Myhre and LAPS syndromes: clinical and molecular review of 32 patients

Caroline Michot; Carine Le Goff; Clémentine Mahaut; Alexandra Afenjar; Alice S. Brooks; Philippe M. Campeau; Anne Destree; Maja Di Rocco; Dian Donnai; Raoul Hennekam; Delphine Heron; Sébastien Jacquemont; Peter Kannu; Angela E. Lin; Sylvie Manouvrier-Hanu; Sahar Mansour; Sandrine Marlin; Ruth McGowan; Helen Murphy; Annick Raas-Rothschild; Marlène Rio; Marleen Simon; Irene Stolte-Dijkstra; James R. Stone; Yves Sznajer; John Tolmie; Renaud Touraine; Jenneke van den Ende; Nathalie van der Aa; Ton van Essen; Alain Verloes; Arnold Munnich; Valérie Cormier-Daire

doi:https://doi.org/10.1038/ejhg.2013.288

Myhre and LAPS syndromes: clinical and molecular review of 32 patients

Caroline Michot, Carine Le Goff, Clémentine Mahaut, Alexandra Afenjar, Alice S. Brooks, Philippe M. Campeau, Anne Destree, Maja Di Rocco, Dian Donnai, Raoul Hennekam, Delphine Heron, Sébastien Jacquemont, Peter Kannu, Angela E. Lin, Sylvie Manouvrier-Hanu, Sahar Mansour, Sandrine Marlin, Ruth McGowan, Helen Murphy, Annick Raas-RothschildMarlène Rio, Marleen Simon, Irene Stolte-Dijkstra, James R. Stone, Yves Sznajer, John Tolmie, Renaud Touraine, Jenneke van den Ende, Nathalie van der Aa, Ton van Essen, Alain Verloes, Arnold Munnich, Valérie Cormier-Daire

Research output: Contribution to journal › Review article › Academic › peer-review

38 Citations (Scopus)

Abstract

Myhre syndrome is characterized by short stature, brachydactyly, facial features, pseudomuscular hypertrophy, joint limitation and hearing loss. We identified SMAD4 mutations as the cause of Myhre syndrome. SMAD4 mutations have also been identified in laryngotracheal stenosis, arthropathy, prognathism and short stature syndrome (LAPS). This study aimed to review the features of Myhre and LAPS patients to define the clinical spectrum of SMAD4 mutations. We included 17 females and 15 males ranging in age from 8 to 48 years. Thirty were diagnosed with Myhre syndrome and two with LAPS. SMAD4 coding sequence was analyzed by Sanger sequencing. Clinical and radiological features were collected from a questionnaire completed by the referring physicians. All patients displayed a typical facial gestalt, thickened skin, joint limitation and muscular pseudohypertrophy. Growth retardation was common (68.7%) and was variable in severity (from -5.5 to -2 SD), as was mild-to-moderate intellectual deficiency (87.5%) with additional behavioral problems in 56.2% of the patients. Significant health concerns like obesity, arterial hypertension, bronchopulmonary insufficiency, laryngotracheal stenosis, pericarditis and early death occurred in four. Twenty-nine patients had a de novo heterozygous SMAD4 mutation, including both patients with LAPS. In 27 cases mutation affected Ile500 and in two cases Arg496. The three patients without SMAD4 mutations had typical findings of Myhre syndrome. Myhre-LAPS syndrome is a clinically homogenous condition with life threatening complications in the course of the disease. Our identification of SMAD4 mutations in 29/32 cases confirms that SMAD4 is the major gene responsible for Myhre syndrome

Original language	English
Pages (from-to)	1272-1277
Journal	European journal of human genetics
Volume	22
Issue number	11
DOIs	https://doi.org/10.1038/ejhg.2013.288
Publication status	Published - 2014

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https://doi.org/10.1038/ejhg.2013.288

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Michot, C., Le Goff, C., Mahaut, C., Afenjar, A., Brooks, A. S., Campeau, P. M., Destree, A., Di Rocco, M., Donnai, D., Hennekam, R., Heron, D., Jacquemont, S., Kannu, P., Lin, A. E., Manouvrier-Hanu, S., Mansour, S., Marlin, S., McGowan, R., Murphy, H., ... Cormier-Daire, V. (2014). Myhre and LAPS syndromes: clinical and molecular review of 32 patients. European journal of human genetics, 22(11), 1272-1277. https://doi.org/10.1038/ejhg.2013.288

