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动态转录特征和细胞命运分析揭示了单个神经板边缘细胞的可塑性。

Dynamic transcriptional signature and cell fate analysis reveals plasticity of individual neural plate border cells.

作者信息

Roellig Daniela, Tan-Cabugao Johanna, Esaian Sevan, Bronner Marianne E

机构信息

Division of Biology and Biological Engineering, California Institute of Technology, Pasadena, United States.

出版信息

Elife. 2017 Mar 29;6:e21620. doi: 10.7554/eLife.21620.

Abstract

The 'neural plate border' of vertebrate embryos contains precursors of neural crest and placode cells, both defining vertebrate characteristics. How these lineages segregate from neural and epidermal fates has been a matter of debate. We address this by performing a fine-scale quantitative temporal analysis of transcription factor expression in the neural plate border of chick embryos. The results reveal significant overlap of transcription factors characteristic of multiple lineages in individual border cells from gastrula through neurula stages. Cell fate analysis using a Sox2 (neural) enhancer reveals that cells that are initially Sox2+ cells can contribute not only to neural tube but also to neural crest and epidermis. Moreover, modulating levels of Sox2 or Pax7 alters the apportionment of neural tube versus neural crest fates. Our results resolve a long-standing question and suggest that many individual border cells maintain ability to contribute to multiple ectodermal lineages until or beyond neural tube closure.

摘要

脊椎动物胚胎的“神经板边界”包含神经嵴和基板细胞的前体,这两者都定义了脊椎动物的特征。这些细胞谱系如何从神经和表皮命运中分离出来一直是一个有争议的问题。我们通过对鸡胚神经板边界中的转录因子表达进行精细的定量时间分析来解决这个问题。结果显示,从原肠胚到神经胚阶段,单个边界细胞中多个谱系特有的转录因子存在显著重叠。使用Sox2(神经)增强子进行的细胞命运分析表明,最初为Sox2+的细胞不仅可以分化为神经管,还可以分化为神经嵴和表皮。此外,调节Sox2或Pax7的水平会改变神经管与神经嵴命运的分配。我们的结果解决了一个长期存在的问题,并表明许多单个边界细胞在神经管闭合之前或之后仍保持分化为多种外胚层谱系的能力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1e6b/5371430/b0744f32f930/elife-21620-fig1.jpg

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