Darren Cameron, Ngoc-Nga Vinh, Parinda Prapaiwongs, Elizabeth A Perry, James T R Walters, Meng Li, Michael C O'Donovan, Nicholas J Bray
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We additionally performed the single nuclei Assay for Transposase-Accessible Chromatin with Sequencing (snATAC-Seq) to map potential regulatory genomic regions operating in individual cell populations of the human GE, using these to test for enrichment of schizophrenia common genetic variant liability and to functionally annotate non-coding variants-associated with the disorder.</p><p><strong>Study results: </strong>Schizophrenia common variant liability was enriched in genes with high expression specificity for developing neuron populations that are predicted to form dopamine D1 and D2 receptor-expressing GABAergic medium spiny neurons of the striatum, cortical somatostatin-positive GABAergic interneurons, calretinin-positive GABAergic neurons, and cholinergic neurons. 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引用次数: 0
摘要
背景:神经节突起(GE)是胎儿特异性结构,可产生前脑的γ-氨基丁酸(GABA)和乙酰胆碱释放神经元。鉴于有证据表明精神分裂症患者存在 GABA 能、胆碱能和神经发育障碍,我们测试了 GE 神经元的发育是否可能参与介导精神分裂症的遗传风险:研究设计:我们将最近一项大规模精神分裂症全基因组关联研究的数据与来自人类GE的单细胞RNA测序数据结合起来,以检验精神分裂症风险变异是否富集在对发育中的GE细胞群具有高表达特异性的基因中。此外,我们还进行了单核转座酶可及染色质测序分析(snATAC-Seq),以绘制人类基因组学单个细胞群中潜在的调控基因组区域图谱,并利用这些图谱检测精神分裂症常见遗传变异的富集情况,同时对与精神分裂症相关的非编码变异进行功能注释:研究结果:精神分裂症常见基因变异责任富集在对发育中神经元群具有高表达特异性的基因中,这些神经元群预计会形成纹状体中表达多巴胺D1和D2受体的GABA能中棘神经元、皮质体生长抑素阳性GABA能中间神经元、钙视蛋白阳性GABA能神经元和胆碱能神经元。与这些发现一致的是,精神分裂症的遗传风险集中在GE发育中神经元群中的预测调控基因组序列中:我们的研究表明,GABA能神经元和胆碱能神经元特定群体的产前发育与日后的精神分裂症易感性有关,并提供了在GE细胞中运行的预测调控基因组元素图谱。
Genetic Implication of Prenatal GABAergic and Cholinergic Neuron Development in Susceptibility to Schizophrenia.
Background: The ganglionic eminences (GE) are fetal-specific structures that give rise to gamma-aminobutyric acid (GABA)- and acetylcholine-releasing neurons of the forebrain. Given the evidence for GABAergic, cholinergic, and neurodevelopmental disturbances in schizophrenia, we tested the potential involvement of GE neuron development in mediating genetic risk for the condition.
Study design: We combined data from a recent large-scale genome-wide association study of schizophrenia with single-cell RNA sequencing data from the human GE to test the enrichment of schizophrenia risk variation in genes with high expression specificity for developing GE cell populations. We additionally performed the single nuclei Assay for Transposase-Accessible Chromatin with Sequencing (snATAC-Seq) to map potential regulatory genomic regions operating in individual cell populations of the human GE, using these to test for enrichment of schizophrenia common genetic variant liability and to functionally annotate non-coding variants-associated with the disorder.
Study results: Schizophrenia common variant liability was enriched in genes with high expression specificity for developing neuron populations that are predicted to form dopamine D1 and D2 receptor-expressing GABAergic medium spiny neurons of the striatum, cortical somatostatin-positive GABAergic interneurons, calretinin-positive GABAergic neurons, and cholinergic neurons. Consistent with these findings, schizophrenia genetic risk was concentrated in predicted regulatory genomic sequence mapped in developing neuronal populations of the GE.
Conclusions: Our study implicates prenatal development of specific populations of GABAergic and cholinergic neurons in later susceptibility to schizophrenia, and provides a map of predicted regulatory genomic elements operating in cells of the GE.
期刊介绍:
Schizophrenia Bulletin seeks to review recent developments and empirically based hypotheses regarding the etiology and treatment of schizophrenia. We view the field as broad and deep, and will publish new knowledge ranging from the molecular basis to social and cultural factors. We will give new emphasis to translational reports which simultaneously highlight basic neurobiological mechanisms and clinical manifestations. Some of the Bulletin content is invited as special features or manuscripts organized as a theme by special guest editors. Most pages of the Bulletin are devoted to unsolicited manuscripts of high quality that report original data or where we can provide a special venue for a major study or workshop report. Supplement issues are sometimes provided for manuscripts reporting from a recent conference.