Differential usage of DNA modifications in neurons, astrocytes, and microglia.

IF 4.2 2区 生物学 Q1 GENETICS & HEREDITY Epigenetics & Chromatin Pub Date : 2023-11-13 DOI:10.1186/s13072-023-00522-6
Kyla B Tooley, Ana J Chucair-Elliott, Sarah R Ocañas, Adeline H Machalinski, Kevin D Pham, Walker Hoolehan, Adam M Kulpa, David R Stanford, Willard M Freeman
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Abstract

Background: Cellular identity is determined partly by cell type-specific epigenomic profiles that regulate gene expression. In neuroscience, there is a pressing need to isolate and characterize the epigenomes of specific CNS cell types in health and disease. In this study, we developed an in vivo tagging mouse model (Camk2a-NuTRAP) for paired isolation of neuronal DNA and RNA without cell sorting and then used this model to assess epigenomic regulation, DNA modifications in particular, of gene expression between neurons and glia.

Results: After validating the cell-specificity of the Camk2a-NuTRAP model, we performed TRAP-RNA-Seq and INTACT-whole genome oxidative bisulfite sequencing (WGoxBS) to assess the neuronal translatome and epigenome in the hippocampus of young mice (4 months old). WGoxBS findings were validated with enzymatic methyl-Seq (EM-Seq) and nanopore sequencing. Comparing neuronal data to microglial and astrocytic data from NuTRAP models, microglia had the highest global mCG levels followed by astrocytes and then neurons, with the opposite pattern observed for hmCG and mCH. Differentially modified regions between cell types were predominantly found within gene bodies and distal intergenic regions, rather than proximal promoters. Across cell types there was a negative correlation between DNA modifications (mCG, mCH, hmCG) and gene expression at proximal promoters. In contrast, a negative correlation of gene body mCG and a positive relationship between distal promoter and gene body hmCG with gene expression was observed. Furthermore, we identified a neuron-specific inverse relationship between mCH and gene expression across promoter and gene body regions.

Conclusions: Neurons, astrocytes, and microglia demonstrate different genome-wide levels of mCG, hmCG, and mCH that are reproducible across analytical methods. However, modification-gene expression relationships are conserved across cell types. Enrichment of differential modifications across cell types in gene bodies and distal regulatory elements, but not proximal promoters, highlights epigenomic patterning in these regions as potentially greater determinants of cell identity. These findings also demonstrate the importance of differentiating between mC and hmC in neuroepigenomic analyses, as up to 30% of what is conventionally interpreted as mCG can be hmCG, which often has a different relationship to gene expression than mCG.

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DNA修饰在神经元、星形胶质细胞和小胶质细胞中的差异用法。
背景:细胞身份部分由调节基因表达的细胞类型特异性表观基因组谱决定。在神经科学中,迫切需要分离和表征健康和疾病中特定中枢神经系统细胞类型的表观基因组。在这项研究中,我们建立了一个体内标记小鼠模型(Camk2a-NuTRAP),用于在不进行细胞分选的情况下成对分离神经元DNA和RNA,然后使用该模型评估表观基因组调控,特别是DNA修饰,神经元和胶质细胞之间的基因表达。结果:在验证了Camk2a-NuTRAP模型的细胞特异性后,我们进行了TRAP-RNA-Seq和完整-全基因组氧化亚硫酸盐测序(WGoxBS)来评估幼龄小鼠(4个月大)海马的神经元翻译组和表观基因组。WGoxBS的发现通过酶甲基测序(EM-Seq)和纳米孔测序进行了验证。将神经元数据与NuTRAP模型的小胶质细胞和星形胶质细胞数据进行比较,发现小胶质细胞的mCG水平最高,其次是星形胶质细胞,然后是神经元,而hmCG和mCH的模式相反。细胞类型之间的差异修饰区域主要存在于基因体和远端基因间区域,而不是近端启动子内。在不同的细胞类型中,DNA修饰(mCG、mCH、hmCG)与近端启动子基因表达呈负相关。相反,基因体mCG与基因表达呈负相关,而远端启动子和基因体hmCG与基因表达呈正相关。此外,我们还发现mCH与启动子和基因体区域的基因表达之间存在神经元特异性的反比关系。结论:神经元、星形胶质细胞和小胶质细胞表现出不同的mCG、hmCG和mCH全基因组水平,这在不同的分析方法中是可重复的。然而,修饰-基因表达关系在细胞类型中是保守的。基因体和远端调控元件(而非近端启动子)中不同细胞类型的差异修饰的富集,突出了这些区域的表观基因组模式作为细胞身份的潜在更大决定因素。这些发现也证明了在神经表观基因组分析中区分mCG和hmC的重要性,因为多达30%的传统解释为mCG的可能是hmCG,而hmCG与基因表达的关系通常与mCG不同。
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来源期刊
Epigenetics & Chromatin
Epigenetics & Chromatin GENETICS & HEREDITY-
CiteScore
7.00
自引率
0.00%
发文量
35
审稿时长
1 months
期刊介绍: Epigenetics & Chromatin is a peer-reviewed, open access, online journal that publishes research, and reviews, providing novel insights into epigenetic inheritance and chromatin-based interactions. The journal aims to understand how gene and chromosomal elements are regulated and their activities maintained during processes such as cell division, differentiation and environmental alteration.
期刊最新文献
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