Clinical and Molecular Study of 320 Children With Marfan Syndrome and Related Type I Fibrillinopathies in a Series of 1009 Probands With Pathogenic FBN1 Mutations

被引:109
作者
Faivre, Laurence [1 ,2 ]
Masurel-Paulet, Alice [1 ]
Collod-Beroud, Gwenaelle [3 ,4 ]
Callewaert, Bert L. [5 ]
Child, Anne H. [6 ]
Stheneur, Chantal [7 ]
Binquet, Christine [2 ,9 ]
Gautier, Elodie [2 ,9 ]
Chevallier, Bertrand [7 ]
Huet, Frederic [1 ]
Loeys, Bart L. [5 ,10 ,11 ]
Arbustini, Eloisa [12 ]
Mayer, Karin [13 ]
Arslan-Kirchner, Mine [14 ]
Kiotsekoglou, Anatoli [7 ]
Comeglio, Paolo [7 ]
Grasso, Maurizia [12 ]
Halliday, Dorothy J. [15 ]
Beroud, Christophe [3 ,4 ,16 ]
Bonithon-Kopp, Claire [2 ,9 ]
Claustres, Mireille [3 ,4 ,16 ]
Robinson, Peter N. [17 ]
Ades, Lesley [18 ,19 ,20 ]
De Backer, Julie [5 ]
Coucke, Paul [5 ]
Francke, Uta [21 ]
De Paepe, Anne [5 ]
Boileau, Catherine [8 ]
Jondeau, Guillaume [22 ]
机构
[1] CHU Dijon, Ctr Genet, Dijon, France
[2] CHU Dijon, Ctr Clin Invest Epidemiol Clin Trials, Dijon, France
[3] INSERM, U827, Montpellier, France
[4] Univ Montpellier 1, Montpellier, France
[5] Ghent Univ Hosp, Ctr Genet Med, B-9000 Ghent, Belgium
[6] Univ London St Georges Hosp, Dept Cardiol Sci, London, England
[7] Univ Versailles, Hop Ambroise Pare, Assistance Publ Hop Paris, Serv Pediat, Boulogne, France
[8] Univ Versailles, Hop Ambroise Pare, Assistance Publ Hop Paris, Mol Genet Lab, Boulogne, France
[9] Ctr Invest Epidemiol, INSERM, Dijon, France
[10] Johns Hopkins Univ, Sch Med, Inst Med Genet, Baltimore, MD USA
[11] Johns Hopkins Univ, Sch Med, Howard Hughes Med Inst, Baltimore, MD 21205 USA
[12] Fdn Inst Ricovero Cura Carattere Sci Policlin San, Ctr Inherited Cardiovasc Dis, Pavia, Italy
[13] Ctr Human Genet & Lab Med, Martinsried, Germany
[14] Inst Human Genet, Hannover, Germany
[15] Univ Oxford, Dept Biochem, Oxford OX1 3QU, England
[16] CHU Montpellier, Arnault de Villeneuve Hosp, Mol Genet Lab, Montpellier, France
[17] Charite Univ Med Berlin, Inst Med Genet, D-13353 Berlin, Germany
[18] Childrens Hosp Westmead, Marfan Res Grp, Sydney, NSW, Australia
[19] Childrens Hosp Westmead, Dept Clin Genet, Sydney, NSW, Australia
[20] Univ Sydney, Discipline Paediat & Child Hlth, Sydney, NSW, Australia
[21] Stanford Univ, Med Ctr, Dept Genet & Pediat, Stanford, CA 94305 USA
[22] Hop Xavier Bichat, AP HP, Paris, France
来源
PEDIATRICS | 2009年 / 123卷 / 01期
关键词
Marfan syndrome; FBN1; childhood; international criteria; CARDIOVASCULAR MANIFESTATIONS; MENTAL-RETARDATION; NATURAL-HISTORY; CHILDHOOD; FIBRILLIN-1; PREVALENCE; DISORDERS; DIAGNOSIS; PHENOTYPE; CRITERIA;
D O I
10.1542/peds.2008-0703
中图分类号
R72 [儿科学];
学科分类号
100202 ;
摘要
From a large series of 1009 probands with pathogenic FBN1 mutations, data for 320 patients <18 years of age at the last follow-up evaluation were analyzed (32%). At the time of diagnosis, the median age was 6.5 years. At the last examination, the population was classified as follows: neonatal Marfan syndrome, 14%; severe Marfan syndrome, 19%; classic Marfan syndrome, 32%; probable Marfan syndrome, 35%. Seventy-one percent had ascending aortic dilation, 55% ectopia lentis, and 28% major skeletal system involvement. Even when aortic complications existed in childhood, the rates of aortic surgery and aortic dissection remained low (5% and 1%, respectively). Some diagnostic features (major skeletal system involvement, striae, dural ectasia, and family history) were more frequent in the 10- to <18-year age group, whereas others (ascending aortic dilation and mitral abnormalities) were more