A distinct transcriptome characterizes neural crest-derived cells at the migratory wavefront during enteric nervous system development

生物 神经嵴 细胞生物学 人口 转录组 祖细胞 肠神经系统 基因表达 神经科学 干细胞 遗传学 基因 胚胎 社会学 人口学
作者
Rhian Stavely,Ryo Hotta,Richard A. Guyer,Nicole Picard,Ahmed A. Rahman,Meredith Omer,Ádám Soós,Emőke Szőcs,Jessica L. Mueller,Allan M. Goldstein,Nándor Nagy
出处
期刊:Development [The Company of Biologists]
卷期号:150 (5) 被引量:10
标识
DOI:10.1242/dev.201090
摘要

ABSTRACT Enteric nervous system development relies on intestinal colonization by enteric neural crest-derived cells (ENCDCs). This is driven by a population of highly migratory and proliferative ENCDCs at the wavefront, but the molecular characteristics of these cells are unknown. ENCDCs from the wavefront and the trailing region were isolated and subjected to RNA-seq. Wavefront-ENCDCs were transcriptionally distinct from trailing ENCDCs, and temporal modelling confirmed their relative immaturity. This population of ENCDCs exhibited altered expression of ECM and cytoskeletal genes, consistent with a migratory phenotype. Unlike trailing ENCDCs, the wavefront lacked expression of genes related to neuronal or glial maturation. As wavefront ENCDC genes were associated with migration and developmental immaturity, the genes that remain expressed in later progenitor populations may be particularly pertinent to understanding the maintenance of ENCDC progenitor characteristics. Dusp6 expression was specifically upregulated at the wavefront. Inhibiting DUSP6 activity prevented wavefront colonization of the hindgut, and inhibited the migratory ability of post-colonized ENCDCs from midgut and postnatal neurospheres. These effects were reversed by simultaneous inhibition of ERK signaling, indicating that DUSP6-mediated ERK inhibition is required for ENCDC migration in mouse and chick.
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