Literature DB >> 32737167

The Neocortical Progenitor Specification Program Is Established through Combined Modulation of SHH and FGF Signaling.

Odessa R Yabut1, Hui-Xuan Ng1, Keejung Yoon1,2, Jessica C Arela1, Thomas Ngo3, Samuel J Pleasure4,5.   

Abstract

Neuronal progenitors in the developing forebrain undergo dynamic competence states to ensure timely generation of specific excitatory and inhibitory neuronal subtypes from distinct neurogenic niches of the dorsal and ventral forebrain, respectively. Here we show evidence of progenitor plasticity when Sonic hedgehog (SHH) signaling is left unmodulated in the embryonic neocortex of the mammalian dorsal forebrain. We found that, at early stages of corticogenesis, loss of Suppressor of Fused (Sufu), a potent inhibitor of SHH signaling, in neocortical progenitors, altered the transcriptomic landscape of male mouse embryos. Ectopic activation of SHH signaling occurred, via degradation of Gli3R, resulting in significant upregulation of fibroblast growth factor 15 (FGF15) gene expression in all E12.5 Sufu-cKO neocortex regardless of sex. Consequently, activation of FGF signaling, and its downstream effector the MAPK signaling, facilitated expression of genes characteristic of ventral forebrain progenitors. Our studies identify the importance of modulating extrinsic niche signals such as SHH and FGF15, to maintain the competency and specification program of neocortical progenitors throughout corticogenesis.SIGNIFICANCE STATEMENT Low levels of FGF15 control progenitor proliferation and differentiation during neocortical development, but little is known on how FGF15 expression is maintained. Our studies identified SHH signaling as a critical activator of FGF15 expression during corticogenesis. We found that Sufu, via Gli3R, ensured low levels of FGF15 was expressed to prevent abnormal specification of neocortical progenitors. These studies advance our knowledge on the molecular mechanisms guiding the generation of specific neocortical neuronal lineages, their implications in neurodevelopmental diseases, and may guide future studies on how progenitor cells may be used for brain repair.
Copyright © 2020 the authors.

Entities:  

Keywords:  FGF; SHH; corticogenesis; lineage fates; neural progenitors; neurogenesis

Year:  2020        PMID: 32737167      PMCID: PMC7470916          DOI: 10.1523/JNEUROSCI.2888-19.2020

Source DB:  PubMed          Journal:  J Neurosci        ISSN: 0270-6474            Impact factor:   6.167


  40 in total

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Review 3.  Intermediate progenitors and Tbr2 in cortical development.

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5.  Suppressor of fused controls cerebellar neuronal differentiation in a manner modulated by GLI3 repressor and Fgf15.

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Review 6.  Regulation of cerebral cortical size and neuron number by fibroblast growth factors: implications for autism.

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7.  Abnormal positioning of diencephalic cell types in neocortical tissue in the dorsal telencephalon of mice lacking functional Gli3.

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8.  Relationship between Sonic hedgehog protein, brain-derived neurotrophic factor and oxidative stress in autism spectrum disorders.

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10.  Low-coverage single-cell mRNA sequencing reveals cellular heterogeneity and activated signaling pathways in developing cerebral cortex.

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Journal:  Nat Biotechnol       Date:  2014-08-03       Impact factor: 54.908

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Review 4.  Extracellular Control of Radial Glia Proliferation and Scaffolding During Cortical Development and Pathology.

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Journal:  Front Cell Dev Biol       Date:  2020-10-16

5.  Cell-Type-Specific Gene Expression in Developing Mouse Neocortex: Intermediate Progenitors Implicated in Axon Development.

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6.  Developmental Origins of Human Cortical Oligodendrocytes and Astrocytes.

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