frequent in the population with neonatal Marfan syndrome. Only 56% of children could be classified as having Marfan syndrome, according to international criteria, at their last follow-up evaluation when the presence of a FBN1 mutation was not considered as a major feature, with increasing frequency in the older age groups. Eighty-five percent of child probands fulfilled international criteria after molecular studies, which indicates that the discovery of a FBN1 mutation can be a valuable diagnostic aid in uncertain cases. The distributions of mutation types and locations in this pediatric series revealed large proportions of probands carrying mutations located in exons 24 to 32 (33%) and in-frame mutations (75%). Apart from lethal neonatal Marfan syndrome, we confirm that the majority of clinical manifestations of Marfan syndrome increase with age, which emphasizes the poor applicability of the international criteria to this diagnosis in childhood and the need for follow-up monitoring in cases of clinical suspicion of Marfan syndrome. Pediatrics 2009;123:391-398
引用
收藏
页码:391 / 398
页数:8
相关论文
共 31 条
  • [1] FBN1, TGFBR1, and the Marfan-craniosynostosis/mental retardation disorders revisited
    Ades, LC
    Sullivan, K
    Biggin, A
    Haan, EA
    Brett, M
    Holman, KJ
    Dixon, J
    Robertson, S
    Holmes, AD
    Rogers, J
    Bennetts, B
    [J]. AMERICAN JOURNAL OF MEDICAL GENETICS PART A, 2006, 140A (10) : 1047 - 1058
  • [2] BEIGHTON P, 1986, AM J MED GENET, V29, P581
  • [3] UMD (Universal Mutation Database):: 2005 update
    Béroud, C
    Hamroun, D
    Collod-Béroud, G
    Boileau, C
    Soussi, T
    Claustres, M
    [J]. HUMAN MUTATION, 2005, 26 (03) : 184 - 191
  • [4] Child AH, 2004, MED INTELL UNIT, P13
  • [5] Update of the UMD-FBN1 mutation database and creation of an FBN1 polymorphlism database
    Collod-Béroud, G
    Le Bourdelles, S
    Ades, L
    Ala-Kokko, L
    Booms, P
    Boxer, M
    Child, A
    Comeglio, P
    De Paepe, A
    Hyland, JC
    Holman, K
    Kaitila, I
    Loeys, B
    Matyas, G
    Nuytinck, L
    Peltonen, L
    Rantamaki, T
    Robinson, P
    Steinmann, B
    Junien, C
    Béroud, C
    Boileau, C
    [J]. HUMAN MUTATION, 2003, 22 (03) : 199 - 208
  • [6] DePaepe A, 1996, AM J MED GENET, V62, P417, DOI 10.1002/(SICI)1096-8628(19960424)62:4<417::AID-AJMG15>3.0.CO
  • [7] 2-R
  • [8] MARFAN-SYNDROME CAUSED BY A RECURRENT DENOVO MISSENSE MUTATION IN THE FIBRILLIN GENE
    DIETZ, HC
    CUTTING, GR
    PYERITZ, RE
    MASLEN, CL
    SAKAI, LY
    CORSON, GM
    PUFFENBERGER, EG
    HAMOSH, A
    NANTHAKUMAR, EJ
    CURRISTIN, SM
    STETTEN, G
    MEYERS, DA
    FRANCOMANO, CA
    [J]. NATURE, 1991, 352 (6333) : 337 - 339
  • [9] CARDIOVASCULAR MANIFESTATIONS OF MARFAN-SYNDROME IN THE YOUNG
    ELHABBAL, MH
    [J]. AMERICAN HEART JOURNAL, 1992, 123 (03) : 752 - 757
  • [10] Contribution of molecular analyses in diagnosing Marfan syndrome and type I fibrillinopathies:: an international study of 1009 probands
    Faivre, L.
    Collod-Beroud, G.
    Child, A.
    Callewaert, B.
    Loeys, B. L.
    Binquet, C.
    Gautier, E.
    Arbustini, E.
    Mayer, K.
    Arslan-Kirchner, M.
    Stheneur, C.
    Kiotsekoglou, A.
    Comeglio, P.
    Marziliano, N.
    Halliday, D.
    Beroud, C.
    Bonithon-Kopp, C.
    Claustres, M.
    Plauchu, H.
    Robinson, P. N.
    Ades, L.
    De Backer, J.
    Coucke, P.
    Francke, U.
    De Paepe, A.
    Boileau, C.
    Jondeau, G.
    [J]. JOURNAL OF MEDICAL GENETICS, 2008, 45 (06) : 384 - 390
1234