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NEXN Gene in Cardiomyopathies and Sudden Cardiac Deaths: Prevalence, Phenotypic Expression, and Prognosis.
Hermida, Alexis; Ader, Flavie; Millat, Gilles; Jedraszak, Guillaume; Maury, Phillipe; Cador, Romain; Catalan, Pierre-Antoine; Clerici, Gaël; Combes, Nicolas; De Groote, Pascal; Dupin-Deguine, Delphine; Eschalier, Romain; Faivre, Laurence; Garcia, Patricia; Guillon, Benoit; Janin, Alexandre; Kugener, Beatrice; Lackmy, Marylin; Laredo, Mikael; Le Guillou, Xavier; Lesaffre, François; Lucron, Hugues; Milhem, Antoine; Nadeau, Gwenaël; Nguyen, Karine; Palmyre, Aurélien; Perdreau, Elodie; Picard, François; Rebotier, Nicolas; Richard, Pascale; Rooryck, Caroline; Seitz, Julien; Verloes, Alain; Vernier, Agathe; Winum, Pierre; Yabeta, Grace-A-Dieu; Bouchot, Océane; Chevalier, Philippe; Charron, Philippe; Gandjbakhch, Estelle.
Afiliação
  • Hermida A; Cardiology, Arrhythmia, and Cardiac Stimulation Service (A.H.), Amiens-Picardie University Hospital.
  • Ader F; EA4666 HEMATIM, University of Picardie-Jules Verne, Amiens (A.H., G.J.).
  • Millat G; Institute of Cardiology and ICAN Institute for Cardiometabolism and Nutrition (A.H., M. Laredo, P. Charron, E.G.).
  • Jedraszak G; Department of Genetics, Department of Cardiology, and Referral center for hereditary cardiac diseases, APHP, Pitié-Salpêtrière Hospital (A.H., P. Charron, E.G.).
  • Maury P; Unité Pédagogique de Biochimie, Département des Sciences Biologiques et Médicales, UFR de Pharmacie-Faculté de Santé, Université Paris Cité (F.A.).
  • Cador R; Unité Fonctionnelle de Cardiogénétique et Myogénétique Moléculaire et Cellulaire, DMU Biogem, Service de Biochimie Métabolique, AP-HP-Sorbonne Université, Pitié-Salpêtrière -Charles Foix (F.A., P.R.).
  • Catalan PA; Sorbonne Université, INSERM 1166, Paris (F.A., M. Laredo, P.R., P. Charron, E.G.).
  • Clerici G; Service de Génétique Moléculaire, Hospices Civils de Lyon (G.M., A.J.).
  • Combes N; Molecular Genetics Laboratory (G.J.), Amiens-Picardie University Hospital.
  • De Groote P; EA4666 HEMATIM, University of Picardie-Jules Verne, Amiens (A.H., G.J.).
  • Dupin-Deguine D; Service de Cardiologie (P.M.), CHU Toulouse.
  • Eschalier R; Service de Cardiologie, Hôpital Saint Joseph, Paris (R.C.).
  • Faivre L; Service de Cardiologie, CHU Clermont Ferrand (P.-A.C., R.E.).
  • Garcia P; Service de Cardiologie, Centre hospitalier universitaire, Saint Pierre, La Réunion (G.C.).
  • Guillon B; Service de Cardiologie, Clinique Pasteur, Toulouse (N.C.).
  • Janin A; France CHU Lille, Service de Cardiologie & Inserm U1167, Institut Pasteur de Lille (P.D.G.).
  • Kugener B; Service de Génétique (D.D.-D.), CHU Toulouse.
  • Lackmy M; Service de Cardiologie, CHU Clermont Ferrand (P.-A.C., R.E.).
  • Laredo M; Centre de Génétique, CHU Dijon (L.F.).
  • Le Guillou X; Unité Mort Inattendue du Nourrisson, Hôpital de la Conception, APHM, Marseille (P.G.).
  • Lesaffre F; Service de Cardiologie, CHU Besançon (B.G.).
  • Lucron H; Service de Génétique Moléculaire, Hospices Civils de Lyon (G.M., A.J.).
  • Milhem A; Urgences Pédiatriques (B.K.), Hôpital Louis Pradel, HCL, Lyon.
  • Nadeau G; Unité de Génétique Clinique, CHU de Guadeloupe, Pointe à Pitre (M. Lackmy).
  • Nguyen K; Institute of Cardiology and ICAN Institute for Cardiometabolism and Nutrition (A.H., M. Laredo, P. Charron, E.G.).
  • Palmyre A; Sorbonne Université, INSERM 1166, Paris (F.A., M. Laredo, P.R., P. Charron, E.G.).
  • Perdreau E; Service de Génétique Clinique, CHU Poitiers, Poitiers (X.L.G.).
  • Picard F; Service de Cardiologie, CHU Reims (F.L.).
  • Rebotier N; Service de Cardiologie pédiatrique, CHU Martinique, Fort-de-France (H.L.).
  • Richard P; Service de Cardiologie, CH La Rochelle (A.M.).
  • Rooryck C; Service de génétique clinique CH Métropole Savoie, Chambéry (G.N.).
  • Seitz J; Service de Génétique, APHM, Marseille (K.N.).
  • Verloes A; APHP, Ambroise Paré Hospital, Department of Genetics and Referral center for cardiac hereditary cardiac diseases, Boulogne-Billancourt (A.P., P. Charron).
  • Vernier A; Département médico chirurgical de cardiologie pédiatrique (E.P.), Hôpital Louis Pradel, HCL, Lyon.
  • Winum P; Service de Cardiologie, Hôpital Cardiologique Haut Leveque, Bordeaux (F.P.).
  • Yabeta GA; Service de Cardiologie, CH Basse-Terre (N.R.).
  • Bouchot O; Unité Fonctionnelle de Cardiogénétique et Myogénétique Moléculaire et Cellulaire, DMU Biogem, Service de Biochimie Métabolique, AP-HP-Sorbonne Université, Pitié-Salpêtrière -Charles Foix (F.A., P.R.).
  • Chevalier P; Sorbonne Université, INSERM 1166, Paris (F.A., M. Laredo, P.R., P. Charron, E.G.).
  • Charron P; CHU Bordeaux, Service de Génétique Médicale (C.R.).
  • Gandjbakhch E; Service de Cardiologie, Hôpital Saint Joseph, Marseille (J.S.).
Circ Genom Precis Med ; 17(1): e004285, 2024 Feb.
Article em En | MEDLINE | ID: mdl-38059363
ABSTRACT