@article{9a7e5e375d9d4559ab622622ba85abae,

title = "Myhre and LAPS syndromes: clinical and molecular review of 32 patients",

abstract = "Myhre syndrome is characterized by short stature, brachydactyly, facial features, pseudomuscular hypertrophy, joint limitation and hearing loss. We identified SMAD4 mutations as the cause of Myhre syndrome. SMAD4 mutations have also been identified in laryngotracheal stenosis, arthropathy, prognathism and short stature syndrome (LAPS). This study aimed to review the features of Myhre and LAPS patients to define the clinical spectrum of SMAD4 mutations. We included 17 females and 15 males ranging in age from 8 to 48 years. Thirty were diagnosed with Myhre syndrome and two with LAPS. SMAD4 coding sequence was analyzed by Sanger sequencing. Clinical and radiological features were collected from a questionnaire completed by the referring physicians. All patients displayed a typical facial gestalt, thickened skin, joint limitation and muscular pseudohypertrophy. Growth retardation was common (68.7%) and was variable in severity (from -5.5 to -2 SD), as was mild-to-moderate intellectual deficiency (87.5%) with additional behavioral problems in 56.2% of the patients. Significant health concerns like obesity, arterial hypertension, bronchopulmonary insufficiency, laryngotracheal stenosis, pericarditis and early death occurred in four. Twenty-nine patients had a de novo heterozygous SMAD4 mutation, including both patients with LAPS. In 27 cases mutation affected Ile500 and in two cases Arg496. The three patients without SMAD4 mutations had typical findings of Myhre syndrome. Myhre-LAPS syndrome is a clinically homogenous condition with life threatening complications in the course of the disease. Our identification of SMAD4 mutations in 29/32 cases confirms that SMAD4 is the major gene responsible for Myhre syndrome",

author = "Caroline Michot and {Le Goff}, Carine and Cl{\'e}mentine Mahaut and Alexandra Afenjar and Brooks, {Alice S.} and Campeau, {Philippe M.} and Anne Destree and {Di Rocco}, Maja and Dian Donnai and Raoul Hennekam and Delphine Heron and S{\'e}bastien Jacquemont and Peter Kannu and Lin, {Angela E.} and Sylvie Manouvrier-Hanu and Sahar Mansour and Sandrine Marlin and Ruth McGowan and Helen Murphy and Annick Raas-Rothschild and Marl{\`e}ne Rio and Marleen Simon and Irene Stolte-Dijkstra and Stone, {James R.} and Yves Sznajer and John Tolmie and Renaud Touraine and {van den Ende}, Jenneke and {van der Aa}, Nathalie and {van Essen}, Ton and Alain Verloes and Arnold Munnich and Val{\'e}rie Cormier-Daire",

year = "2014",

doi = "https://doi.org/10.1038/ejhg.2013.288",

language = "English",

volume = "22",

pages = "1272--1277",

journal = "European journal of human genetics",

issn = "1018-4813",

publisher = "Nature Publishing Group",

number = "11",

}

Michot, C, Le Goff, C, Mahaut, C, Afenjar, A, Brooks, AS, Campeau, PM, Destree, A, Di Rocco, M, Donnai, D, Hennekam, R, Heron, D, Jacquemont, S, Kannu, P, Lin, AE, Manouvrier-Hanu, S, Mansour, S, Marlin, S, McGowan, R, Murphy, H, Raas-Rothschild, A, Rio, M, Simon, M, Stolte-Dijkstra, I, Stone, JR, Sznajer, Y, Tolmie, J, Touraine, R, van den Ende, J, van der Aa, N, van Essen, T, Verloes, A, Munnich, A & Cormier-Daire, V 2014, 'Myhre and LAPS syndromes: clinical and molecular review of 32 patients', European journal of human genetics, vol. 22, no. 11, pp. 1272-1277. https://doi.org/10.1038/ejhg.2013.288

TY - JOUR

T1 - Myhre and LAPS syndromes: clinical and molecular review of 32 patients

AU - Michot, Caroline

AU - Le Goff, Carine

AU - Mahaut, Clémentine

AU - Afenjar, Alexandra

AU - Brooks, Alice S.

AU - Campeau, Philippe M.

AU - Destree, Anne

AU - Di Rocco, Maja

AU - Donnai, Dian

AU - Hennekam, Raoul

AU - Heron, Delphine

AU - Jacquemont, Sébastien

AU - Kannu, Peter

AU - Lin, Angela E.

