Journal of neuroscience & cognitive studies最新文献

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Replicated risk CACNA1C variants for major psychiatric disorders may serve as potential therapeutic targets for the shared depressive endophenotype. 主要精神疾病的复制风险CACNA1C变异可能作为共同抑郁内表型的潜在治疗靶点。

Journal of neuroscience & cognitive studies

Pub Date : 2020-01-01 Epub Date: 2020-10-27

Xiaoyun Guo, Yingmei Fu, Yong Zhang, Tong Wang, Lu Lu, Xingqun Luo, Kesheng Wang, Juncao Huang, Ting Xie, Chengchou Zheng, Kebing Yang, Jinghui Tong, Lingjun Zuo, Longli Kang, Yunlong Tan, Kaida Jiang, Chiang-Shan R Li, Xingguang Luo

Genome-wide association studies (GWASs) have reported numerous associations between risk variants and major psychiatric disorders (MPDs) including schizophrenia (SCZ), bipolar disorder (BPD), major depressive disorder (MDD) and others. We reviewed all of the published GWASs, and extracted the genome-wide significant (p<10^-6) and replicated associations between risk SNPs and MPDs. We found the associations of 6 variants located in 6 genes, including L type voltage-gated calcium channel (LTCCs) subunit alpha1 C gene (CACNA1C), that were genome-wide significant (2.0×10 ^-8 ≤p≤1.0×10 ^-6 ) and replicated at single-point level across at least two GWASs. Among them, the associations between MPDs and rs1006737 within CACNA1C are most robust. Thus, as a next step, the expression of the replicated risk genes in human hippocampus was analyzed. We found CACNA1C had significant mRNA expression in human hippocampus in two independent cohorts. Finally, we tried to elucidate the roles of venlafaxine and ω-3 PUFAs in the mRNA expression regulation of the replicated risk genes in hippocampus. We used cDNA chip-based microarray profiling to explore the transcriptome-wide mRNA expression regulation by ω-3 PUFAs (0.72/kg/d) and venlafaxine (0.25/kg/d) treatment in chronic mild stress (CMS) rats. ω-3 PUFAs and venlafaxine treatment elicited significant CACNA1C up-regulation. We concluded that CACNA1C might confer the genetic vulnerability to the shared depressive symptoms across MPDs and CACNA1C might be the therapeutic target for depressive endophenotype as well.

全基因组关联研究(GWASs)已经报道了风险变异与包括精神分裂症(SCZ)、双相情感障碍(BPD)、重度抑郁症(MDD)等主要精神疾病(MPDs)之间的许多关联。我们回顾了所有已发表的GWASs，提取了全基因组显著性(p-6)，并复制了风险snp与mpd之间的关联。我们发现位于6个基因中的6个变异的关联，包括L型电压门控钙通道(LTCCs)亚基α 1c基因(CACNA1C)，这些变异在全基因组范围内显著(2.0×10 -8≤p≤1.0×10 -6)，并且在至少两个GWASs中以单点水平复制。其中，MPDs与rs1006737在CACNA1C中的相关性最强。因此，作为下一步，我们分析了人类海马中复制风险基因的表达。在两个独立的队列中，我们发现CACNA1C在人海马中有显著的mRNA表达。最后，我们试图阐明文拉法辛和ω-3 PUFAs在海马复制风险基因mRNA表达调控中的作用。采用cDNA芯片微阵列分析技术，探讨ω-3 PUFAs (0.72/kg/d)和文拉法辛(0.25/kg/d)对慢性轻度应激(CMS)大鼠转录组mRNA表达的调控作用。ω-3 PUFAs和文拉法辛处理引起CACNA1C显著上调。我们的结论是，CACNA1C可能赋予mpd之间共同抑郁症状的遗传易感性，CACNA1C也可能是抑郁内表型的治疗靶点。

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