Two new cases of interstitial 7q35q36.1 deletion including CNTNAP2 and KMT2C

Lucie Tosca; Loïc Drévillon; Aurélie Mouka; Laure Lecerf; Audrey Briand; Valérie Ortonne; Virginie Benoit; Sophie Brisset; Lionel Van Maldergem; Quitterie Laudouar; Solveig Heide; Michel Goossens; Irina Giurgea; Gérard Tachdjian; Corinne Métay

doi:10.1002/mgg3.1645

Molecular Genetics & Genomic Medicine (Nov 2021)

Two new cases of interstitial 7q35q36.1 deletion including CNTNAP2 and KMT2C

Lucie Tosca,
Loïc Drévillon,
Aurélie Mouka,
Laure Lecerf,
Audrey Briand,
Valérie Ortonne,
Virginie Benoit,
Sophie Brisset,
Lionel Van Maldergem,
Quitterie Laudouar,
Solveig Heide,
Michel Goossens,
Irina Giurgea,
Gérard Tachdjian,
Corinne Métay

Affiliations

Lucie Tosca: Service d'Histologie, Embryologie et Cytogénétique AP‐HP. Université Paris SaclayHôpital Antoine Béclère Clamart France
Loïc Drévillon: Service d'Histologie, Embryologie et Cytogénétique AP‐HP. Université Paris SaclayHôpital Antoine Béclère Clamart France
Aurélie Mouka: Service d'Histologie, Embryologie et Cytogénétique AP‐HP. Université Paris SaclayHôpital Antoine Béclère Clamart France
Laure Lecerf: Service de Biochimie et Génétique AP‐HP. Hôpitaux Universitaires Henri MondorHôpital Henri Mondor Créteil France
Audrey Briand: Service de Biochimie et Génétique AP‐HP. Hôpitaux Universitaires Henri MondorHôpital Henri Mondor Créteil France
Valérie Ortonne: Service de Biochimie et Génétique AP‐HP. Hôpitaux Universitaires Henri MondorHôpital Henri Mondor Créteil France
Virginie Benoit: Service d'Histologie, Embryologie et Cytogénétique AP‐HP. Université Paris SaclayHôpital Antoine Béclère Clamart France
Sophie Brisset: Service d'Histologie, Embryologie et Cytogénétique AP‐HP. Université Paris SaclayHôpital Antoine Béclère Clamart France
Lionel Van Maldergem: Centre de Génétique Humaine Université de Franche‐Comté Besançon France
Quitterie Laudouar: Service de Réanimation Néonatale AP‐HP. Université Paris SaclayHôpital Bicêtre Le Kremlin‐Bicêtre France
Solveig Heide: UF Génétique Clinique AP‐HP. Sorbonne UniversitéHôpital universitaire Pitié‐Salpêtrière Paris France
Michel Goossens: Service de Biochimie et Génétique AP‐HP. Hôpitaux Universitaires Henri MondorHôpital Henri Mondor Créteil France
Irina Giurgea: Département de Génétique Médicale INSERM Childhood Genetic DiseasesAP‐HP. Sorbonne UniversitéHôpital Trousseau Paris France
Gérard Tachdjian: Service d'Histologie, Embryologie et Cytogénétique AP‐HP. Université Paris SaclayHôpital Antoine Béclère Clamart France
Corinne Métay: Service de Biochimie et Génétique AP‐HP. Hôpitaux Universitaires Henri MondorHôpital Henri Mondor Créteil France

DOI: https://doi.org/10.1002/mgg3.1645
Journal volume & issue: Vol. 9, no. 11
pp. n/a – n/a

Abstract

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Abstract Background Terminal deletions of the long arm of chromosome 7 are well known and frequently associated with syndromic holoprosencephaly due to the involvement of the SHH (aliases HHG1, SMMCI, TPT, TPTPS, and MCOPCB5) gene region. However, interstitial deletions including CNTNAP2 (aliases Caspr2, KIAA0868, and NRXN4) and excluding the SHH region are less common. Methods We report the clinical and molecular characterization associated with pure 7q35 and 7q35q36.1 deletion in two unrelated patients as detected by oligonucleotide‐based array‐CGH analysis. Results The common clinical features were abnormal maternal serum screening during first‐trimester pregnancy, low occipitofrontal circumference at birth, hypotonia, abnormal feet, developmental delay, impaired language development, generalized seizures, hyperactive behavior, friendly personality, and cranio‐facial dysmorphism. Both deletions occurred de novo and sequencing of CNTNAP2, a candidate gene for epilepsy and autism showed absence of mutation on the contralateral allele. Conclusion Combined haploinsufficiency of GALNTL5 (alias GalNAc‐T5L), CUL1, SSPO (aliases SCO‐spondin, KIAA0543, and FLJ36112), AOC1 (alias DAO), RHEB, and especially KMT2C (alias KIAA1506 and HALR) with monoallelic disruption of CNTNAP2 may explain neurologic abnormalities, hypotonia, and exostoses. Haploinsufficiency of PRKAG2 (aliases AAKG, AAKG2, H91620p, WPWS, and CMH6) and KCNH2 (aliases Kv11.1, HERG, and erg1) genes may be responsible of long QT syndrome observed for one patient.

Published in Molecular Genetics & Genomic Medicine

ISSN: 2324-9269 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General): Genetics
Website: https://onlinelibrary.wiley.com/journal/23249269

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