregulated in the PFC of schizophrenia patients who completed suicide. Our results support previous studies that have implicated the endocannabinoid system in the pathology of schizophrenia and provided additional insight into the mechanism of increasing risk for schizophrenia in the adolescent cannabis users.

摘要

大麻不仅是世界上使用最广泛的精神活性药物之一,还被确定为精神疾病的环境风险因素。尽管大麻使用与精神疾病之间的关系仍然存在争议,但青少年早期大麻使用与随后的精神病风险之间的一致关联表明,青春期可能是一个特别脆弱的时期。先前关于基因-环境相互作用的研究结果表明,大麻的使用可能只会增加那些具有特定遗传易感性的个体患精神病的风险。I 型大麻素受体(CB1)由 CNR1 基因编码,是内源性大麻素系统的关键组成部分。作为大脑中的主要内源性大麻素受体,CB1 是内源性大麻素配体以及大麻的主要精神活性成分四氢大麻酚(THC)的主要分子靶点。在这项研究中,我们检查了人类前额叶皮层(PFC)、海马体和尾状核样本中 CNR1 的 mRNA 表达和 DNA 甲基化。CNR1 在胎儿 PFC 和海马体中的表达较高,然后在出生后急剧下降。在 DLPFC 中,CNR1 表达的寿命轨迹与 COMT 基因中的 rs4680 功能多态性的等位基因变异相关的年龄差异相关。与 COMT 蛋氨酸携带者相比,COMT 缬氨酸等位基因的白种人携带者在 DLPFC 中 CNR1 的表达与年龄之间呈更强的负相关。相比之下,与 PFC 中 CNR1 表达呈负相关的 cg02498983 的甲基化水平在 COMT 缬氨酸白种人携带者的 PFC 中与年龄呈最强的正相关。此外,我们观察到精神分裂症患者的 DLPFC 中 CNR1 的 mRNA 表达减少。进一步分析显示,一个正的 eQTL SNP rs806368 预测了 DLPFC、海马体和尾状核中 CNR1 新转录本的表达。该 SNP 与成瘾和其他精神疾病有关。THC 或乙醇均与情感障碍患者 PFC 中 CNR1 的失调表达显著相关,并且在完成自杀的精神分裂症患者的 PFC 中 CNR1 的表达显著上调。我们的结果支持先前的研究,这些研究表明内源性大麻素系统参与了精神分裂症的病理学,并为青少年大麻使用者患精神分裂症风险增加的机制提供了更多的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dc19/7237456/c2115eae94b6/41398_2020_832_Fig1_HTML.jpg

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