31 results on '"Faure, Christophe"'
Search Results
2. Male-biased aganglionic megacolon in the TashT mouse model of Hirschsprung disease involves upregulation of p53 protein activity and Ddx3y gene expression
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Cardinal, Tatiana, Bergeron, Karl-Frédérik, Soret, Rodolphe, Souchkova, Ouliana, Faure, Christophe, Guillon, Amélina, Pilon, Nicolas, Cardinal, Tatiana, Bergeron, Karl-Frédérik, Soret, Rodolphe, Souchkova, Ouliana, Faure, Christophe, Guillon, Amélina, and Pilon, Nicolas
- Abstract
Hirschsprung disease (HSCR) is a complex genetic disorder of neural crest development resulting in incomplete formation of the enteric nervous system (ENS). This life-threatening neurocristopathy affects 1/5000 live births, with a currently unexplained male-biased ratio. To address this lack of knowledge, we took advantage of the TashT mutant mouse line, which is the only HSCR model to display a robust male bias. Our prior work revealed that the TashT insertional mutation perturbs a Chr.10 silencer-enriched non-coding region, leading to transcriptional dysregulation of hundreds of genes in neural crest-derived ENS progenitors of both sexes. Here, through sex-stratified transcriptome analyses and targeted overexpression in ENS progenitors, we show that male-biased ENS malformation in TashT embryos is not due to upregulation of Sry–the murine ortholog of a candidate gene for the HSCR male bias in humans–but instead involves upregulation of another Y-linked gene, Ddx3y. This discovery might be clinically relevant since we further found that the DDX3Y protein is also expressed in the ENS of a subset of male HSCR patients. Mechanistically, other data including chromosome conformation captured-based assays and CRISPR/Cas9-mediated deletions suggest that Ddx3y upregulation in male TashT ENS progenitors is due to increased transactivation by p53, which appears especially active in these cells yet without triggering apoptosis. Accordingly, in utero treatment of TashT embryos with the p53 inhibitor pifithrin-α decreased Ddx3y expression and abolished the otherwise more severe ENS defect in TashT males. Our data thus highlight novel pathogenic roles for p53 and DDX3Y during ENS formation in mice, a finding that might help to explain the intriguing male bias of HSCR in humans.
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- 2020
3. Glial Cell Derived Neurotrophic Factor Induces Enteric Neurogenesis and Improves Colon Structure and Function in Mouse Models of Hirschsprung Disease
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Soret, Rodolphe, Schneider, Sabine, Bernas, Guillaume, Christophers, Briana, Souchkova, Ouliana, Charrier, Baptiste, Righini-Grunder, Franziska, Aspirot, Ann, Landry, Mathieu, Kembel, Steven W., Faure, Christophe, Heuckeroth, Robert O., Pilon, Nicolas, Soret, Rodolphe, Schneider, Sabine, Bernas, Guillaume, Christophers, Briana, Souchkova, Ouliana, Charrier, Baptiste, Righini-Grunder, Franziska, Aspirot, Ann, Landry, Mathieu, Kembel, Steven W., Faure, Christophe, Heuckeroth, Robert O., and Pilon, Nicolas
- Abstract
Background & Aims: Hirschsprung disease (HSCR) is a life-threatening birth defect in which the distal colon is devoid of enteric neural ganglia. HSCR is treated by surgical removal of aganglionic bowel, but many children continue to have severe problems after surgery. We studied whether administration of glial cell derived neurotrophic factor (GDNF) induces enteric nervous system regeneration in mouse models of HSCR. Methods: We performed studies with four mouse models of HSCR: Holstein (HolTg/Tg, a model for trisomy 21-associated HSCR), TashT (TashTTg/Tg, a model for male-biased HSCR), Piebald-lethal(Ednrbs-l//s-l, a model for EDNRB mutation-associated HSCR), and Ret9/- (with aganglionosis induced by mycophenolate). Mice were given rectal enemas containing GDNF or saline (control) from postnatal days 4 through 8. We measured survival times of mice, and colon tissues were analyzed by histology, immunofluorescence, and immunoblots. Neural ganglia regeneration and structure, bowel motility, epithelial permeability, muscle thickness, and neutrophil infiltration were studied in colon tissues and in mice. Stool samples were collected, and microbiomes were analyzed by 16S rRNA gene sequencing. Time-lapse imaging and genetic cell-lineage tracing were used to identify a source of GDNF-targeted neural progenitors. Human aganglionic colon explants from children with HSCR were cultured with GDNF and evaluated for neurogenesis. Results: GDNF significantly prolonged mean survival times of HolTg/Tgmice, Ednrbs-l//s-l mice, and male TashTTg/Tg mice, compared with control mice, but not Ret9/- mice (which had mycophenolate toxicity). Mice given GDNF developed neurons and glia in distal bowel tissues that were aganglionic incontrol mice, had a significant increase in colon motility, and had significant decreases in epithelial permeability, muscle thickness, and neutrophil density. We observed dysbiosis in fecal samples from HolTg/Tg mice compared with feces from wild-type mice; fecal
- Published
- 2020
4. J'ai mal au ventre! : Les problèmes gastro-intestinaux chez les enfants
- Author
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Alvarez, Fernando, Faure, Christophe, Alvarez, Fernando, Alvarez, Fernando, Faure, Christophe, and Alvarez, Fernando
- Abstract
Ce livre traite des problèmes gastro-intestinaux ou liés à l’alimentation, de la naissance à l’adolescence. Il propose des attitudes aidantes à adopter et confirme les approches de soulagement ou de traitement à envisager.
