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单细胞多组学方法揭示常见Cre驱动对神经系统的多样化标记

Single-Cell Multiomic Approaches Reveal Diverse Labeling of the Nervous System by Common Cre-Drivers.

作者信息

Keuls Rachel A, Parchem Ronald J

机构信息

Development, Disease Models & Therapeutics Graduate Program, Baylor College of Medicine, Houston, TX, United States.

Center for Cell and Gene Therapy, Stem Cells and Regenerative Medicine Center, Baylor College of Medicine, Houston, TX, United States.

出版信息

Front Cell Neurosci. 2021 Apr 14;15:648570. doi: 10.3389/fncel.2021.648570. eCollection 2021.

Abstract

Neural crest development involves a series of dynamic, carefully coordinated events that result in human disease when not properly orchestrated. Cranial neural crest cells acquire unique multipotent developmental potential upon specification to generate a broad variety of cell types. Studies of early mammalian neural crest and nervous system development often use the Cre-loxP system to lineage trace and mark cells for further investigation. Here, we carefully profile the activity of two common neural crest Cre-drivers at the end of neurulation in mice. RNA sequencing of labeled cells at E9.5 reveals that Wnt1-Cre2 marks cells with neuronal characteristics consistent with neuroepithelial expression, whereas Sox10-Cre predominantly labels the migratory neural crest. We used single-cell mRNA and single-cell ATAC sequencing to profile the expression of and and identify transcription factors that may regulate the expression of Wnt1-Cre2 in the neuroepithelium and Sox10-Cre in the migratory neural crest. Our data identify cellular heterogeneity during cranial neural crest development and identify specific populations labeled by two Cre-drivers in the developing nervous system.

摘要

神经嵴发育涉及一系列动态、精心协调的事件,若这些事件未得到妥善编排,就会导致人类疾病。颅神经嵴细胞在特化时获得独特的多能发育潜能,以产生多种细胞类型。早期哺乳动物神经嵴和神经系统发育的研究通常使用Cre-loxP系统进行谱系追踪和标记细胞,以便进一步研究。在此,我们仔细分析了小鼠神经胚形成末期两种常见的神经嵴Cre驱动因子的活性。在E9.5对标记细胞进行RNA测序发现,Wnt1-Cre2标记的细胞具有与神经上皮表达一致的神经元特征,而Sox10-Cre主要标记迁移的神经嵴。我们使用单细胞mRNA和单细胞ATAC测序来分析基因的表达,并确定可能调节神经上皮中Wnt1-Cre2表达和迁移神经嵴中Sox10-Cre表达的转录因子。我们的数据确定了颅神经嵴发育过程中的细胞异质性,并确定了发育中的神经系统中由两种Cre驱动因子标记的特定细胞群。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/87de/8079645/4e966856baeb/fncel-15-648570-g0001.jpg

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