Diagnostic yield of next-generation sequencing in very early-onset inflammatory bowel diseases: a multicenter study

Charbit-Henrion, F.; Parlato, M.; Hanein, S.; Duclaux-Loras, R.; Nowak, J.; Begue, B.; Rakotobe, S.; Bruneau, J.; Fourrage, C.; Alibeu, O.; Rieux-Laucat, F.; Lévy, E.; Stolzenberg, M.; Mazerolles, F.; Latour, S.; Lenoir, C.; Fischer, A.; Picard, C.; Aloi, M.; Dias, J.A.; Hariz, M.B.; Bourrier, A.; Breuer, C.; Breton, A.; Bronsky, J.; Buderus, S.; Cananzi, M.; Coopman, S.; Crémilleux, C.; Dabadie, A.; Dumant-Forest, C.; Gurkan, O.E.; Fabre, A.; Fischer, A.; Diaz, M.G.; Gonzalez-Lama, Y.; Goulet, O.; Guariso, G.; Gurcan, N.; Homan, M.; Hugot, J.; Jeziorski, E.; Karanika, E.; Lachaux, A.; Lewindon, P.; Lima, R.; Magro, F.; Major, J.; Malamut, G.; Mas, E.; Mattyus, I.; Mearin, L.M.; Melek, J.; Navas-Lopez, V.M.; Paerregaard, A.; Pelatan, C.; Pigneur, B.; Pais, I.P.; Rebeuh, J.; Romano, C.; Siala, N.; Strisciuglio, C.; Tempia-Caliera, M.; Tounian, P.; Turner, D.; Urbonas, V.; Willot, S.; Ruemmele, F.M.; Cerf-Bensussan, N.

doi:10.1093/ecco-jcc/jjy068

Background and aims: An expanding number of monogenic defects have been identified as causative of severe forms of very early-onset inflammatory bowel diseases [VEO-IBD]. The present study aimed at defining how next-generation sequencing [NGS] methods can be used to improve identification of known molecular diagnosis and to adapt treatment. Methods: A total of 207 children were recruited in 45 paediatric centres through an international collaborative network [ESPGHAN GENIUS working group] with a clinical presentation of severe VEO-IBD [n = 185] or an anamnesis suggestive of a monogenic disorder [n = 22]. Patients were divided at inclusion into three phenotypic subsets: predominantly small bowel inflammation, colitis with perianal lesions, and colitis only. Methods to obtain molecular diagnosis included functional tests followed by specific Sanger sequencing, custom-made targeted NGS, and in selected cases whole exome sequencing [WES] of parents-child trios. Genetic findings were validated clinically and/or functionally. Results: Molecular diagnosis was achieved in 66/207 children [32%]: 61% with small bowel inflammation, 39% with colitis and perianal lesions, and 18% with colitis only. Targeted NGS pinpointed gene mutations causative of atypical presentations, and identified large exonic copy number variations previously missed by WES. Conclusions: Our results lead us to propose an optimised diagnostic strategy to identify known monogenic causes of severe IBD.

Diagnostic yield of next-generation sequencing in very early-onset inflammatory bowel diseases: a multicenter study / F. Charbit-Henrion, M. Parlato, S. Hanein, R. Duclaux-Loras, J. Nowak, B. Begue, S. Rakotobe, J. Bruneau, C. Fourrage, O. Alibeu, F. Rieux-Laucat, E. Lévy, M. Stolzenberg, F. Mazerolles, S. Latour, C. Lenoir, A. Fischer, C. Picard, M. Aloi, J.A. Dias, M.B. Hariz, A. Bourrier, C. Breuer, A. Breton, J. Bronsky, S. Buderus, M. Cananzi, S. Coopman, C. Crémilleux, A. Dabadie, C. Dumant-Forest, O.E. Gurkan, A. Fabre, A. Fischer, M.G. Diaz, Y. Gonzalez-Lama, O. Goulet, G. Guariso, N. Gurcan, M. Homan, J. Hugot, E. Jeziorski, E. Karanika, A. Lachaux, P. Lewindon, R. Lima, F. Magro, J. Major, G. Malamut, E. Mas, I. Mattyus, L.M. Mearin, J. Melek, V.M. Navas-Lopez, A. Paerregaard, C. Pelatan, B. Pigneur, I.P. Pais, J. Rebeuh, C. Romano, N. Siala, C. Strisciuglio, M. Tempia-Caliera, P. Tounian, D. Turner, V. Urbonas, S. Willot, F.M. Ruemmele, N. Cerf-Bensussan. - In: JOURNAL OF CROHN'S AND COLITIS. - ISSN 1873-9946. - 12:9(2018 Sep), pp. 1104-1112. [10.1093/ecco-jcc/jjy068]