AU - Manouvrier-Hanu, Sylvie

AU - Mansour, Sahar

AU - Marlin, Sandrine

AU - McGowan, Ruth

AU - Murphy, Helen

AU - Raas-Rothschild, Annick

AU - Rio, Marlène

AU - Simon, Marleen

AU - Stolte-Dijkstra, Irene

AU - Stone, James R.

AU - Sznajer, Yves

AU - Tolmie, John

AU - Touraine, Renaud

AU - van den Ende, Jenneke

AU - van der Aa, Nathalie

AU - van Essen, Ton

AU - Verloes, Alain

AU - Munnich, Arnold

AU - Cormier-Daire, Valérie

PY - 2014

Y1 - 2014

N2 - Myhre syndrome is characterized by short stature, brachydactyly, facial features, pseudomuscular hypertrophy, joint limitation and hearing loss. We identified SMAD4 mutations as the cause of Myhre syndrome. SMAD4 mutations have also been identified in laryngotracheal stenosis, arthropathy, prognathism and short stature syndrome (LAPS). This study aimed to review the features of Myhre and LAPS patients to define the clinical spectrum of SMAD4 mutations. We included 17 females and 15 males ranging in age from 8 to 48 years. Thirty were diagnosed with Myhre syndrome and two with LAPS. SMAD4 coding sequence was analyzed by Sanger sequencing. Clinical and radiological features were collected from a questionnaire completed by the referring physicians. All patients displayed a typical facial gestalt, thickened skin, joint limitation and muscular pseudohypertrophy. Growth retardation was common (68.7%) and was variable in severity (from -5.5 to -2 SD), as was mild-to-moderate intellectual deficiency (87.5%) with additional behavioral problems in 56.2% of the patients. Significant health concerns like obesity, arterial hypertension, bronchopulmonary insufficiency, laryngotracheal stenosis, pericarditis and early death occurred in four. Twenty-nine patients had a de novo heterozygous SMAD4 mutation, including both patients with LAPS. In 27 cases mutation affected Ile500 and in two cases Arg496. The three patients without SMAD4 mutations had typical findings of Myhre syndrome. Myhre-LAPS syndrome is a clinically homogenous condition with life threatening complications in the course of the disease. Our identification of SMAD4 mutations in 29/32 cases confirms that SMAD4 is the major gene responsible for Myhre syndrome

AB - Myhre syndrome is characterized by short stature, brachydactyly, facial features, pseudomuscular hypertrophy, joint limitation and hearing loss. We identified SMAD4 mutations as the cause of Myhre syndrome. SMAD4 mutations have also been identified in laryngotracheal stenosis, arthropathy, prognathism and short stature syndrome (LAPS). This study aimed to review the features of Myhre and LAPS patients to define the clinical spectrum of SMAD4 mutations. We included 17 females and 15 males ranging in age from 8 to 48 years. Thirty were diagnosed with Myhre syndrome and two with LAPS. SMAD4 coding sequence was analyzed by Sanger sequencing. Clinical and radiological features were collected from a questionnaire completed by the referring physicians. All patients displayed a typical facial gestalt, thickened skin, joint limitation and muscular pseudohypertrophy. Growth retardation was common (68.7%) and was variable in severity (from -5.5 to -2 SD), as was mild-to-moderate intellectual deficiency (87.5%) with additional behavioral problems in 56.2% of the patients. Significant health concerns like obesity, arterial hypertension, bronchopulmonary insufficiency, laryngotracheal stenosis, pericarditis and early death occurred in four. Twenty-nine patients had a de novo heterozygous SMAD4 mutation, including both patients with LAPS. In 27 cases mutation affected Ile500 and in two cases Arg496. The three patients without SMAD4 mutations had typical findings of Myhre syndrome. Myhre-LAPS syndrome is a clinically homogenous condition with life threatening complications in the course of the disease. Our identification of SMAD4 mutations in 29/32 cases confirms that SMAD4 is the major gene responsible for Myhre syndrome

U2 - https://doi.org/10.1038/ejhg.2013.288

DO - https://doi.org/10.1038/ejhg.2013.288

M3 - Review article

C2 - 24424121

SN - 1018-4813

VL - 22

SP - 1272

EP - 1277

JO - European journal of human genetics

JF - European journal of human genetics

IS - 11

ER -