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- 2019
5. J'ai mal au ventre! : Les problèmes gastro-intestinaux chez les enfants
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Alvarez, Fernando, Faure, Christophe, Alvarez, Fernando, Alvarez, Fernando, Faure, Christophe, and Alvarez, Fernando
- Abstract
Ce livre traite des problèmes gastro-intestinaux ou liés à l’alimentation, de la naissance à l’adolescence. Il propose des attitudes aidantes à adopter et confirme les approches de soulagement ou de traitement à envisager.
- Published
- 2019
6. J'ai mal au ventre! : Les problèmes gastro-intestinaux chez les enfants
- Author
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Alvarez, Fernando, Faure, Christophe, Alvarez, Fernando, Alvarez, Fernando, Faure, Christophe, and Alvarez, Fernando
- Abstract
Ce livre traite des problèmes gastro-intestinaux ou liés à l’alimentation, de la naissance à l’adolescence. Il propose des attitudes aidantes à adopter et confirme les approches de soulagement ou de traitement à envisager.
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- 2019
7. J'ai mal au ventre! : Les problèmes gastro-intestinaux chez les enfants
- Author
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Alvarez, Fernando, Faure, Christophe, Alvarez, Fernando, Alvarez, Fernando, Faure, Christophe, and Alvarez, Fernando
- Abstract
Ce livre traite des problèmes gastro-intestinaux ou liés à l’alimentation, de la naissance à l’adolescence. Il propose des attitudes aidantes à adopter et confirme les approches de soulagement ou de traitement à envisager.
- Published
- 2019
8. J'ai mal au ventre! : Les problèmes gastro-intestinaux chez les enfants
- Author
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Alvarez, Fernando, Faure, Christophe, Alvarez, Fernando, Alvarez, Fernando, Faure, Christophe, and Alvarez, Fernando
- Abstract
Ce livre traite des problèmes gastro-intestinaux ou liés à l’alimentation, de la naissance à l’adolescence. Il propose des attitudes aidantes à adopter et confirme les approches de soulagement ou de traitement à envisager.
- Published
- 2019
9. J'ai mal au ventre! : Les problèmes gastro-intestinaux chez les enfants
- Author
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Alvarez, Fernando, Faure, Christophe, Alvarez, Fernando, Alvarez, Fernando, Faure, Christophe, and Alvarez, Fernando
- Abstract
Ce livre traite des problèmes gastro-intestinaux ou liés à l’alimentation, de la naissance à l’adolescence. Il propose des attitudes aidantes à adopter et confirme les approches de soulagement ou de traitement à envisager.
- Published
- 2019
10. The Case for Thoughtful Prescribing of Proton Pump Inhibitors in Infants.
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Rosen, Rachel L, Rosen, Rachel L, Krishnan, Usha, Mousa, Hayat, Dall'oglio, Luigi, Faure, Christophe, Gottrand, Frederic, Rosen, Rachel L, Rosen, Rachel L, Krishnan, Usha, Mousa, Hayat, Dall'oglio, Luigi, Faure, Christophe, and Gottrand, Frederic
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- 2018
11. The Case for Thoughtful Prescribing of Proton Pump Inhibitors in Infants.
- Author
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Rosen, Rachel L, Rosen, Rachel L, Krishnan, Usha, Mousa, Hayat, Dall'oglio, Luigi, Faure, Christophe, Gottrand, Frederic, Rosen, Rachel L, Rosen, Rachel L, Krishnan, Usha, Mousa, Hayat, Dall'oglio, Luigi, Faure, Christophe, and Gottrand, Frederic
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- 2018
12. How to Care for Patients with EA-TEF: The Known and the Unknown.
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Mousa, Hayat, Mousa, Hayat, Krishnan, Usha, Hassan, Maheen, Dall'Oglio, Luigi, Rosen, Rachel, Gottrand, Frédéric, Faure, Christophe, Mousa, Hayat, Mousa, Hayat, Krishnan, Usha, Hassan, Maheen, Dall'Oglio, Luigi, Rosen, Rachel, Gottrand, Frédéric, and Faure, Christophe
- Abstract
PURPOSE OF REVIEW:Guidelines were recently published highlighting why esophageal atresia (EA) patients are prone to complication risks, and the need for long-term follow-up. In this review, we will focus on how to investigate and treat potential complications, as well as the pros and cons of different investigative and treatment modalities, and what areas continue to need further research. RECENT FINDINGS:EA patients are at high risk for gastroesophageal reflux and esophageal strictures, and the sequela that result. Extraintestinal manifestations of gastroesophageal reflux disease (GERD) can appear similar to other pathologic diagnoses commonly found in EA patients, such as congenital stricture, eosinophilic esophagitis, esophageal dysmotility, tracheomalacia, recurrent fistula, aspiration, etc. Therefore, it is important to have a standardized way to monitor for these issues. pH impedance allows for detection of nonacid reflux and the height of reflux, which are important in correlating symptoms with reflux episodes. A multidisciplinary approach is beneficial in evaluating and monitoring EA patients in the long term.
