Mutations of the Imprinted CDKN1C Gene as a Cause of the Overgrowth Beckwith-Wiedemann Syndrome: Clinical Spectrum and Functional Characterization

被引：58

作者：

Brioude, Frederic ^{[1
,2
,3
]}

Netchine, Irene ^{[1
,2
,3
]}

Praz, Francoise ^{[1
,3
]}

Le Jule, Marilyne ^{[2
]}

Calmel, Claire ^{[3
]}

Lacombe, Didier ^{[4
,5
]}

Edery, Patrick ^{[6
,7
]}

Catala, Martin ^{[8
,9
,10
]}

Odent, Sylvie ^{[11
,12
]}

Isidor, Bertrand ^{[13
,14
]}

Lyonnet, Stanislas ^{[15
,16
]}

Sigaudy, Sabine ^{[17
]}

Leheup, Bruno ^{[18
,19
]}

Audebert-Bellanger, Severine ^{[20
]}

Burglen, Lydie ^{[21
,22
]}

Giuliano, Fabienne ^{[23
]}

Alessandri, Jean-Luc ^{[24
]}

Cormier-Daire, Valerie ^{[25
,26
]}

Laffargue, Fanny ^{[27
]}

Blesson, Sophie ^{[28
]}

Coupier, Isabelle ^{[29
]}

Lespinasse, James ^{[30
]}

Blanchet, Patricia ^{[31
]}

Boute, Odile ^{[32
]}

Baumann, Clarisse ^{[33
,34
]}

Polak, Michel ^{[35
,36
]}

Doray, Berenice ^{[37
]}

Verloes, Alain ^{[33
,34
]}

Viot, Geraldine ^{[38
]}

Le Bouc, Yves ^{[1
,2
,3
]}

Rossignol, Sylvie ^{[3
,37
]}

机构：

[1] Univ Paris 06, Sorbonne Univ, F-75005 Paris, France

[2] Hop Armand Trousseau, AP HP, Explorat Fonctionnelles Endocriniennes, F-75012 Paris, France

[3] Ctr Rech St Antoine, INSERM, UMR S 938, F-75012 Paris, France

[4] CHU Bordeaux, Serv Genet Med, Bordeaux, France

[5] Univ Bordeaux, Lab Malad Rares Genet & Metab MRGM, Bordeaux, France

[6] Hop Femme Mere Enfant, Serv Genet, Hospices Civils Lyon, Bron, France

[7] Ctr Res Neurosci Lyon, CNRS UMR UCBL 5292, INSERM 1028, Lyon, France

[8] Federat Neurol Grp Hosp Pitie Salpetrie, F-75651 Paris, France

[9] CNRS, Dev Biol Lab, UMR 7622, F-75252 Paris, France

[10] Univ Paris 06, F-75252 Paris, France

[11] CHU Rennes, Hop Sud, Serv Genet Clin, F-35203 Rennes, France

[12] Univ Rennes 1, Rennes, France

[13] CHU Nantes, Serv Genet, F-44035 Nantes 01, France

[14] INSERM, UMR S 957, Nantes, France

[15] Univ Paris 05, Sorbonne Paris Cite, INSERM, Inst Imagine,UMR 1163, Paris, France

[16] Hop Univ Necker Enfants Malades, AP HP, Dept Genet, Paris, France

[17] CHU Marseille, Hop Enfants La Timone, Serv Genet Med, Marseille, France

[18] CHU Nancy, Pole Enfants, Serv Med Infantile & Genet Clin, Ctr Reference Syndrome Malformatif & Anomalies De, Vandoeuvre Les Nancy, France

[19] Univ Lorraine, Fac Med, Unite INSERM U954, Vandoeuvre Les Nancy, France

[20] CHU Morvan, Serv Genet Med, Brest, France

[21] Hop Armand Trousseau, AP HP, Serv Genet, Ctr Reference Malformat & Malad Congenit Cervelet, F-75012 Paris, France

[22] INSERM, U1141, F-75019 Paris, France

[23] CHU Nice, Serv Genet Med, Hop Archet2, F-06202 Nice, France

[24] CHU La Reunion, CH Felix Guyon, Pole Femme Mere Enfant St Denis, La Reunion, France

[25] Hop Necker Enfants Malad, IMAGINE Inst, Paris, France

[26] Univ Paris 05, INSERM, UMR1163, Paris, France

[27] CHU Estaing, Serv Genet Med, Clermont Ferrand, France

[28] CHU Tours, Serv Genet, Tours, France

[29] CHU Arnaud Villeneuve, Serv Genet Med, Unite Oncogenet, Montpellier, France

[30] Ctr Hosp Chambery Hotel Dieu, UF Genet Chromos, Chambery, France

[31] CHU Arnaud Villeneuve, Serv Genet Med, Clin Genet Unit, Montpellier, France

[32] CHRU Lille, Serv Genet, F-59037 Lille, France

[33] Hop Robert Debre, AP HP, Dept Med Genet, F-75019 Paris, France

[34] INSERM, UMR 1141, Paris, France

[35] Hop Univ Necker Enfants Malades, AP HP, Endocrinol Gynecol Diabetol Pediatr, Paris, France

[36] Univ Paris 05, INSERM, IMAGINE Inst, U1016, Paris, France

[37] Hop Univ Strasbourg, Ctr Reference Anomalies Dev FECLAD, Serv Genet Med, Strasbourg, France

[38] Hop Port Royal, AP HP, Serv Genet, Paris, France

来源：

HUMAN MUTATION | 2015年 / 36卷 / 09期

关键词：

Beckwith-Wiedemann; imprinting; CDKN1C; cell cycle; overgrowth syndrome; COPY NUMBER VARIATIONS; PCNA-BINDING DOMAIN; SILVER-RUSSELL; P57(KIP2); INHIBITOR; PHENOTYPE; REGION; DIFFERENTIATION; POLYMORPHISMS;

D O I：

10.1002/humu.22824

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Beckwith-Wiedemann syndrome (BWS) is an imprinting disorder associating macroglossia, abdominal wall defects, visceromegaly, and a high risk of childhood tumor. Molecular anomalies are mostly epigenetic; however, mutations of CDKN1C are implicated in 8% of cases, including both sporadic and familial forms. We aimed to describe the phenotype of BWS patients with CDKN1C mutations and develop a functional test for CDKN1C mutations. For each propositus, we sequenced the three exons and intron-exon boundaries of CDKN1C in patients presenting a BWS phenotype, including abdominal wall defects, without 11p15 methylation defects. We developed a functional test based on flow cytometry. We identified 37 mutations in 38 pedigrees (50 patients and seven fetuses). Analysis of parental samples when available showed that all mutations tested but one was inherited from the mother. The four missense mutations led to a less severe phenotype (lower frequency of exomphalos) than the other 33 mutations. The following four tumors occurred: one neuroblastoma, one ganglioneuroblastoma, one melanoma, and one acute lymphoid leukemia. Cases of BWS caused by CDKN1C mutations are not rare. CDKN1C sequencing should be performed for BWS patients presenting with abdominal wall defects or cleft palate without 11p15 methylation defects or body asymmetry, or in familial cases of BWS. (C) 2015 Wiley Periodicals, Inc.

引用

页码：894 / 902

页数：9

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