Diagnostic yield of next-generation sequencing in very early-onset inflammatory bowel diseases: a multicenter study

Charbit-Henrion, Fabienne^Primo;Parlato, Marianna^Secondo;Hanein, Sylvain;Duclaux-Loras, Rémi;Nowak, Jan;Begue, Bernadette;Rakotobe, Sabine;Bruneau, Julie;Fourrage, Cécile;Alibeu, Olivier;Rieux-Laucat, Frédéric;Lévy, Eva;Stolzenberg, Marie-Claude;Mazerolles, Fabienne;Latour, Sylvain;Lenoir, Christelle;Fischer, Alain;Picard, Capucine;M. Aloi;Dias, Jorge Amil;Hariz, Mongi Ben;Bourrier, Anne;Breuer, Christian;Breton, Anne;Bronsky, Jiri;Buderus, Stephan;Cananzi, Mara;Coopman, Stéphanie;Crémilleux, Clara;Dabadie, Alain;Dumant-Forest, Clémentine;Gurkan, Odul Egritas;Fabre, Alexandre;Fischer, Aude;Diaz, Marta German;Gonzalez-Lama, Yago;Goulet, Olivier;Guariso, Graziella;Gurcan, Neslihan;Homan, Matjaz;Hugot, Jean-Pierre;Jeziorski, Eric;Karanika, Evi;Lachaux, Alain;Lewindon, Peter;Lima, Rosa;Magro, Fernando;Major, Janos;Malamut, Georgia;Mas, Emmanuel;Mattyus, Istvan;Mearin, Luisa M;Melek, Jan;Navas-Lopez, Victor Manuel;Paerregaard, Anders;Pelatan, Cecile;Pigneur, Bénédicte;Pais, Isabel Pinto;Rebeuh, Julie;Romano, Claudio;Siala, Nadia;Strisciuglio, Caterina;Tempia-Caliera, Michela;Tounian, Patrick;Turner, Dan;Urbonas, Vaidotas;Willot, Stéphanie;Ruemmele, Frank M^Penultimo;

2018

Abstract

Background and aims: An expanding number of monogenic defects have been identified as causative of severe forms of very early-onset inflammatory bowel diseases [VEO-IBD]. The present study aimed at defining how next-generation sequencing [NGS] methods can be used to improve identification of known molecular diagnosis and to adapt treatment. Methods: A total of 207 children were recruited in 45 paediatric centres through an international collaborative network [ESPGHAN GENIUS working group] with a clinical presentation of severe VEO-IBD [n = 185] or an anamnesis suggestive of a monogenic disorder [n = 22]. Patients were divided at inclusion into three phenotypic subsets: predominantly small bowel inflammation, colitis with perianal lesions, and colitis only. Methods to obtain molecular diagnosis included functional tests followed by specific Sanger sequencing, custom-made targeted NGS, and in selected cases whole exome sequencing [WES] of parents-child trios. Genetic findings were validated clinically and/or functionally. Results: Molecular diagnosis was achieved in 66/207 children [32%]: 61% with small bowel inflammation, 39% with colitis and perianal lesions, and 18% with colitis only. Targeted NGS pinpointed gene mutations causative of atypical presentations, and identified large exonic copy number variations previously missed by WES. Conclusions: Our results lead us to propose an optimised diagnostic strategy to identify known monogenic causes of severe IBD.

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	Parole chiave
	
				Genetics and molecular epidemiology; TNGS; VEO-IBD; monogenic disorders; paediatrics;
			
	Settori scientifico-disciplinari dell'articolo (validi dal 09/05/2024)
	
				Settore MEDS-20/A - Pediatria generale e specialistica
			
	Titolo del progetto
	
	Titolo Progetto
	
									Host-microbiota interactions across the gut immune system:lessons from early onset inflammatory bowel diseases and from gnotobiotic mice
								
	Acronimo
	
									IMMUNOBIOTA
								
	Nome finanziatore
	
										European Commission
									
	Finanziamento
	
									SEVENTH FRAMEWORK PROGRAMME - SP2-Ideas - ERC
								
	N. Contratto
	
									339407
								
	Data di pubblicazione
	
				set-2018
			
	Data ahead of print o data di stampa
	
				18-mag-2018
			
	Rivista in ANCE
	
				JOURNAL OF CROHN'S AND COLITIS
			
	DOI
	
				https://dx.doi.org/10.1093/ecco-jcc/jjy068
			
	Tipologia
	
				Article (author)
			
	Appare nelle tipologie:
	
				01 - Articolo su periodico

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