- Published
- 2017
13. Pediatric Neurogastroenterology: Gastrointestinal Motility and Functional Disorders in Children
- Author
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Faure, Christophe., editor, Thapar, Nikhil., editor, Di Lorenzo, Carlo., editor, Faure, Christophe., editor, Thapar, Nikhil., editor, and Di Lorenzo, Carlo., editor
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- 2017
14. Pediatric Neurogastroenterology: Gastrointestinal Motility and Functional Disorders in Children
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Faure, Christophe., editor, Thapar, Nikhil., editor, Di Lorenzo, Carlo., editor, Faure, Christophe., editor, Thapar, Nikhil., editor, and Di Lorenzo, Carlo., editor
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- 2017
15. Pediatric Neurogastroenterology: Gastrointestinal Motility and Functional Disorders in Children
- Author
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Faure, Christophe., editor, Thapar, Nikhil., editor, Di Lorenzo, Carlo., editor, Faure, Christophe., editor, Thapar, Nikhil., editor, and Di Lorenzo, Carlo., editor
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- 2017
16. Pediatric Neurogastroenterology: Gastrointestinal Motility and Functional Disorders in Children
- Author
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Faure, Christophe., editor, Thapar, Nikhil., editor, Di Lorenzo, Carlo., editor, Faure, Christophe., editor, Thapar, Nikhil., editor, and Di Lorenzo, Carlo., editor
- Published
- 2017
17. How to Care for Patients with EA-TEF: The Known and the Unknown.
- Author
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Mousa, Hayat, Mousa, Hayat, Krishnan, Usha, Hassan, Maheen, Dall'Oglio, Luigi, Rosen, Rachel, Gottrand, Frédéric, Faure, Christophe, Mousa, Hayat, Mousa, Hayat, Krishnan, Usha, Hassan, Maheen, Dall'Oglio, Luigi, Rosen, Rachel, Gottrand, Frédéric, and Faure, Christophe
- Abstract
PURPOSE OF REVIEW:Guidelines were recently published highlighting why esophageal atresia (EA) patients are prone to complication risks, and the need for long-term follow-up. In this review, we will focus on how to investigate and treat potential complications, as well as the pros and cons of different investigative and treatment modalities, and what areas continue to need further research. RECENT FINDINGS:EA patients are at high risk for gastroesophageal reflux and esophageal strictures, and the sequela that result. Extraintestinal manifestations of gastroesophageal reflux disease (GERD) can appear similar to other pathologic diagnoses commonly found in EA patients, such as congenital stricture, eosinophilic esophagitis, esophageal dysmotility, tracheomalacia, recurrent fistula, aspiration, etc. Therefore, it is important to have a standardized way to monitor for these issues. pH impedance allows for detection of nonacid reflux and the height of reflux, which are important in correlating symptoms with reflux episodes. A multidisciplinary approach is beneficial in evaluating and monitoring EA patients in the long term.
- Published
- 2017
18. Pediatric Neurogastroenterology: Gastrointestinal Motility and Functional Disorders in Children
- Author
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Faure, Christophe., editor, Thapar, Nikhil., editor, Di Lorenzo, Carlo., editor, Faure, Christophe., editor, Thapar, Nikhil., editor, and Di Lorenzo, Carlo., editor
- Published
- 2017
19. Pediatric Neurogastroenterology: Gastrointestinal Motility and Functional Disorders in Children
- Author
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Faure, Christophe., editor, Thapar, Nikhil., editor, Di Lorenzo, Carlo., editor, Faure, Christophe., editor, Thapar, Nikhil., editor, and Di Lorenzo, Carlo., editor
- Published
- 2017
20. ESPGHAN-NASPGHAN Guidelines for the Evaluation and Treatment of Gastrointestinal and Nutritional Complications in Children With Esophageal Atresia-Tracheoesophageal Fistula.
- Author
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Krishnan, Usha, Krishnan, Usha, Mousa, Hayat, Dall'Oglio, Luigi, Homaira, Nusrat, Rosen, Rachel, Faure, Christophe, Gottrand, Frédéric, Krishnan, Usha, Krishnan, Usha, Mousa, Hayat, Dall'Oglio, Luigi, Homaira, Nusrat, Rosen, Rachel, Faure, Christophe, and Gottrand, Frédéric
- Abstract
BackgroundEsophageal atresia (EA) is one of the most common congenital digestive anomalies. With improvements in surgical techniques and intensive care treatments, the focus of care of these patients has shifted from mortality to morbidity and quality-of-life issues. These children face gastrointestinal (GI) problems not only in early childhood but also through adolescence and adulthood. There is, however, currently a lack of a systematic approach to the care of these patients. The GI working group of International Network on Esophageal Atresia comprises members from ESPGHAN/NASPGHAN and was charged with the task of developing uniform evidence-based guidelines for the management of GI complications in children with EA.MethodsThirty-six clinical questions addressing the diagnosis, treatment, and prognosis of the common GI complications in patients with EA were formulated. Questions on the diagnosis, and treatment of gastroesophageal reflux, management of "cyanotic spells," etiology, investigation and management of dysphagia, feeding difficulties, anastomotic strictures, congenital esophageal stenosis in EA patients were addressed. The importance of excluding eosinophilic esophagitis and associated GI anomalies in symptomatic patients with EA is discussed as is the quality of life of these patients and the importance of a systematic transition of care to adulthood. A systematic literature search was performed from inception to March 2014 using Embase, MEDLINE, the Cochrane Database of Systematic Reviews, Cochrane Central Register of Controlled Clinical Trials, and PsychInfo databases. The approach of the Grading of Recommendations Assessment, Development and Evaluation was applied to evaluate outcomes. During 2 consensus meetings, all recommendations were discussed and finalized. The group members voted on each recommendation, using the nominal voting technique. Expert opinion was used where no randomized controlled trials were available to support the recommendation.
