The gene for X-linked hypophosphataemic rickets maps to a 200–300 kb region in Xp22.1, and is located on a single YAC containing a putative vitamin D response element (VDRE)

Peter Rowe(North Middlesex Hospital), K E Davies(University of Oxford), Hans Lehrach(Max Planck Institute for Molecular Genetics), Tina C. Summerfield(North Middlesex Hospital), R. Mountford(University of Liverpool), Fiona Francis(Inserm), O. Oudet(Centre National de la Recherche Scientifique), J. Weissenbach, André Hanauer(Institut de génétique et de biologie moléculaire et cellulaire), M. K. Drezner(Duke Medical Center), W.D. