HOXC8 initiates an ectopic mammary program by regulating Fgf10 and Tbx3 expression, and Wnt/β-catenin signaling

Carroll, Lara; Capecchi, Mario R.

doi:10.1242/dev.128298

Cited by 21 publications

(15 citation statements)

References 74 publications

(79 reference statements)

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“…This expression pattern likely paralleled the rapid down-regulation of Hoxd8 transcription occurring in the MB between E12.5 and E13.5. This dataset, along with previous contributions (36)(37)(38), indicates that Hox genes are differentially expressed both among the various pairs of MBs and during the development of these structures, suggesting that temporal and spatial Hox combinations may contribute to MG development and specification.…”

Section: Resultssupporting

confidence: 62%

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Control of Hoxd gene transcription in the mammary bud by hijacking a preexisting regulatory landscape

Schep

Necşulea

Rodríguez-Carballo

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Vertebrate Hox genes encode transcription factors operating during the development of multiple organs and structures. However, the evolutionary mechanism underlying this remarkable pleiotropy remains to be fully understood. Here, we show that Hoxd8 and Hoxd9, two genes of the HoxD complex, are transcribed during mammary bud (MB) development. However, unlike in other developmental contexts, their coexpression does not rely on the same regulatory mechanism. Hoxd8 is regulated by the combined activity of closely located sequences and the most distant telomeric gene desert. On the other hand, Hoxd9 is controlled by an enhancer-rich region that is also located within the telomeric gene desert but has no impact on Hoxd8 transcription, thus constituting an exception to the global regulatory logic systematically observed at this locus. The latter DNA region is also involved in Hoxd gene regulation in other contexts and strongly interacts with Hoxd9 in all tissues analyzed thus far, indicating that its regulatory activity was already operational before the appearance of mammary glands. Within this DNA region and neighboring a strong limb enhancer, we identified a short sequence conserved in therian mammals and capable of enhancer activity in the MBs. We propose that Hoxd gene regulation in embryonic MBs evolved by hijacking a preexisting regulatory landscape that was already at work before the emergence of mammals in structures such as the limbs or the intestinal tract.enhancers | TAD | mammalian development | mammary gland

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Section: Resultssupporting

confidence: 62%

“…Likewise, these genes have been implicated in MG development (36)(37)(38), with Hoxc8 being one of the first markers of MP specification, where it contributes to define the number and positions where these structures will form (37). The expression of Hoxc8 is nevertheless completely abrogated by E12.5.…”

Section: Significancementioning

confidence: 99%

Control of Hoxd gene transcription in the mammary bud by hijacking a preexisting regulatory landscape

Schep

Necşulea

Rodríguez-Carballo

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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“…Strikingly, very few candidate target genes are components or essential regulators of the Wnt/β-catenin, FGF, and TGF-β/Activin/BMP signaling pathways that have been identified as downstream pathways of several HOX proteins in embryonic development, neural differentiation and tumorigenesis ( Chen et al, 2005 ; Schiedlmeier et al, 2007 ; Bami et al, 2011 ; Makki and Capecchi, 2011 ; Donaldson et al, 2012 ; Carroll and Capecchi, 2015 ; Duan et al, 2015 ; Hrycaj et al, 2015 ; Roux et al, 2015 ; Karmakar et al, 2017 ; Zhang et al, 2017 ). Moreover, except from Pcp2 (see Supplementary Table S3 , line 17), none of the already identified direct or indirect targets of HOXA5 was significantly downregulated in our analysis (e.g., Ptn, Fslt1 ) ( Sanlioglu et al, 1998 ; Chen et al, 2005 ; Boucherat et al, 2013 ).…”

Section: Discussionmentioning

confidence: 99%

Conditional Loss of Hoxa5 Function Early after Birth Impacts on Expression of Genes with Synaptic Function

Lizen

Moens

Mouheiche

et al. 2017

Front. Mol. Neurosci.

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Hoxa5 is a member of the Hox gene family that plays critical roles in successive steps of the central nervous system formation during embryonic and fetal development. In the mouse, Hoxa5 was recently shown to be expressed in the medulla oblongata and the pons from fetal stages to adulthood. In these territories, Hoxa5 transcripts are enriched in many precerebellar neurons and several nuclei involved in autonomic functions, while the HOXA5 protein is detected mainly in glutamatergic and GABAergic neurons. However, whether HOXA5 is functionally required in these neurons after birth remains unknown. As a first approach to tackle this question, we aimed at determining the molecular programs downstream of the HOXA5 transcription factor in the context of the postnatal brainstem. A comparative transcriptomic analysis was performed in combination with gene expression localization, using a conditional postnatal Hoxa5 loss-of-function mouse model. After inactivation of Hoxa5 at postnatal days (P)1–P4, we established the transcriptome of the brainstem from P21 Hoxa5 conditional mutants using RNA-Seq analysis. One major finding was the downregulation of several genes associated with synaptic function in Hoxa5 mutant specimens including different actors involved in glutamatergic synapse, calcium signaling pathway, and GABAergic synapse. Data were confirmed and extended by reverse transcription quantitative polymerase chain reaction analysis, and the expression of several HOXA5 candidate targets was shown to co-localize with Hoxa5 transcripts in precerebellar nuclei. Together, these new results revealed that HOXA5, through the regulation of key actors of the glutamatergic/GABAergic synapses and calcium signaling, might be involved in synaptogenesis, synaptic transmission, and synaptic plasticity of the cortico-ponto-cerebellar circuitry in the postnatal brainstem.

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“…In both the CNCC‐ and the PM‐specific Ezh2 mutants, multiple Hox genes are upregulated (Dudakovic et al, ; Schwarz et al, ). Hox genes have been associated with repression of Runx2 in skull bone in vivo (Carroll & Capecchi, ; Santagati, Minoux, Ren, & Rijli, ). In addition, the SOA‐mesenchyme lacks expression of all Hox genes, resulting in a potential sensitivity to ectopic Hox gene expression.…”

Section: H3k27me3 Is the Primary Epigenetic Modifier During Skull Bonmentioning

confidence: 99%

A tale of two cities: The genetic mechanisms governing calvarial bone development

Ferguson

Atit

2018

Genesis

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The skull bones must grow in a coordinated, three-dimensional manner to coalesce and form the head and face. Mammalian skull bones have a dual embryonic origin from cranial neural crest cells (CNCC) and paraxial mesoderm (PM) and ossify through intramembranous ossification. The calvarial bones, the bones of the cranium which cover the brain, are derived from the supraorbital arch (SOA) region mesenchyme. The SOA is the site of frontal and parietal bone morphogenesis and primary center of ossification. The objective of this review is to frame our current in vivo understanding of the morphogenesis of the calvarial bones and the gene networks regulating calvarial bone initiation in the SOA mesenchyme.

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HOXC8 initiates an ectopic mammary program by regulating Fgf10 and Tbx3 expression, and Wnt/β-catenin signaling

Cited by 21 publications

References 74 publications

Control of Hoxd gene transcription in the mammary bud by hijacking a preexisting regulatory landscape

Control of Hoxd gene transcription in the mammary bud by hijacking a preexisting regulatory landscape

Conditional Loss of Hoxa5 Function Early after Birth Impacts on Expression of Genes with Synaptic Function

A tale of two cities: The genetic mechanisms governing calvarial bone development

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