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- 2016
21. Prevalence of Barrett Esophagus in Adolescents and Young Adults With Esophageal Atresia.
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UCL - SSS/IREC/PEDI - Pôle de Pédiatrie, UCL - (SLuc) Service de gastro-entérologie et hépatologie pédiatrique, Schneider, Anne, Gottrand, Frédéric, Bellaiche, Marc, Becmeur, François, Lachaux, Alain, Bridoux-Henno, Laure, Michel, Jean-Luc, Faure, Christophe, Philippe, Paul, Vandenplas, Yvan, Dupont, Claire, Breton, Anne, Gaudin, Jean, Lamireau, Thierry, Muyshont, Laurence, Podevin, Guillaume, Viola, Sheila, Bertrand, Valérie, Caldari, Dominique, Colinet, Stéphanie, Wanty, Catherine, Sauleau, Erik, Leteurtre, Emmanuelle, Michaud, Laurent, UCL - SSS/IREC/PEDI - Pôle de Pédiatrie, UCL - (SLuc) Service de gastro-entérologie et hépatologie pédiatrique, Schneider, Anne, Gottrand, Frédéric, Bellaiche, Marc, Becmeur, François, Lachaux, Alain, Bridoux-Henno, Laure, Michel, Jean-Luc, Faure, Christophe, Philippe, Paul, Vandenplas, Yvan, Dupont, Claire, Breton, Anne, Gaudin, Jean, Lamireau, Thierry, Muyshont, Laurence, Podevin, Guillaume, Viola, Sheila, Bertrand, Valérie, Caldari, Dominique, Colinet, Stéphanie, Wanty, Catherine, Sauleau, Erik, Leteurtre, Emmanuelle, and Michaud, Laurent
- Abstract
To study the prevalence of Barrett esophagus (BE) (gastric and/or intestinal metaplasia) in adolescents treated for esophageal atresia (EA). SUMMARY OF BACKGROUND DATA: EA patients are at high risk of BE. METHODS: This multicenter prospective study included EA patients aged 15 to 19 years. All eligible patients were proposed an upper endoscopy with multistaged esophageal biopsies under general anesthesia. Histological suspicion of metaplasia was confirmed centrally. RESULTS: One hundred twenty patients [mean age, 16.5 years (±1.4)] were included; 70% had been treated for gastroesophageal reflux disease (GERD) during infancy. At evaluation, 8% were undernourished, 41% had received antireflux surgery, and 41% presented with GERD symptoms, although only 28% were receiving medical treatment. Esophagitis was found at endoscopy in 34% and confirmed at histology in 67%. BE was suspected after endoscopy in 37% and was confirmed by histology for 43% of patients (50 gastric and 1 intestinal metaplasia). No endoscopic or histological anomalies were found at the anastomosis site. BE was not significantly related to clinical symptoms. In multivariate analysis, BE was associated with EA without fistula (P = 0.03), previous multiple antireflux surgery (P = 0.04), esophageal dilation (P = 0.04), suspicion of BE at endoscopy (P < 0.001), and histological esophagitis (P = 0.02). CONCLUSIONS: Patients with EA are at high risk of persistent GERD and BE. The development of BE is related to GERD history. Long-term systematic follow-up of the esophageal mucosa including multistaged biopsies is required, even in asymptomatic patients.
- Published
- 2016
22. ESPGHAN-NASPGHAN Guidelines for the Evaluation and Treatment of Gastrointestinal and Nutritional Complications in Children With Esophageal Atresia-Tracheoesophageal Fistula.
- Author
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Krishnan, Usha, Krishnan, Usha, Mousa, Hayat, Dall'Oglio, Luigi, Homaira, Nusrat, Rosen, Rachel, Faure, Christophe, Gottrand, Frédéric, Krishnan, Usha, Krishnan, Usha, Mousa, Hayat, Dall'Oglio, Luigi, Homaira, Nusrat, Rosen, Rachel, Faure, Christophe, and Gottrand, Frédéric
- Abstract
BackgroundEsophageal atresia (EA) is one of the most common congenital digestive anomalies. With improvements in surgical techniques and intensive care treatments, the focus of care of these patients has shifted from mortality to morbidity and quality-of-life issues. These children face gastrointestinal (GI) problems not only in early childhood but also through adolescence and adulthood. There is, however, currently a lack of a systematic approach to the care of these patients. The GI working group of International Network on Esophageal Atresia comprises members from ESPGHAN/NASPGHAN and was charged with the task of developing uniform evidence-based guidelines for the management of GI complications in children with EA.MethodsThirty-six clinical questions addressing the diagnosis, treatment, and prognosis of the common GI complications in patients with EA were formulated. Questions on the diagnosis, and treatment of gastroesophageal reflux, management of "cyanotic spells," etiology, investigation and management of dysphagia, feeding difficulties, anastomotic strictures, congenital esophageal stenosis in EA patients were addressed. The importance of excluding eosinophilic esophagitis and associated GI anomalies in symptomatic patients with EA is discussed as is the quality of life of these patients and the importance of a systematic transition of care to adulthood. A systematic literature search was performed from inception to March 2014 using Embase, MEDLINE, the Cochrane Database of Systematic Reviews, Cochrane Central Register of Controlled Clinical Trials, and PsychInfo databases. The approach of the Grading of Recommendations Assessment, Development and Evaluation was applied to evaluate outcomes. During 2 consensus meetings, all recommendations were discussed and finalized. The group members voted on each recommendation, using the nominal voting technique. Expert opinion was used where no randomized controlled trials were available to support the recommendation.
