青少年狂饮乙醇会影响突触基因的 H3K9me3 占有率和少突胶质细胞的发育调控

IF 3.5 3区 医学 Q2 NEUROSCIENCES Frontiers in Molecular Neuroscience Pub Date : 2024-05-22 DOI:10.3389/fnmol.2024.1389100
Emily R Brocato, Rachel Easter, Alanna Morgan, Meenakshi Kakani, Grace Lee, Jennifer T. Wolstenholme
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引用次数: 0

摘要

青少年时期大量饮酒会破坏髓鞘形成,导致大脑结构变化,这种变化会持续到成年。年轻时饮酒会增加这些变化的易感性。为了解乙醇对髓鞘和白质的作用而建立的动物模型显示,青春期暴饮乙醇会改变少突胶质细胞的发育轨迹、髓鞘结构和髓鞘纤维密度。少突胶质细胞的分化受 H3K9 三甲基化(H3K9me3)的表观遗传调控。先前的研究表明,青少年酗酒会导致 H3K9 甲基化失调,并降低 PFC 中 H3K9 相关基因的表达。在这里,我们评估了乙醇诱导的青少年 PFC 发育中基因组位点的 H3K9me3 占有率变化。我们在少突胶质细胞富集细胞中采用qPCR时程方法进一步评估了乙醇诱导的转录水平变化,以具体评估少突胶质细胞祖细胞和少突胶质细胞的变化。青少年酗酒会以性别特异性的方式改变突触相关基因以及谷氨酸和钾通道特异性基因的H3K9me3调控。在前脑功能区组织中,我们发现与少突胶质细胞分化相关的转录因子的基因表达发生了早期变化,这可能导致后来髓鞘相关基因表达的显著下降。对少突胶质细胞富集时间过程和剂量反应研究的进一步探索可能表明,少突胶质细胞成熟在转录水平上存在持久的失调。总之,这些研究表明,狂饮乙醇可能会通过改变突触相关基因的 H3K9me3 占有率来阻碍少突胶质细胞的分化,而这种分化是 PFC 中髓鞘持续发育所必需的。我们发现了可能导致青少年酗酒乙醇相关髓鞘丢失的潜在基因。
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Adolescent binge ethanol impacts H3K9me3-occupancy at synaptic genes and the regulation of oligodendrocyte development
Binge drinking in adolescence can disrupt myelination and cause brain structural changes that persist into adulthood. Alcohol consumption at a younger age increases the susceptibility of these changes. Animal models to understand ethanol’s actions on myelin and white matter show that adolescent binge ethanol can alter the developmental trajectory of oligodendrocytes, myelin structure, and myelin fiber density. Oligodendrocyte differentiation is epigenetically regulated by H3K9 trimethylation (H3K9me3). Prior studies have shown that adolescent binge ethanol dysregulates H3K9 methylation and decreases H3K9-related gene expression in the PFC.Here, we assessed ethanol-induced changes to H3K9me3 occupancy at genomic loci in the developing adolescent PFC. We further assessed ethanol-induced changes at the transcription level with qPCR time course approaches in oligodendrocyte-enriched cells to assess changes in oligodendrocyte progenitor and oligodendrocytes specifically.Adolescent binge ethanol altered H3K9me3 regulation of synaptic-related genes and genes specific for glutamate and potassium channels in a sex-specific manner. In PFC tissue, we found an early change in gene expression in transcription factors associated with oligodendrocyte differentiation that may lead to the later significant decrease in myelin-related gene expression. This effect appeared stronger in males.Further exploration in oligodendrocyte cell enrichment time course and dose response studies could suggest lasting dysregulation of oligodendrocyte maturation at the transcriptional level. Overall, these studies suggest that binge ethanol may impede oligodendrocyte differentiation required for ongoing myelin development in the PFC by altering H3K9me3 occupancy at synaptic-related genes. We identify potential genes that may be contributing to adolescent binge ethanol-related myelin loss.
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来源期刊
CiteScore
5.70
自引率
2.10%
发文量
669
审稿时长
14 weeks
期刊介绍: Frontiers in Molecular Neuroscience is a first-tier electronic journal devoted to identifying key molecules, as well as their functions and interactions, that underlie the structure, design and function of the brain across all levels. The scope of our journal encompasses synaptic and cellular proteins, coding and non-coding RNA, and molecular mechanisms regulating cellular and dendritic RNA translation. In recent years, a plethora of new cellular and synaptic players have been identified from reduced systems, such as neuronal cultures, but the relevance of these molecules in terms of cellular and synaptic function and plasticity in the living brain and its circuits has not been validated. The effects of spine growth and density observed using gene products identified from in vitro work are frequently not reproduced in vivo. Our journal is particularly interested in studies on genetically engineered model organisms (C. elegans, Drosophila, mouse), in which alterations in key molecules underlying cellular and synaptic function and plasticity produce defined anatomical, physiological and behavioral changes. In the mouse, genetic alterations limited to particular neural circuits (olfactory bulb, motor cortex, cortical layers, hippocampal subfields, cerebellum), preferably regulated in time and on demand, are of special interest, as they sidestep potential compensatory developmental effects.
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