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Dive into the research topics where Pierre M. Del Moral is active.

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Featured researches published by Pierre M. Del Moral.


Respiratory Research | 2003

Growth factor signaling in lung morphogenetic centers: automaticity, stereotypy and symmetry

David Warburton; Saverio Bellusci; Pierre M. Del Moral; Vesa Kaartinen; Matt Lee; Denise Tefft; Wei Shi

Lung morphogenesis is stereotypic, both for lobation and for the first several generations of airways, implying mechanistic control by a well conserved, genetically hardwired developmental program. This program is not only directed by transcriptional factors and peptide growth factor signaling, but also co-opts and is modulated by physical forces. Peptide growth factors signal within repeating epithelial-mesenchymal temporospatial patterns that constitute morphogenetic centers, automatically directing millions of repetitive events during both stereotypic branching and nonstereotypic branching as well as alveolar surface expansion phases of lung development. Transduction of peptide growth factor signaling within these centers is finely regulated at multiple levels. These may include ligand expression, proteolytic activation of latent ligand, ligand bioavailability, ligand binding proteins and receptor affinity and presentation, receptor complex assembly and kinase activation, phosphorylation and activation of adapter and messenger protein complexes as well as downstream events and cross-talk both inside and outside the nucleus. Herein we review the critical Sonic Hedgehog, Fibroblast Growth Factor, Bone Morphogenetic Protein, Vascular Endothelial Growth Factor and Transforming Growth Factorβ signaling pathways and propose how they may be functionally coordinated within compound, highly regulated morphogenetic gradients that drive first stereotypic and then non-stereotypic, automatically repetitive, symmetrical as well as asymmetrical branching events in the lung.


The Journal of Physiology | 2008

Regulation of mouse lung development by the extracellular calcium-sensing receptor, CaR

Brenda A. Finney; Pierre M. Del Moral; William James Wilkinson; S. Cayzac; Martin Cole; David Warburton; Paul J. Kemp; Daniela Riccardi

Postnatal lung function is critically dependent upon optimal embryonic lung development. As the free ionized plasma calcium concentration ([Ca2+]o) of the fetus is higher than that of the adult, the process of lung development occurs in a hypercalcaemic environment. In the adult, [Ca2+]o is monitored by the G‐protein coupled, extracellular calcium‐sensing receptor (CaR), but neither its ontogeny nor its potential role in lung development are known. Here, we demonstrate that CaR is expressed in the mouse lung epithelium, and that its expression is developmentally regulated, with a peak of expression at embryonic day 12.5 (E12.5) and a subsequent decrease by E18, after which the receptor is absent. Experiments carried out using the lung explant culture model in vitro show that lung branching morphogenesis is sensitive to [Ca2+]o, being maximal at physiological adult [Ca2+]o (i.e. 1.0–1.3 mm) and lowest at the higher, fetal (i.e. 1.7 mm) [Ca2+]o. Administration of the specific CaR positive allosteric modulator, the calcimimetic R‐568, mimics the suppressive effects of high [Ca2+]o on branching morphogenesis while both phospholipase C and PI3 kinase inhibition reverse these effects. CaR activation suppresses cell proliferation while it enhances intracellular calcium signalling, lung distension and fluid secretion. Conditions which are restrictive either to branching or to secretion can be rescued by manipulating [Ca2+]o in the culture medium. In conclusion, fetal Ca2+o, acting through a developmentally regulated CaR, is an important extrinsic factor that modulates the intrinsic lung developmental programme. Our observations support a novel role for the CaR in preventing hyperplastic lung disease in utero.


Developmental Dynamics | 2009

Induction of fibroblast growth factor 10 (FGF10) in the ileal crypt epithelium after massive small bowel resection suggests a role for FGF10 in gut adaptation.