BACKGROUND:

Few clinical data are available on NEXN mutation carriers, and the gene's involvement in cardiomyopathies or sudden death has not been fully established. Our objectives were to assess the prevalence of putative pathogenic variants in NEXN and to describe the phenotype and prognosis of patients carrying the variants.

METHODS:

DNA samples from consecutive patients with cardiomyopathy or sudden cardiac death/sudden infant death syndrome/idiopathic ventricular fibrillation were sequenced with a custom panel of genes. Index cases carrying at least one putative pathogenic variant in the NEXN gene were selected.

RESULTS:

Of the 9516 index patients sequenced, 31 were carriers of a putative pathogenic variant in NEXN only, including 2 with double variants and 29 with a single variant. Of the 29 unrelated probands with a single variant (16 males; median age at diagnosis, 32.0 [26.0-49.0] years), 21 presented with dilated cardiomyopathy (prevalence, 0.33%), and 3 presented with hypertrophic cardiomyopathy (prevalence, 0.14%). Three patients had idiopathic ventricular fibrillation, and there were 2 cases of sudden infant death syndrome (prevalence, 0.46%). For patients with dilated cardiomyopathy, the median left ventricle ejection fraction was 37.5% (26.25-50.0) at diagnosis and improved with treatment in 13 (61.9%). Over a median follow-up period of 6.0 years, we recorded 3 severe arrhythmic events and 2 severe hemodynamic events.

CONCLUSIONS:

Putative pathogenic NEXN variants were mainly associated with dilated cardiomyopathy; in these individuals, the prognosis appeared to be relatively good. However, severe and early onset phenotypes were also observed-especially in patients with double NEXN variants. We also detected NEXN variants in patients with hypertrophic cardiomyopathy and sudden infant death syndrome/idiopathic ventricular fibrillation, although a causal link could not be established.
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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Morte Súbita do Lactente / Fibrilação Ventricular / Cardiomiopatia Hipertrófica / Cardiomiopatia Dilatada / Cardiomiopatias Limite: Adult / Humans / Infant / Male / Middle aged Idioma: En Revista: Circ Genom Precis Med Ano de publicação: 2024 Tipo de documento: Article
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Morte Súbita do Lactente / Fibrilação Ventricular / Cardiomiopatia Hipertrófica / Cardiomiopatia Dilatada / Cardiomiopatias Limite: Adult / Humans / Infant / Male / Middle aged Idioma: En Revista: Circ Genom Precis Med Ano de publicação: 2024 Tipo de documento: Article