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染色质可及性动态和单细胞 RNA-Seq 揭示了神经祖细胞再生的新调节因子。

Chromatin accessibility dynamics and single cell RNA-Seq reveal new regulators of regeneration in neural progenitors.

机构信息

Department of Biochemistry, University of Washington, Seattle, United States.

Oregon Health Sciences Center For Early Detection Advanced Research Center (CEDAR), Portland, United States.

出版信息

Elife. 2020 Apr 27;9:e52648. doi: 10.7554/eLife.52648.

Abstract

Vertebrate appendage regeneration requires precisely coordinated remodeling of the transcriptional landscape to enable the growth and differentiation of new tissue, a process executed over multiple days and across dozens of cell types. The heterogeneity of tissues and temporally-sensitive fate decisions involved has made it difficult to articulate the gene regulatory programs enabling regeneration of individual cell types. To better understand how a regenerative program is fulfilled by neural progenitor cells (NPCs) of the spinal cord, we analyzed -expressing NPCs isolated from regenerating tails. By intersecting chromatin accessibility data with single-cell transcriptomics, we find that NPCs place an early priority on neuronal differentiation. Late in regeneration, the priority returns to proliferation. Our analyses identify Pbx3 and Meis1 as critical regulators of tail regeneration and axon organization. Overall, we use transcriptional regulatory dynamics to present a new model for cell fate decisions and their regulators in NPCs during regeneration.

摘要

脊椎动物附肢的再生需要精确协调的转录景观重塑,以促进新组织的生长和分化,这个过程需要持续数天,并涉及数十种细胞类型。组织的异质性和时间敏感的命运决定使得阐明单个细胞类型再生的基因调控程序变得困难。为了更好地理解脊髓神经祖细胞 (NPCs) 如何完成再生程序,我们分析了从再生的尾巴中分离出的 NPCs 中表达的基因。通过将染色质可及性数据与单细胞转录组学交叉分析,我们发现 NPCs 优先进行神经元分化。在再生后期,优先级又回到了增殖。我们的分析确定了 PBX3 和 MEIS1 是尾巴再生和轴突组织的关键调节因子。总的来说,我们利用转录调控动力学为 NPCs 在再生过程中的细胞命运决定及其调控因子提出了一个新的模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/be5f/7250574/b62a4c017500/elife-52648-fig1.jpg

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