Cindy C. Tai; Jennifer L. Curtis; Frederic G. Sala; Pierre M. Del Moral; Nikunj K. Chokshi; Robert J. Kanard; Denise Al Alam; Jin Wang; R. Cartland Burns; Henri R. Ford; Anatoly Grishin; Kasper S. Wang; Saverio Bellusci

We have previously reported that fibroblast growth factor 10 (FGF10) is crucial for the survival and proliferation of progenitor cells during embryonic gastrointestinal development. We sought to characterize the potential role of FGF10 signaling in the adaptive response following small bowel resection. Adult wild‐type and Fgf10LacZ mice underwent 50% small bowel resection (SBR) or sham operation. Tissues were harvested 24 or 48 hr after surgery for histology, immunohistochemistry, and in situ hybridization. After SBR, Fgf10 expression was demonstrated in the epithelium at the base of the crypts. Moreover, there was a statistically significant increase in proliferating cells and goblet cells after SBR. In vitro studies using rat intestinal epithelial crypt (IEC‐6) cells exposed to medium with or without recombinant FGF10 showed increased proliferation and phosphorylation of Raf and AKT with the addition of FGF10. Our results suggest that FGF10 may play a therapeutic role in diseases involving intestinal failure. Developmental Dynamics 238:294–301, 2009.


Developmental Biology | 2007

Fgf10 dosage is critical for the amplification of epithelial cell progenitors and for the formation of multiple mesenchymal lineages during lung development.

Suresh K. Ramasamy; Arnaud Mailleux; Varsha V. Gupte; Francisca Mata; Frederic G. Sala; Jacqueline M. Veltmaat; Pierre M. Del Moral; Stijn De Langhe; Sara Parsa; Lisa K. Kelly; Robert G. Kelly; Wei Shia; Eli Keshet; Parviz Minoo; David Warburton; Saverio Bellusci


Journal of Pediatric Surgery | 2005

Colonic atresia without mesenteric vascular occlusion. The role of the fibroblast growth factor 10 signaling pathway

Timothy Fairbanks; Robert Kanard; Pierre M. Del Moral; F.G. Sala; Stijn De Langhe; Chrissy Lopez; Jacqueline M. Veltmaat; David Warburton; Kathryn D. Anderson; Saverio Bellusci; R. Cartland Burns


Journal of Pediatric Surgery | 2006

The fibroblast growth factor pathway serves a regulatory role in proliferation and apoptosis in the pathogenesis of intestinal atresia

Timothy Fairbanks; Frederic G. Sala; Robert Kanard; Jennifer L. Curtis; Pierre M. Del Moral; Stijn De Langhe; David Warburton; Kathryn D. Anderson; Saverio Bellusci; R. Cartland Burns


Journal of Pediatric Surgery | 2005

Fibroblast growth factor-10 serves a regulatory role in duodenal development

Robert Kanard; Timothy Fairbanks; Stijn De Langhe; F.G. Sala; Pierre M. Del Moral; Chrissy Lopez; David Warburton; Kathryn D. Anderson; Saverio Bellusci; R. Cartland Burns


Journal of Pediatric Surgery | 2004

Fibroblast growth factor receptor 2 IIIb invalidation—a potential cause of familial duodenal atresia

Timothy Fairbanks; Robert Kanard; Pierre M. Del Moral; Frederic G. Sala; Stijn De Langhe; David Warburton; Kathryn D. Anderson; Saverio Bellusci; R. Cartland Burns


Cell Signaling and Growth Factors in Development: From Molecules to Organogenesis | 2008

Cell Signaling and Growth Factors in Lung Development

David Warburton; Saverio Bellusci; Pierre M. Del Moral; Stijn DeLanghe; Vesa Kaartinen; Matt Lee; Denise Tefft; Wei Shi


The FASEB Journal | 2008

Extracellular calcium regulates embryonic mouse lung function through the calcium-sensing receptor

Brenda A. Finney; Pierre M. Del Moral; William W. Wilkinson; Martin Cole; David M. A. Martin; David Warburton; Paul J. Kemp; Daniela Riccardi

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David Warburton

Children's Hospital Los Angeles

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R. Cartland Burns

Children's Hospital Los Angeles

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Stijn De Langhe

Children's Hospital Los Angeles

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Kathryn D. Anderson

Children's Hospital Los Angeles

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Robert Kanard

Children's Hospital Los Angeles

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Timothy Fairbanks

Children's Hospital Los Angeles

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Frederic G. Sala

Children's Hospital Los Angeles

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Chrissy Lopez

Children's Hospital Los Angeles

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