Fat4-Dchs1 signalling controls cell proliferation in developing vertebrae

Kuta, Anna; Mao, Yaopan; Martin, Tina; Sousa, Catia; Whiting, Danielle; Zakaria, Sana; Crespo-Enríquez, Iván; Evans, Philippa; Balczerski, Bartosz; Mankoo, Baljinder S.; Irvine, Kenneth D.; Francis‐West, Philippa

doi:10.1242/dev.131037

Cited by 21 publications

(20 citation statements)

References 55 publications

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“…Mutations in Fat’s closest mammalian homolog Fat4 (FatJ) and its Ds-like ligands strongly disrupt PCP-like processes, and have in humans been associated with the multisystem defects of Hennekam and Van Maldergem syndromes ( Alders et al, 2014 ; Mao et al, 2011 ; Saburi et al, 2008 ; Zakaria et al, 2014 ). There has been some debate, however, about whether the mammalian proteins retain direct regulation of Hippo activity ( Bagherie-Lachidan et al, 2015 ; Bossuyt et al, 2014 ; Pan et al, 2013 ; Sadeqzadeh et al, 2014 ; Kuta et al, 2016 ). Nonetheless, Fat4 has been linked to Hippo changes in both normal development and tumors ( Qi et al, 2009 ; Van Hateren et al, 2011 ), mutations in Fat4 or Dachsous1 change the balance of precursors and mature neurons in the developing neuroepithelium of both humans and mice, and the mouse defect can be reversed by knockdown of the Yki homolog Yap ( Cappello et al, 2013 ).…”

Section: Discussionmentioning

confidence: 99%

The novel SH3 domain protein Dlish/CG10933 mediates fat signaling in Drosophila by binding and regulating Dachs

Zhang

Wang

Matsumoto

et al. 2016

eLife

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Much of the Hippo and planar cell polarity (PCP) signaling mediated by the Drosophila protocadherin Fat depends on its ability to change the subcellular localization, levels and activity of the unconventional myosin Dachs. To better understand this process, we have performed a structure-function analysis of Dachs, and used this to identify a novel and important mediator of Fat and Dachs activities, a Dachs-binding SH3 protein we have named Dlish. We found that Dlish is regulated by Fat and Dachs, that Dlish also binds Fat and the Dachs regulator Approximated, and that Dlish is required for Dachs localization, levels and activity in both wild type and fat mutant tissue. Our evidence supports dual roles for Dlish. Dlish tethers Dachs to the subapical cell cortex, an effect partly mediated by the palmitoyltransferase Approximated under the control of Fat. Conversely, Dlish promotes the Fat-mediated degradation of Dachs.DOI: http://dx.doi.org/10.7554/eLife.16624.001

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Section: Discussionmentioning

confidence: 99%

The novel SH3 domain protein Dlish/CG10933 mediates fat signaling in Drosophila by binding and regulating Dachs

Zhang

Wang

Matsumoto

et al. 2016

eLife

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“…The increased proliferation within the osteogenic progenitors is analogous to the role of Dchs1-Fat4 signalling in the cerebral cortex and heart (Cappello et al, 2013;Ragni et al, 2017) and in contrast to the decreased proliferation observed in the kidney and somites (Kuta et al, 2016;Mao et al, 2011). As in the heart and brain, loss of Dchs1-Fat4 signalling also resulted in increased Yap activity.…”

