Journal article

The molecular basis of X-linked spondyloepiphyseal dysplasia tarda

AK Gedeon, GE Tiller, M Le Merrer, L Tranebjaerg, D Chitayat, S Robertson, IA Glass, R Savarirayan, WG Cole, DL Rimoin, BG Kousseff, B Zabel, A Munnich, J Gecz, JC Mulley

American Journal of Human Genetics | UNIV CHICAGO PRESS | Published : 2001

Abstract

The X-linked form of spondyloepiphyseal dysplasia tarda (SEDL), a radiologically distinct skeletal dysplasia affecting the vertebrae and epiphyses, is caused by mutations in the SEDL gene. To characterize the molecular basis for SEDL, we have identified the spectrum of SEDL mutations in 30 of 36 unrelated cases of X-linked SEDL ascertained from different ethnic populations. Twenty-one different disease-associated mutations now have been identified throughout the SEDL gene. These include nonsense mutations in exons 4 and 5, missense mutations in exons 4 and 6, small (2-7 bp) and large (>1 kb) deletions, insertions, and putative splicing errors, with one splicing error due to a complex deletio..

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University of Melbourne Researchers