bHLH transcription factor Her5 links patterning to regional inhibition of neurogenesis at the midbrain-hindbrain boundary

Geling, Andrea; Itoh, Motoyuki; Tallafuß, Alexandra; Chapouton, Prisca; Tannhäuser, Birgit; Kuwada, John Y.; Chitnis, Ajay B.; Bally‐Cuif, Laure

doi:10.1242/dev.00375

Cited by 78 publications

(110 citation statements)

References 70 publications

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“…Homozygous mutation of Tbx1 gene in mouse causes birth defects derived from developmental abnormalities of the embryonic pharyngeal sysIt has been shown that hairy controls the pattern of sensory organ formation by repressing achaete-scute (Orenic et al, 1993). In the zebrafish midbrain-hindbrain boundary, mouse olfactory placode and the inter-proneural stripes of Xenopus, Hairy and Enhancer of Split homologues (Hes/Her) repress neural fate (Cau et al, 2000, Geling et al, 2003, Bae et al, 2005. In chick otic cups, Hairy1 (Hes1 in mammals) is expressed restricted in the nonneural domain, disclosing a putative role in repressing proneural fate in the posterior region (Abelló et al, 2007).…”

Section: Model C: Successive Inductions and Repression Of Neural Fatementioning

confidence: 99%

Establishment of a proneural field in the inner ear

Abelló

Alsina²

2007

Int. J. Dev. Biol.

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Hair-cells, supporting cells and sensory neurons are the main specialized cell-types responsible for mechanotransduction in the inner ear. They derive from precursors expressing proneural genes and recent data has underlined the importance of SoxB1 genes as upstream activators of proneural genes during cranial placode development. Here we review the steps of establishing a proneural field and propose several models for how early otic regionalization into a proneural territory is achieved.

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Section: Model C: Successive Inductions and Repression Of Neural Fatementioning

confidence: 99%

Establishment of a proneural field in the inner ear

Abelló

Alsina²

2007

Int. J. Dev. Biol.

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“…Hes1 directly contributes to the promotion of progenitor cell proliferation through transcriptional repression of a cyclin-dependent kinase inhibitor, p27Kip1, in embryonic carcinoma cells (Murata et al, 2005). Zebrafish p27 xic1 expression is negatively regulated by Her5 in the midbrain-hindbrain boundary (Geling et al, 2003). These findings suggested that hes-related genes might be involved in maintaining neural crest stem cells in the mitotic and undifferentiated state.…”

Section: Introductionmentioning

confidence: 96%

Xenopus hairy2 functions in neural crest formation by maintaining cells in a mitotic and undifferentiated state

Nagatomo

Hashimoto

2007

Developmental Dynamics

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The neural crest is a population of mitotically active, multipotent progenitor cells that arise at the neural plate border. Neural crest progenitors must be maintained in a multipotent state until after neural tube closure. However, the molecular underpinnings of this process have yet to be fully elucidated. Here we show that the basic helix-loop-helix (bHLH) transcriptional repressor gene, Xenopus hairy2 (Xhairy2), is an essential early regulator of neural crest formation in Xenopus. During gastrulation, Xhairy2 is localized at the presumptive neural crest prior to the expression of such neural crest markers as Slug and FoxD3. Morpholino-mediated knockdown of Xhairy2 results in the repression of neural crest marker gene expression while inducing the ectopic expression of the cell cycle inhibitor p27 xic1 in the presumptive neural crest. We also found that ectopic p27 xic1 disturbs neural crest formation. Furthermore, the depletion of Xhairy2 leads to the apoptosis of mitotic cells. Our results suggest that Xhairy2 functions in neural crest specification by maintaining cells in the mitotic and undifferentiated state.

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“…For example, three neurogenic zones form along the dorsoventral axis of the spinal cord during primary neurogenesis due to inhibition of differentiation in the intervening regions by specific Hes/Her and Zic genes (Brewster et al, 1998;Bae et al, 2005). Similarly, a non-neurogenic zone forms at the midbrainhindbrain boundary due to the inhibitory action of Hes/Her family members (Geling et al, 2003;Geling et al, 2004). In these examples, the expression of transcription factors that inhibit neuronal differentiation appears to be linked to dorsoventral and anteroposterior patterning within the neural epithelium that underlies cell type and regional specification.…”

Section: Introductionmentioning

confidence: 99%

Signalling from hindbrain boundaries regulates neuronal clustering that patterns neurogenesis

Terriente

Gerety²,

Watanabe-Asaka³

et al. 2012

Development

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SUMMARYDuring central nervous system development, neural progenitors are patterned to form discrete neurogenic and non-neurogenic zones. In the zebrafish hindbrain, neurogenesis is organised by Fgf20a emanating from neurons located at each segment centre that inhibits neuronal differentiation in adjacent progenitors. Here, we have identified a molecular mechanism that clusters fgf20a-expressing neurons in segment centres and uncovered a requirement for this positioning in the regulation of neurogenesis. Disruption of hindbrain boundary cell formation alters the organisation of fgf20a-expressing neurons, consistent with a role of chemorepulsion from boundaries. The semaphorins Sema3fb and Sema3gb, which are expressed by boundary cells, and their receptor Nrp2a are required for clustering of fgf20a-expressing neurons at segment centres. The dispersal of fgf20a-expressing neurons that occurs following the disruption of boundaries or of Sema3fb/Sema3gb signalling leads to reduced FGF target gene expression in progenitors and an increased number of differentiating neurons. Sema3 signalling from boundaries thus links hindbrain segmentation to the positioning of fgf20a-expressing neurons that regulates neurogenesis.

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bHLH transcription factor Her5 links patterning to regional inhibition of neurogenesis at the midbrain-hindbrain boundary

Cited by 78 publications

References 70 publications

Establishment of a proneural field in the inner ear

Establishment of a proneural field in the inner ear

Xenopus hairy2 functions in neural crest formation by maintaining cells in a mitotic and undifferentiated state

Signalling from hindbrain boundaries regulates neuronal clustering that patterns neurogenesis

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