4.3 Article

Early molecular events during retinoic acid induced differentiation of neuromesodermal progenitors

Journal

BIOLOGY OPEN
Volume 5, Issue 12, Pages 1821-1833

Publisher

COMPANY OF BIOLOGISTS LTD
DOI: 10.1242/bio.020891

Keywords

Embryonic stem cells; Neuromesodermal progenitors; Raldh2 knockout embryos; Retinoic acid target genes; Nkx1-2; Zfp503; Zfp703; Gbx2; Id1; Retinoic acid response elements

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Funding

  1. National Institute of General Medical Sciences [GM062848]

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Bipotent neuromesodermal progenitors (NMPs) residing in the caudal epiblast drive coordinated body axis extension by generating both posterior neuroectoderm and presomitic mesoderm. Retinoic acid (RA) is required for body axis extension, however the early molecular response to RA signaling is poorly defined, as is its relationship to NMP biology. As endogenous RA is first seen near the time when NMPs appear, we used WNT/FGF agonists to differentiate embryonic stem cells to NMPs which were then treated with a short 2-h pulse of 25 nM RA or 1 mu M RA followed by RNA-seq transcriptome analysis. Differential expression analysis of this dataset indicated that treatment with 25 nM RA, but not 1 mu M RA, provided physiologically relevant findings. The 25 nM RA dataset yielded a cohort of previously known caudal RA target genes including Fgf8 (repressed) and Sox2 (activated), plus novel early RA signaling targets with nearby conserved RA response elements. Importantly, validation of top-ranked genes in vivo using RA- deficient Raldh2(-/-) embryos identified novel examples of RA activation (Nkx1-2, Zfp503, Zfp703, Gbx2, Fgf15, Nt5e) or RA repression (Id1) of genes expressed in the NMP niche or progeny. These findings provide evidence for early instructive and permissive roles of RA in controlling differentiation of NMPs to neural and mesodermal lineages.

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