Genomic imbalances in patients with a clinical presentation in the spectrum of Cornelia de Lange syndrome

BACKGROUND: Cornelia de Lange syndrome (CdLS) is a rare autosomal-dominant disorder characterised by facial dysmorphism, growth and psychomotor developmental delay and skeletal defects. To date, causative mutations in the NIPBL (cohesin regulator) and SMC1A (cohesin structural subunit) genes account...

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Autores principales: Gervasini, Cristina, Picinelli, Chiara, Azzollini, Jacopo, Rusconi, Daniela, Masciadri, Maura, Cereda, Anna, Marzocchi, Cinzia, Zampino, Giuseppe, Selicorni, Angelo, Tenconi, Romano, Russo, Silvia, Larizza, Lidia, Finelli, Palma
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3626829/
https://www.ncbi.nlm.nih.gov/pubmed/23551878
http://dx.doi.org/10.1186/1471-2350-14-41
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author Gervasini, Cristina
Picinelli, Chiara
Azzollini, Jacopo
Rusconi, Daniela
Masciadri, Maura
Cereda, Anna
Marzocchi, Cinzia
Zampino, Giuseppe
Selicorni, Angelo
Tenconi, Romano
Russo, Silvia
Larizza, Lidia
Finelli, Palma
author_facet Gervasini, Cristina
Picinelli, Chiara
Azzollini, Jacopo
Rusconi, Daniela
Masciadri, Maura
Cereda, Anna
Marzocchi, Cinzia
Zampino, Giuseppe
Selicorni, Angelo
Tenconi, Romano
Russo, Silvia
Larizza, Lidia
Finelli, Palma
author_sort Gervasini, Cristina
collection PubMed
description BACKGROUND: Cornelia de Lange syndrome (CdLS) is a rare autosomal-dominant disorder characterised by facial dysmorphism, growth and psychomotor developmental delay and skeletal defects. To date, causative mutations in the NIPBL (cohesin regulator) and SMC1A (cohesin structural subunit) genes account for > 50% and 6% of cases, respectively. METHODS: We recruited 50 patients with a CdLS clinical diagnosis or with features that overlap with CdLS, who were negative for mutations at NIPBL and SMC1A at molecular screening. Chromosomal rearrangements accounting for the clinical diagnosis were screened for using array Comparative Genomic Hybridisation (aCGH). RESULTS: Four patients were shown to carry imbalances considered to be candidates for having pathogenic roles in their clinical phenotypes: patient 1 had a 4.2 Mb de novo deletion at chromosome 20q11.2-q12; patient 2 had a 4.8 Mb deletion at chromosome 1p36.23-36.22; patient 3 carried an unbalanced translocation, t(7;17), with a 14 Mb duplication of chromosome 17q24.2-25.3 and a 769 Kb deletion at chromosome 7p22.3; patient 4 had an 880 Kb duplication of chromosome 19p13.3, for which his mother, who had a mild phenotype, was also shown to be a mosaic. CONCLUSIONS: Notwithstanding the variability in size and gene content of the rearrangements comprising the four different imbalances, they all map to regions containing genes encoding factors involved in cell cycle progression or genome stability. These functional similarities, also exhibited by the known CdLS genes, may explain the phenotypic overlap between the patients included in this study and CdLS. Our findings point to the complexity of the clinical diagnosis of CdLS and confirm the existence of phenocopies, caused by imbalances affecting multiple genomic regions, comprising 8% of patients included in this study, who did not have mutations at NIPBL and SMC1A. Our results suggests that analysis by aCGH should be recommended for CdLS spectrum cases with an unexplained clinical phenotype and included in the flow chart for diagnosis of cases with a clinical evaluation in the CdLS spectrum.
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spelling pubmed-36268292013-04-16 Genomic imbalances in patients with a clinical presentation in the spectrum of Cornelia de Lange syndrome Gervasini, Cristina Picinelli, Chiara Azzollini, Jacopo Rusconi, Daniela Masciadri, Maura Cereda, Anna Marzocchi, Cinzia Zampino, Giuseppe Selicorni, Angelo Tenconi, Romano Russo, Silvia Larizza, Lidia Finelli, Palma BMC Med Genet Research Article BACKGROUND: Cornelia de Lange syndrome (CdLS) is a rare autosomal-dominant disorder characterised by facial dysmorphism, growth and psychomotor developmental delay and skeletal defects. To date, causative mutations in the NIPBL (cohesin regulator) and SMC1A (cohesin structural subunit) genes account for > 50% and 6% of cases, respectively. METHODS: We recruited 50 patients with a CdLS clinical diagnosis or with features that overlap with CdLS, who were negative for mutations at NIPBL and SMC1A at molecular screening. Chromosomal rearrangements accounting for the clinical diagnosis were screened for using array Comparative Genomic Hybridisation (aCGH). RESULTS: Four patients were shown to carry imbalances considered to be candidates for having pathogenic roles in their clinical phenotypes: patient 1 had a 4.2 Mb de novo deletion at chromosome 20q11.2-q12; patient 2 had a 4.8 Mb deletion at chromosome 1p36.23-36.22; patient 3 carried an unbalanced translocation, t(7;17), with a 14 Mb duplication of chromosome 17q24.2-25.3 and a 769 Kb deletion at chromosome 7p22.3; patient 4 had an 880 Kb duplication of chromosome 19p13.3, for which his mother, who had a mild phenotype, was also shown to be a mosaic. CONCLUSIONS: Notwithstanding the variability in size and gene content of the rearrangements comprising the four different imbalances, they all map to regions containing genes encoding factors involved in cell cycle progression or genome stability. These functional similarities, also exhibited by the known CdLS genes, may explain the phenotypic overlap between the patients included in this study and CdLS. Our findings point to the complexity of the clinical diagnosis of CdLS and confirm the existence of phenocopies, caused by imbalances affecting multiple genomic regions, comprising 8% of patients included in this study, who did not have mutations at NIPBL and SMC1A. Our results suggests that analysis by aCGH should be recommended for CdLS spectrum cases with an unexplained clinical phenotype and included in the flow chart for diagnosis of cases with a clinical evaluation in the CdLS spectrum. BioMed Central 2013-04-03 /pmc/articles/PMC3626829/ /pubmed/23551878 http://dx.doi.org/10.1186/1471-2350-14-41 Text en Copyright © 2013 Gervasini et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Gervasini, Cristina
Picinelli, Chiara
Azzollini, Jacopo
Rusconi, Daniela
Masciadri, Maura
Cereda, Anna
Marzocchi, Cinzia
Zampino, Giuseppe
Selicorni, Angelo
Tenconi, Romano
Russo, Silvia
Larizza, Lidia
Finelli, Palma
Genomic imbalances in patients with a clinical presentation in the spectrum of Cornelia de Lange syndrome
title Genomic imbalances in patients with a clinical presentation in the spectrum of Cornelia de Lange syndrome
title_full Genomic imbalances in patients with a clinical presentation in the spectrum of Cornelia de Lange syndrome
title_fullStr Genomic imbalances in patients with a clinical presentation in the spectrum of Cornelia de Lange syndrome
title_full_unstemmed Genomic imbalances in patients with a clinical presentation in the spectrum of Cornelia de Lange syndrome
title_short Genomic imbalances in patients with a clinical presentation in the spectrum of Cornelia de Lange syndrome
title_sort genomic imbalances in patients with a clinical presentation in the spectrum of cornelia de lange syndrome
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3626829/
https://www.ncbi.nlm.nih.gov/pubmed/23551878
http://dx.doi.org/10.1186/1471-2350-14-41
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