Section: Discussionmentioning

confidence: 70%

Dchs1-Fat4 regulation of osteogenic differentiation in mouse

et al. 2019

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In human, mutations of the protocadherins FAT4 and DCHS1 result in Van Maldergem syndrome, which is characterised, in part, by craniofacial abnormalities. Here, we analyse the role of Dchs1-Fat4 signalling during osteoblast differentiation in mouse. We show that Fat4 and Dchs1 mutants mimic the craniofacial phenotype of the human syndrome and that Dchs1-Fat4 signalling is essential for osteoblast differentiation. In Dchs1/Fat4 mutants, proliferation of osteoprogenitors is increased and osteoblast differentiation is delayed. We show that loss of Dchs1-Fat4 signalling is linked to increased Yap-Tead activity and that Yap is expressed and required for proliferation in osteoprogenitors. In contrast, Taz is expressed in more-committed Runx2-expressing osteoblasts, Taz does not regulate osteoblast proliferation and Taz-Tead activity is unaffected in Dchs1/Fat4 mutants. Finally, we show that Yap and Taz differentially regulate the transcriptional activity of Runx2, and that the activity of Yap-Runx2 and Taz-Runx2 complexes is altered in Dchs1/Fat4 mutant osteoblasts. In conclusion, these data identify Dchs1-Fat4 as a signalling pathway in osteoblast differentiation, reveal its crucial role within the early Runx2 progenitors, and identify distinct requirements for Yap and Taz during osteoblast differentiation.

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“…Dachsous cadherin-related 1 (DCHS1) expression is up regulated in hypoxic conditions by fivefold and is a cellular adhesion molecule member of the cadherin superfamily. Lack of DCHS1 results in developmental defects of the early sclerotome associated with fewer chondrogenic cells within the developing vertebral body [ 35 ]. Keratin 19 (KRT19) expression showed a fourfold increase in hypoxic cultured samples and is an intermediate filament protein that is part of the keratin family.…”

Section: Resultsmentioning

confidence: 99%

Comparing atmospheric and hypoxic cultured mesenchymal stem cell transcriptome: implication for stem cell therapies targeting intervertebral discs

Elabd¹,

Ichim

Miller³

et al. 2018

J Transl Med

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BackgroundMesenchymal stem cells (MSCs) represent an attractive avenue for cellular therapies targeting degenerative diseases. MSC in vitro expansion is required in order to obtain therapeutic numbers during the manufacturing process. It is known that culture conditions impact cellular properties and behavior after in vivo transplantation. In this study, we aimed at evaluating the benefit of hypoxic culturing of human bone marrow derived mesenchymal stem cells on cell fitness and whole genome expression and discussed its implication on cellular therapies targeting orthopedic diseases such as chronic lower back pain.MethodsHuman bone marrow mesenchymal stem cells (hBMMSCs) were isolated from fresh human anticoagulated whole bone marrow and were cultured side by side in atmospheric (20% O2) and hypoxic (5% O2) oxygen partial pressure for up to 3 passages. Stem cell fitness was assessed by clonogenic assay, cell surface marker expression and differentiation potential. Whole genome expression was performed by mRNA sequencing. Data from clonogenic assays, cell surface marker by flow cytometry and gene expression by quantitative PCR were analyzed by two-tailed paired Student’s t-test. Data from mRNA sequencing were aligned to hg19 using Tophat-2.0.13 and analyzed using Cufflinks-2.1.1.ResultsHypoxic culturing of hBMMSCs had positive effects on cell fitness, as evidenced by an increased clonogenicity and improved differentiation potential towards adipocyte and chondrocyte lineages. No difference in osteoblast differentiation or in cell surface markers were observed. Only a small subset of genes (34) were identified by mRNA sequencing to be significantly dysregulated by hypoxia. When clustered by biological function, these genes were associated with chondrogenesis and cartilage metabolism, inflammation and immunomodulation, cellular survival, migration and proliferation, vasculogenesis and angiogenesis.ConclusionsHypoxic culturing positively impacted hBMMSCs fitness and transcriptome, potentially improving inherent properties of these cells that are critical for the development of successful cellular therapies. Hypoxic culturing should be considered for the in vitro expansion of hBMMSCs during manufacturing of cellular therapies targeting orthopedic disorders such as lower back pain.

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Fat4-Dchs1 signalling controls cell proliferation in developing vertebrae

Cited by 21 publications

References 55 publications

The novel SH3 domain protein Dlish/CG10933 mediates fat signaling in Drosophila by binding and regulating Dachs

The novel SH3 domain protein Dlish/CG10933 mediates fat signaling in Drosophila by binding and regulating Dachs

Dchs1-Fat4 regulation of osteogenic differentiation in mouse

Comparing atmospheric and hypoxic cultured mesenchymal stem cell transcriptome: implication for stem cell therapies targeting intervertebral discs

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