Possible incomplete penetrance of Xq28 int22h-1/int22h-2 duplication.

Billes, Alexis; Pujalte, Mathilde; Jedraszak, Guillaume; Amsallem, Daniel; Boudry-Labis, Elise; Boute, Odile; Bouquillon, Sonia; Brischoux-Boucher, Elise; Callier, Patrick; Coutton, Charles; Denizet, Anne-Laude Avice; Dieterich, Klaus; Kuentz, Paul; Lespinasse, James; Mazel, Benoît; Morin, Gilles; Amram, Florence; Pennamen, Perrine; Rio, Marlène; Piard, Juliette; Putoux, Audrey; Rama, Mélanie; Roze-Guillaumey, Virginie; Schluth-Bolard, Caroline; Till, Marianne; Trouvé, Chloé; Vieville, Gaëlle; Rooryck, Caroline; Sanlaville, Damien; Chatron, Nicolas

Billes, Alexis; Pujalte, Mathilde; Jedraszak, Guillaume; Amsallem, Daniel; Boudry-Labis, Elise; Boute, Odile; Bouquillon, Sonia; Brischoux-Boucher, Elise; Callier, Patrick; Coutton, Charles; Denizet, Anne-Laude Avice; Dieterich, Klaus; Kuentz, Paul; Lespinasse, James; Mazel, Benoît; Morin, Gilles; Amram, Florence; Pennamen, Perrine; Rio, Marlène; Piard, Juliette; Putoux, Audrey; Rama, Mélanie; Roze-Guillaumey, Virginie; Schluth-Bolard, Caroline; Till, Marianne; Trouvé, Chloé; Vieville, Gaëlle; Rooryck, Caroline; Sanlaville, Damien; Chatron, Nicolas.

Afiliação

Billes A; CHU Amiens Picardie, Service de Génétique Clinique, Amiens, France.
Pujalte M; CHU Amiens Picardie, Laboratoire de Génétique Constitutionnelle, Amiens, France.
Jedraszak G; Service de Génétique, Groupement Hospitalier Est, Hospices Civils de Lyon, Bron, France.
Amsallem D; CHU Amiens Picardie, Laboratoire de Génétique Constitutionnelle, Amiens, France.
Boudry-Labis E; CHU Amiens Picardie, Département de génétique, UR4666 HEMATIM, CURS, Université Picardie Jules Verne, Amiens, France.
Boute O; Service de Neuropédiatrie, CHU de Besançon, Besançon, France.
Bouquillon S; Institut de Génétique Médicale, Hôpital Jeanne de Flandre, Centre Hospitalier Universitaire de Lille, Lille, France.
Brischoux-Boucher E; Génétique Clinique, Centre Hospitalier Universitaire de Lille, Hôpital Jeanne de Flandre, Lille, France.
Callier P; Institut de Génétique Médicale, Hôpital Jeanne de Flandre, Centre Hospitalier Universitaire de Lille, Lille, France.
Coutton C; Centre de Génétique Humaine - CHU de Besançon, Université de Bourgogne-Franche-Comté, Besançon, France.
Denizet AA; Inserm UMR 1231 GAD Génétique des Anomalies du Développement, Université de Bourgogne, Dijon, France.
Dieterich K; Unité Fonctionnelle Innovation diagnostique dans les maladies rares, laboratoire de génétique chromosomique et moléculaire, Plateau Technique de Biologie, CHU Dijon Bourgogne, Dijon, France.
Kuentz P; Fédération Hospitalo-Universitaire Médecine Translationnelle et Anomalies du Développement (FHU TRANSLAD), CHU Dijon Bourgogne et Université de Bourgogne-Franche Comté, Dijon, France.
Lespinasse J; Service de Génétique, Génomique, et Procréation, Centre Hospitalier Universitaire Grenoble Alpes, La Tronche, France.
Mazel B; INSERM 1209, CNRS UMR 5309, Institut pour l'Avancée des Biosciences (IAB), Université Grenoble Alpes, Grenoble, France.
Morin G; Centre de Génétique Humaine - CHU de Besançon, Université de Bourgogne-Franche-Comté, Besançon, France.
Amram F; Université Grenoble Alpes, Inserm, U1216, CHU Grenoble Alpes, Medical Genetics, Grenoble Institute of Neurosciences, Grenoble, France.
Pennamen P; CHU Grenoble, UM Génétique Chromosomique, Grenoble, France.
Rio M; Oncobiologie Génétique Bioinformatique, PCBio, CHU de Besançon, Besançon, France.
Piard J; UFR Des Sciences de Santé, INSERM-Université de Bourgogne UMR1231 GAD "Génétique des Anomalies du Développement", FHUTRANSLAD, Dijon, France.
Putoux A; Centre Hospitalier de Chambéry, Service de Cytogénétique, Chambéry, France.
Rama M; Centre de Génétique et Centre de Référence Anomalies du Développement et Syndromes Malformatifs, FHUTRANSLAD - CHU Dijon Bourgogne, Dijon, France.
Roze-Guillaumey V; CHU Amiens Picardie, Service de Génétique Clinique, Amiens, France.
Schluth-Bolard C; CHU Amiens Picardie, Service de Génétique Clinique, Amiens, France.
Till M; CHU Bordeaux, Laboratoire de Génétique Biologique, Bordeaux, France.
Trouvé C; Université Paris Cité, Institut Imagine, Inserm U1163, Paris, France.
Vieville G; Service de Médecine Génomique des maladies rares, AP-HP, Centre Hôpital Necker-Enfants Malades, Paris, France.
Rooryck C; Centre de Génétique Humaine - CHU de Besançon, Université de Bourgogne-Franche-Comté, Besançon, France.
Sanlaville D; UMR 1231 GAD, Inserm, Université de Bourgogne Franche Comté, Dijon, France.
Chatron N; Hospices Civils de Lyon, Service de Génétique, Groupement Hospitalier Est, Bron, France.

Clin Genet ; 106(3): 234-246, 2024 Sep.

Article em En | MEDLINE | ID: mdl-38561231

ABSTRACT

ABSTRACT

Xq28 int22h-1/int22h-2 duplication is the result of non-allelic homologous recombination between int22h-1/int22h-2 repeats separated by 0.5 Mb. It is responsible for a syndromic form of intellectual disability (ID), with recurrent infections and atopic diseases. Minor defects, nonspecific facial dysmorphic features, and overweight have also been described. Half of female carriers have been reported with ID, whereas all reported evaluated born males present mild to moderate ID, suggesting complete penetrance. We collected data on 15 families from eight university hospitals. Among them, 40 patients, 21 females (one fetus), and 19 males (two fetuses), were carriers of typical or atypical Xq28 int22h-1/int22h-2 duplication. Twenty-one individuals were considered asymptomatic (16 females and 5 males), without significantly higher rate of recurrent infections, atopia, overweight, or facial dysmorphism. Approximately 67% live-born males and 23% live-born female carriers of the typical duplication did not have obvious signs of intellectual disability, suggesting previously undescribed incomplete penetrance or low expression in certain carriers. The possibility of a second-hit or modifying factors to this possible susceptibility locus is yet to be studied but a possible observational bias should be considered in assessing such challenging X-chromosome copy number gains. Additional segregation studies should help to quantify this newly described incomplete penetrance.

Assuntos

Cromossomos Humanos X; Deficiência Intelectual; Penetrância; Humanos; Masculino; Feminino; Cromossomos Humanos X/genética; Deficiência Intelectual/genética; Criança; Adulto; Adolescente; Pré-Escolar; Fenótipo; Duplicação Cromossômica/genética; Duplicação Gênica; Linhagem; Adulto Jovem

Palavras-chave

CLIC2; RAB39B; Xq28 duplication; Xq28 int22h1/int22h2 duplication; Xlinked intellectual disability; incomplete penetrance

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Penetrância / Cromossomos Humanos X / Deficiência Intelectual Limite: Adolescent / Adult / Child / Child, preschool / Female / Humans / Male Idioma: En Revista: Clin Genet Ano de publicação: 2024 Tipo de documento: Article País de afiliação: França

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