Heterozygous germline mutations in the p53 homolog p63 are the cause of EEC syndrome

J Celli; P Duijf; BCJ Hamel; M Bamshad; B Kramer; APT Smits; R Newbury-Ecob; RCM Hennekam; G Van Buggenhout; B van Haeringen; CG Woods; AJ van Essen; R de Waal; G Vriend; DA Haber; A Yang; F McKeon; HG Brunner; H van Bokhoven

Heterozygous germline mutations in the p53 homolog p63 are the cause of EEC syndrome

J Celli, P Duijf, BCJ Hamel, M Bamshad, B Kramer, APT Smits, R Newbury-Ecob, RCM Hennekam, G Van Buggenhout, B van Haeringen, CG Woods, AJ van Essen, R de Waal, G Vriend, DA Haber, A Yang, F McKeon, HG Brunner, H van Bokhoven^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

EEC syndrome is an autosomal dominant disorder characterized by ectrodactyly, ectodermal dysplasia, and facial clefts. We have mapped the genetic defect in several EEC syndrome families to a region of chromosome 3q27 previously implicated in the EEC-like disorder, limb mammary syndrome (LMS). Analysis of the p63 gene, a homolog of p53 located in the critical LMS/EEC interval, revealed heterozygous mutations in nine unrelated EEC families. Eight mutations result in amino acid substitutions that are predicted to abolish the DNA binding capacity of p63. The ninth is a frameshift mutation that affects the p63 alpha, but not p63 beta and p63 gamma isotypes. Transactivation studies with these mutant p63 isotypes provide a molecular explanation for the dominant character of p63 mutations in EEC syndrome.

Original language	English
Pages (from-to)	143-153
Number of pages	11
Journal	Cell
Volume	99
Issue number	2
Publication status	Published - 15-Oct-1999

Keywords

SPLIT FOOT LOCUS
LIMB DEVELOPMENT
GENE
PROTEIN
EXPRESSION
SEQUENCE
DATABASE
COMPLEX
DEFECTS
MODEL

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Celli, J., Duijf, P., Hamel, BCJ., Bamshad, M., Kramer, B., Smits, APT., Newbury-Ecob, R., Hennekam, RCM., Van Buggenhout, G., van Haeringen, B., Woods, CG., van Essen, AJ., de Waal, R., Vriend, G., Haber, DA., Yang, A., McKeon, F., Brunner, HG., & van Bokhoven, H. (1999). Heterozygous germline mutations in the p53 homolog p63 are the cause of EEC syndrome. Cell, 99(2), 143-153.

@article{31caaf5fa9b14c4cb2ea8287527f0112,

title = "Heterozygous germline mutations in the p53 homolog p63 are the cause of EEC syndrome",

abstract = "EEC syndrome is an autosomal dominant disorder characterized by ectrodactyly, ectodermal dysplasia, and facial clefts. We have mapped the genetic defect in several EEC syndrome families to a region of chromosome 3q27 previously implicated in the EEC-like disorder, limb mammary syndrome (LMS). Analysis of the p63 gene, a homolog of p53 located in the critical LMS/EEC interval, revealed heterozygous mutations in nine unrelated EEC families. Eight mutations result in amino acid substitutions that are predicted to abolish the DNA binding capacity of p63. The ninth is a frameshift mutation that affects the p63 alpha, but not p63 beta and p63 gamma isotypes. Transactivation studies with these mutant p63 isotypes provide a molecular explanation for the dominant character of p63 mutations in EEC syndrome.",

keywords = "SPLIT FOOT LOCUS, LIMB DEVELOPMENT, GENE, PROTEIN, EXPRESSION, SEQUENCE, DATABASE, COMPLEX, DEFECTS, MODEL",

author = "J Celli and P Duijf and BCJ Hamel and M Bamshad and B Kramer and APT Smits and R Newbury-Ecob and RCM Hennekam and {Van Buggenhout}, G and {van Haeringen}, B and CG Woods and {van Essen}, AJ and {de Waal}, R and G Vriend and DA Haber and A Yang and F McKeon and HG Brunner and {van Bokhoven}, H",

year = "1999",

month = oct,

day = "15",

language = "English",

volume = "99",

pages = "143--153",

journal = "Cell",

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}

Celli, J, Duijf, P, Hamel, BCJ, Bamshad, M, Kramer, B, Smits, APT, Newbury-Ecob, R, Hennekam, RCM, Van Buggenhout, G, van Haeringen, B, Woods, CG, van Essen, AJ, de Waal, R, Vriend, G, Haber, DA, Yang, A, McKeon, F, Brunner, HG & van Bokhoven, H 1999, 'Heterozygous germline mutations in the p53 homolog p63 are the cause of EEC syndrome', Cell, vol. 99, no. 2, pp. 143-153.

TY - JOUR

T1 - Heterozygous germline mutations in the p53 homolog p63 are the cause of EEC syndrome

AU - Celli, J

AU - Duijf, P

AU - Hamel, BCJ

AU - Bamshad, M

AU - Kramer, B

AU - Smits, APT

AU - Newbury-Ecob, R

AU - Hennekam, RCM

AU - Van Buggenhout, G

AU - van Haeringen, B

AU - Woods, CG

AU - van Essen, AJ

AU - de Waal, R

AU - Vriend, G

AU - Haber, DA

AU - Yang, A

AU - McKeon, F

AU - Brunner, HG

AU - van Bokhoven, H

PY - 1999/10/15

Y1 - 1999/10/15

N2 - EEC syndrome is an autosomal dominant disorder characterized by ectrodactyly, ectodermal dysplasia, and facial clefts. We have mapped the genetic defect in several EEC syndrome families to a region of chromosome 3q27 previously implicated in the EEC-like disorder, limb mammary syndrome (LMS). Analysis of the p63 gene, a homolog of p53 located in the critical LMS/EEC interval, revealed heterozygous mutations in nine unrelated EEC families. Eight mutations result in amino acid substitutions that are predicted to abolish the DNA binding capacity of p63. The ninth is a frameshift mutation that affects the p63 alpha, but not p63 beta and p63 gamma isotypes. Transactivation studies with these mutant p63 isotypes provide a molecular explanation for the dominant character of p63 mutations in EEC syndrome.

AB - EEC syndrome is an autosomal dominant disorder characterized by ectrodactyly, ectodermal dysplasia, and facial clefts. We have mapped the genetic defect in several EEC syndrome families to a region of chromosome 3q27 previously implicated in the EEC-like disorder, limb mammary syndrome (LMS). Analysis of the p63 gene, a homolog of p53 located in the critical LMS/EEC interval, revealed heterozygous mutations in nine unrelated EEC families. Eight mutations result in amino acid substitutions that are predicted to abolish the DNA binding capacity of p63. The ninth is a frameshift mutation that affects the p63 alpha, but not p63 beta and p63 gamma isotypes. Transactivation studies with these mutant p63 isotypes provide a molecular explanation for the dominant character of p63 mutations in EEC syndrome.

KW - SPLIT FOOT LOCUS

KW - LIMB DEVELOPMENT

KW - GENE

KW - PROTEIN

KW - EXPRESSION

KW - SEQUENCE

KW - DATABASE

KW - COMPLEX

KW - DEFECTS

KW - MODEL

M3 - Article

SN - 0092-8674

VL - 99

SP - 143

EP - 153

JO - Cell

JF - Cell

IS - 2

ER -

Heterozygous germline mutations in the p53 homolog p63 are the cause of EEC syndrome

Abstract

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