- Published
- 2016
23. Prevalence of barrett esophagus in adolescents and young adults with esophageal atresia
- Author
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Schneider, Anne, Vandenplas, Yvan, Dupont, Claire, Breton, Anne, Gaudin, Jean, Lamireau, Thierry, Muyshont, Laurence, Podevin, Guillaume, Viola, Sheila, Bertrand, Valérie, Caldari, Dominique, Gottrand, Frederic, Colinet, Stéphanie, Wanty, Catherine, Sauleau, Erik, Leteurtre, Emmanuelle, Michaud, Laurent, Bellaiche, Marc, Becmeur, Francois, Lachaux, Alain, Bridoux-Henno, Laure, Michel, Jean-Luc, Faure, Christophe, Philippe, Paul, Schneider, Anne, Vandenplas, Yvan, Dupont, Claire, Breton, Anne, Gaudin, Jean, Lamireau, Thierry, Muyshont, Laurence, Podevin, Guillaume, Viola, Sheila, Bertrand, Valérie, Caldari, Dominique, Gottrand, Frederic, Colinet, Stéphanie, Wanty, Catherine, Sauleau, Erik, Leteurtre, Emmanuelle, Michaud, Laurent, Bellaiche, Marc, Becmeur, Francois, Lachaux, Alain, Bridoux-Henno, Laure, Michel, Jean-Luc, Faure, Christophe, and Philippe, Paul
- Abstract
Objective: To study the prevalence of Barrett esophagus (BE) (gastric and/or intestinal metaplasia) in adolescents treated for esophageal atresia (EA). Summary of Background Data: EA patients are at high risk of BE. Methods: This multicenter prospective study included EA patients aged 15 to 19 years. All eligible patients were proposed an upper endoscopy with multistaged esophageal biopsies under general anesthesia. Histological suspicion of metaplasia was confirmed centrally. Results: One hundred twenty patients [mean age, 16.5 years (1.4)] were included; 70% had been treated for gastroesophageal reflux disease (GERD) during infancy. At evaluation, 8% were undernourished, 41% had received antireflux surgery, and 41% presented with GERD symptoms, although only 28% were receiving medical treatment. Esophagitis was found at endoscopy in 34% and confirmed at histology in 67%. BE was suspected after endoscopy in 37% and was confirmed by histology for 43% of patients (50 gastric and 1 intestinal metaplasia). No endoscopic or histological anomalies were found at the anastomosis site. BE was not significantly related to clinical symptoms. In multivariate analysis, BE was associated with EA without fistula (P=0.03), previous multiple antireflux surgery (P=0.04), esophageal dilation (P=0.04), suspicion of BE at endoscopy (P<0.001), and histological esophagitis (P=0.02). Conclusions: Patients with EA are at high risk of persistent GERD and BE. The development of BE is related to GERD history. Long-term systematic follow-up of the esophageal mucosa including multistaged biopsies is required, even in asymptomatic patients. (NCT02495051)., SCOPUS: ar.j, info:eu-repo/semantics/published
- Published
- 2016
24. A collagen VI–dependent pathogenic mechanism for Hirschsprung’s disease
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Soret, Rodolphe, Mennetrey, Mathilde, Bergeron, Karl F., Dariel, Anne, Neunlist, Michel, Grunder, Franziska, Faure, Christophe, Silversides, David W., Pilon, Nicolas, Soret, Rodolphe, Mennetrey, Mathilde, Bergeron, Karl F., Dariel, Anne, Neunlist, Michel, Grunder, Franziska, Faure, Christophe, Silversides, David W., and Pilon, Nicolas
- Abstract
Hirschsprung’s disease (HSCR) is a severe congenital anomaly of the enteric nervous system (ENS) characterized by functional intestinal obstruction due to a lack of intrinsic innervation in the distal bowel. Distal innervation deficiency results from incomplete colonization of the bowel by enteric neural crest cells (eNCCs), the ENS precursors. Here, we report the generation of a mouse model for HSCR — named Holstein — that contains an untargeted transgenic insertion upstream of the collagen- 6α4 (Col6a4) gene. This insertion induces eNCC-specific upregulation of Col6a4 expression that increases total collagen VI protein levels in the extracellular matrix (ECM) surrounding both the developing and the postnatal ENS. Increased collagen VI levels during development mainly result in slower migration of eNCCs. This appears to be due to the fact that collagen VI is a poor substratum for supporting eNCC migration and can even interfere with the migration-promoting effects of fibronectin. Importantly, for a majority of patients in a HSCR cohort, the myenteric ganglia from the ganglionated region are also specifically surrounded by abundant collagen VI microfibrils, an outcome accentuated by Down syndrome. Collectively, our data thus unveil a clinically relevant pathogenic mechanism for HSCR that involves cell-autonomous changes in ECM composition surrounding eNCCs. Moreover, as COL6A1 and COL6A2 are on human Chr.21q, this mechanism is highly relevant to the predisposition of patients with Down syndrome to HSCR.
- Published
- 2015
25. Current pediatric indications for cisapride: A position paper by a panel convened by the European Society for Pediatric Gastroenterology, Hepatology and Nutrition
- Author
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Vandenplas, Yvan, Belli, Dominique, Badriul, Hegar, Branski, David, Cadranel, Samy, Cervetto, J.L., Cleghorn, Geoffrey John G., Cucchiara, Salvatore, Davidson, Geoffrey Paul, Dias, Jorge Amil, Dupont, Christophe, Faure, Christophe, Firmansyah, Agus, Gottrand, Fréderique, Hassall, Eric, Heymans, Hugo Sa, Quak, Seng Hock, Jasinski, Christopher, Kneepkens, Frank, Koletzko, Sibylle, Kostovski, Aco, Leung, Y.K., Markiewicz, M., Maherzi, Abed, Ramirez-Mayans, Jaime Alfonso J., Milla, Peter P.J., Nurko, Samuel, Olafsdottir, Edda, Orsi, María Clelia M., Rodrigues Silva, Luciana, Poets, K., Polanco, Isabel Allué, Seo, Jeong Jea, Spolidoro, José, Saelzer, E., Staiano, Annamaria Maria, Szajewska, Hania, Vandenplas, Yvan, Belli, Dominique, Badriul, Hegar, Branski, David, Cadranel, Samy, Cervetto, J.L., Cleghorn, Geoffrey John G., Cucchiara, Salvatore, Davidson, Geoffrey Paul, Dias, Jorge Amil, Dupont, Christophe, Faure, Christophe, Firmansyah, Agus, Gottrand, Fréderique, Hassall, Eric, Heymans, Hugo Sa, Quak, Seng Hock, Jasinski, Christopher, Kneepkens, Frank, Koletzko, Sibylle, Kostovski, Aco, Leung, Y.K., Markiewicz, M., Maherzi, Abed, Ramirez-Mayans, Jaime Alfonso J., Milla, Peter P.J., Nurko, Samuel, Olafsdottir, Edda, Orsi, María Clelia M., Rodrigues Silva, Luciana, Poets, K., Polanco, Isabel Allué, Seo, Jeong Jea, Spolidoro, José, Saelzer, E., Staiano, Annamaria Maria, and Szajewska, Hania
- Abstract
SCOPUS: re.j, info:eu-repo/semantics/published
- Published
- 2000
26. Current pediatric indications for cisapride: A position paper by a panel convened by the European Society for Pediatric Gastroenterology, Hepatology and Nutrition
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Vandenplas, Yvan, Belli, Dominique, Badriul, Hegar, Branski, David, Cadranel, Samy, Cervetto, J.L., Cleghorn, Geoffrey John G., Cucchiara, Salvatore, Davidson, Geoffrey Paul, Dias, Jorge Amil, Dupont, Christophe, Faure, Christophe, Firmansyah, Agus, Gottrand, Fréderique, Hassall, Eric, Heymans, Hugo Sa, Quak, Seng Hock, Jasinski, Christopher, Kneepkens, Frank, Koletzko, Sibylle, Kostovski, Aco, Leung, Y.K., Markiewicz, M., Maherzi, Abed, Ramirez-Mayans, Jaime Alfonso J., Milla, Peter P.J., Nurko, Samuel, Olafsdottir, Edda, Orsi, María Clelia M., Rodrigues Silva, Luciana, Poets, K., Polanco, Isabel Allué, Seo, Jeong Jea, Spolidoro, José, Saelzer, E., Staiano, Annamaria Maria, Szajewska, Hania, Vandenplas, Yvan, Belli, Dominique, Badriul, Hegar, Branski, David, Cadranel, Samy, Cervetto, J.L., Cleghorn, Geoffrey John G., Cucchiara, Salvatore, Davidson, Geoffrey Paul, Dias, Jorge Amil, Dupont, Christophe, Faure, Christophe, Firmansyah, Agus, Gottrand, Fréderique, Hassall, Eric, Heymans, Hugo Sa, Quak, Seng Hock, Jasinski, Christopher, Kneepkens, Frank, Koletzko, Sibylle, Kostovski, Aco, Leung, Y.K., Markiewicz, M., Maherzi, Abed, Ramirez-Mayans, Jaime Alfonso J., Milla, Peter P.J., Nurko, Samuel, Olafsdottir, Edda, Orsi, María Clelia M., Rodrigues Silva, Luciana, Poets, K., Polanco, Isabel Allué, Seo, Jeong Jea, Spolidoro, José, Saelzer, E., Staiano, Annamaria Maria, and Szajewska, Hania
- Abstract
SCOPUS: re.j, info:eu-repo/semantics/published
- Published
- 2000
27. A critical appraisal of current management practices for infant regurgitation - Recommendations of a working party
- Author
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Vandenplas, Yvan, Belli, Dominique, Benhamou, Pierre Yves, Dupont, Christophe, Cadranel, Samy, Cézard, Jean-Pierre, Faure, Christophe, Cucchiara, Salvatore, Gottrand, Frederic, Hassall, Eric, Heymans, Hugo Sa, Kneepkens, Frank, Sandhu, Bhupinder Kaur, Vandenplas, Yvan, Belli, Dominique, Benhamou, Pierre Yves, Dupont, Christophe, Cadranel, Samy, Cézard, Jean-Pierre, Faure, Christophe, Cucchiara, Salvatore, Gottrand, Frederic, Hassall, Eric, Heymans, Hugo Sa, Kneepkens, Frank, and Sandhu, Bhupinder Kaur
- Abstract
Regurgitation is a common manifestation in infants below the age of 1 year and a frequent reason of counselling of general practitioners and paediatricians. Current management starts with postural and dietary measures, followed by antacids and prokinetics. Recent issues such as an increased risk of sudden infant death in the prone sleeping position and persistent occult gastro-oesophageal reflux in a subset of infants receiving milk thickeners or thickened 'anti-regurgitation formula' challenge the established approach. Therefore, the clinical practices for management of infant regurgitation have been critically evaluated with respect to their efficacy, safety and practical implications. The updated recommendations reached by the working party on the management of infant regurgigation contain five phases: (1A) parental reassurance; (1B) milk-thickening agents; (2) prokinetics; (3) positional therapy as an adjuvant therapy; (4A) H2-blockers; (4B) proton pump inhibitors; (5) surgery., SCOPUS: re.j, info:eu-repo/semantics/published
