Exclusion of the MSX1 homeobox gene as the gene for the Ellis van Creveld syndrome in the Amish

Susan E. Ide; Rosa Isela Ortiz De Luna; Clair A. Francomano; Mihael H. Polymeropoulos

doi:10.1007/s004390050261

Exclusion of the MSX1 homeobox gene as the gene for the Ellis van Creveld syndrome in the Amish

Susan E. Ide, Rosa Isela Ortiz De Luna, Clair A. Francomano, Mihael H. Polymeropoulos

School of Medicine

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

12 Scopus citations

Abstract

Ellis van Creveld syndrome (EVC) is an autosomal recessive disorder which has previously been mapped to human chromosome 4p16.1. This disorder is characterized by disproportionate dwarfism, polydactyly, cleft palate, natal teeth, and congenital heart disease. The MSX1 homeobox gene also maps to the 4p16.1 region. Msx gene transcripts in the mouse embryo are known to be involved in pattern formation of the developing limb bud and craniofacial bones. Thus, on the basis of both map location and known gene function, MSX1 was an excellent candidate as the causative gene for EVC. Nonetheless, direct DNA sequencing of both exons of the MSX1 gene in five affected individuals segregating with the EVC phenotype, as well as those of two obligate carriers, revealed no mutations in the coding region of the gene.

Original language	English (US)
Pages (from-to)	572-575
Number of pages	4
Journal	Human genetics
Volume	98
Issue number	5
DOIs	https://doi.org/10.1007/s004390050261
State	Published - Dec 5 1996

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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title = "Exclusion of the MSX1 homeobox gene as the gene for the Ellis van Creveld syndrome in the Amish",

abstract = "Ellis van Creveld syndrome (EVC) is an autosomal recessive disorder which has previously been mapped to human chromosome 4p16.1. This disorder is characterized by disproportionate dwarfism, polydactyly, cleft palate, natal teeth, and congenital heart disease. The MSX1 homeobox gene also maps to the 4p16.1 region. Msx gene transcripts in the mouse embryo are known to be involved in pattern formation of the developing limb bud and craniofacial bones. Thus, on the basis of both map location and known gene function, MSX1 was an excellent candidate as the causative gene for EVC. Nonetheless, direct DNA sequencing of both exons of the MSX1 gene in five affected individuals segregating with the EVC phenotype, as well as those of two obligate carriers, revealed no mutations in the coding region of the gene.",

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T1 - Exclusion of the MSX1 homeobox gene as the gene for the Ellis van Creveld syndrome in the Amish

AU - Ide, Susan E.

AU - De Luna, Rosa Isela Ortiz

AU - Francomano, Clair A.

AU - Polymeropoulos, Mihael H.

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N2 - Ellis van Creveld syndrome (EVC) is an autosomal recessive disorder which has previously been mapped to human chromosome 4p16.1. This disorder is characterized by disproportionate dwarfism, polydactyly, cleft palate, natal teeth, and congenital heart disease. The MSX1 homeobox gene also maps to the 4p16.1 region. Msx gene transcripts in the mouse embryo are known to be involved in pattern formation of the developing limb bud and craniofacial bones. Thus, on the basis of both map location and known gene function, MSX1 was an excellent candidate as the causative gene for EVC. Nonetheless, direct DNA sequencing of both exons of the MSX1 gene in five affected individuals segregating with the EVC phenotype, as well as those of two obligate carriers, revealed no mutations in the coding region of the gene.

AB - Ellis van Creveld syndrome (EVC) is an autosomal recessive disorder which has previously been mapped to human chromosome 4p16.1. This disorder is characterized by disproportionate dwarfism, polydactyly, cleft palate, natal teeth, and congenital heart disease. The MSX1 homeobox gene also maps to the 4p16.1 region. Msx gene transcripts in the mouse embryo are known to be involved in pattern formation of the developing limb bud and craniofacial bones. Thus, on the basis of both map location and known gene function, MSX1 was an excellent candidate as the causative gene for EVC. Nonetheless, direct DNA sequencing of both exons of the MSX1 gene in five affected individuals segregating with the EVC phenotype, as well as those of two obligate carriers, revealed no mutations in the coding region of the gene.

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Exclusion of the MSX1 homeobox gene as the gene for the Ellis van Creveld syndrome in the Amish

Abstract

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