- Published
- 1997
28. A critical appraisal of current management practices for infant regurgitation - Recommendations of a working party
- Author
-
Vandenplas, Yvan, Belli, Dominique, Benhamou, Pierre Yves, Dupont, Christophe, Cadranel, Samy, Cézard, Jean-Pierre, Faure, Christophe, Cucchiara, Salvatore, Gottrand, Frederic, Hassall, Eric, Heymans, Hugo Sa, Kneepkens, Frank, Sandhu, Bhupinder Kaur, Vandenplas, Yvan, Belli, Dominique, Benhamou, Pierre Yves, Dupont, Christophe, Cadranel, Samy, Cézard, Jean-Pierre, Faure, Christophe, Cucchiara, Salvatore, Gottrand, Frederic, Hassall, Eric, Heymans, Hugo Sa, Kneepkens, Frank, and Sandhu, Bhupinder Kaur
- Abstract
Regurgitation is a common manifestation in infants below the age of 1 year and a frequent reason of counselling of general practitioners and paediatricians. Current management starts with postural and dietary measures, followed by antacids and prokinetics. Recent issues such as an increased risk of sudden infant death in the prone sleeping position and persistent occult gastro-oesophageal reflux in a subset of infants receiving milk thickeners or thickened 'anti-regurgitation formula' challenge the established approach. Therefore, the clinical practices for management of infant regurgitation have been critically evaluated with respect to their efficacy, safety and practical implications. The updated recommendations reached by the working party on the management of infant regurgigation contain five phases: (1A) parental reassurance; (1B) milk-thickening agents; (2) prokinetics; (3) positional therapy as an adjuvant therapy; (4A) H2-blockers; (4B) proton pump inhibitors; (5) surgery., SCOPUS: re.j, info:eu-repo/semantics/published
- Published
- 1997
29. Current concepts and issues in the management of regurgitation of infants: A reappraisal: Management guidelines from a working party
- Author
-
Vandenplas, Yvan, Belli, Dominique, Benhamou, Pierre Yves, Dupont, Christophe, Cadranel, Samy, Cézard, Jean-Pierre, Faure, Christophe, Cucchiara, Salvatore, Gottrand, Frederic, Hassall, Eric, Heymans, Hugo Sa, Kneepkens, Frank, Sandhu, Bhupinder Kaur, Vandenplas, Yvan, Belli, Dominique, Benhamou, Pierre Yves, Dupont, Christophe, Cadranel, Samy, Cézard, Jean-Pierre, Faure, Christophe, Cucchiara, Salvatore, Gottrand, Frederic, Hassall, Eric, Heymans, Hugo Sa, Kneepkens, Frank, and Sandhu, Bhupinder Kaur
- Abstract
Regurgitation in infants is a common problem. Recent issues, such as the increased risk of sudden infant death in the prone sleeping position, the finding of persisting occult gastro-oesophageal reflux with feed thickeners, and the increasing awareness of the cost-benefit ratio of medications may challenge the currently recommended management approach. A round table was organized to elaborate on the impact of (i) the pro supine sleeping campaigns in relation to sudden infant death and (ii) advancement in medical treatment on therapeutic strategies in regurgitating infants. The participants were opinion leaders from Europe and North America (Belgium, Canada, France, UK, Italy, Switzerland and The Netherlands). The importance of parental reassurance is stressed. As a consequence of the supine sleeping campaigns aiming to decrease the incidence of sudden infant death syndrome, the "prone elevated sleeping position" is no longer advised as a first-line therapeutic approach, although it is still recommended in "complicated reflux". It is emphasized that milk thickeners are an adequate therapeutic tool for regurgitation, but not in reflux disease. According to the literature, the efficacy of (alginate-)antacids, although very popular in some countries, is questionable. These recommendations will be of interest to first-line paediatricians, since about 40% of their patients, according to the literature, present because of regurgitation., SCOPUS: re.j, FLWNA, info:eu-repo/semantics/published
- Published
- 1996
30. Current concepts and issues in the management of regurgitation of infants: A reappraisal: Management guidelines from a working party
- Author
-
Vandenplas, Yvan, Belli, Dominique, Benhamou, Pierre Yves, Dupont, Christophe, Cadranel, Samy, Cézard, Jean-Pierre, Faure, Christophe, Cucchiara, Salvatore, Gottrand, Frederic, Hassall, Eric, Heymans, Hugo Sa, Kneepkens, Frank, Sandhu, Bhupinder Kaur, Vandenplas, Yvan, Belli, Dominique, Benhamou, Pierre Yves, Dupont, Christophe, Cadranel, Samy, Cézard, Jean-Pierre, Faure, Christophe, Cucchiara, Salvatore, Gottrand, Frederic, Hassall, Eric, Heymans, Hugo Sa, Kneepkens, Frank, and Sandhu, Bhupinder Kaur
- Abstract
Regurgitation in infants is a common problem. Recent issues, such as the increased risk of sudden infant death in the prone sleeping position, the finding of persisting occult gastro-oesophageal reflux with feed thickeners, and the increasing awareness of the cost-benefit ratio of medications may challenge the currently recommended management approach. A round table was organized to elaborate on the impact of (i) the pro supine sleeping campaigns in relation to sudden infant death and (ii) advancement in medical treatment on therapeutic strategies in regurgitating infants. The participants were opinion leaders from Europe and North America (Belgium, Canada, France, UK, Italy, Switzerland and The Netherlands). The importance of parental reassurance is stressed. As a consequence of the supine sleeping campaigns aiming to decrease the incidence of sudden infant death syndrome, the "prone elevated sleeping position" is no longer advised as a first-line therapeutic approach, although it is still recommended in "complicated reflux". It is emphasized that milk thickeners are an adequate therapeutic tool for regurgitation, but not in reflux disease. According to the literature, the efficacy of (alginate-)antacids, although very popular in some countries, is questionable. These recommendations will be of interest to first-line paediatricians, since about 40% of their patients, according to the literature, present because of regurgitation., SCOPUS: re.j, FLWNA, info:eu-repo/semantics/published
- Published
- 1996
31. Glial Cell Derived Neurotrophic Factor Induces Enteric Neurogenesis and Improves Colon Structure and Function in Mouse Models of Hirschsprung Disease
- Author
-
Soret, Rodolphe, Schneider, Sabine, Bernas, Guillaume, Christophers, Briana, Souchkova, Ouliana, Charrier, Baptiste, Righini-Grunder, Franziska, Aspirot, Ann, Landry, Mathieu, Kembel, Steven W., Faure, Christophe, Heuckeroth, Robert O., Pilon, Nicolas, Soret, Rodolphe, Schneider, Sabine, Bernas, Guillaume, Christophers, Briana, Souchkova, Ouliana, Charrier, Baptiste, Righini-Grunder, Franziska, Aspirot, Ann, Landry, Mathieu, Kembel, Steven W., Faure, Christophe, Heuckeroth, Robert O., and Pilon, Nicolas
- Abstract
Background & Aims: Hirschsprung disease (HSCR) is a life-threatening birth defect in which the distal colon is devoid of enteric neural ganglia. HSCR is treated by surgical removal of aganglionic bowel, but many children continue to have severe problems after surgery. We studied whether administration of glial cell derived neurotrophic factor (GDNF) induces enteric nervous system regeneration in mouse models of HSCR. Methods: We performed studies with four mouse models of HSCR: Holstein (HolTg/Tg, a model for trisomy 21-associated HSCR), TashT (TashTTg/Tg, a model for male-biased HSCR), Piebald-lethal(Ednrbs-l//s-l, a model for EDNRB mutation-associated HSCR), and Ret9/- (with aganglionosis induced by mycophenolate). Mice were given rectal enemas containing GDNF or saline (control) from postnatal days 4 through 8. We measured survival times of mice, and colon tissues were analyzed by histology, immunofluorescence, and immunoblots. Neural ganglia regeneration and structure, bowel motility, epithelial permeability, muscle thickness, and neutrophil infiltration were studied in colon tissues and in mice. Stool samples were collected, and microbiomes were analyzed by 16S rRNA gene sequencing. Time-lapse imaging and genetic cell-lineage tracing were used to identify a source of GDNF-targeted neural progenitors. Human aganglionic colon explants from children with HSCR were cultured with GDNF and evaluated for neurogenesis. Results: GDNF significantly prolonged mean survival times of HolTg/Tgmice, Ednrbs-l//s-l mice, and male TashTTg/Tg mice, compared with control mice, but not Ret9/- mice (which had mycophenolate toxicity). Mice given GDNF developed neurons and glia in distal bowel tissues that were aganglionic incontrol mice, had a significant increase in colon motility, and had significant decreases in epithelial permeability, muscle thickness, and neutrophil density. We observed dysbiosis in fecal samples from HolTg/Tg mice compared with feces from wild-type mice; fecal
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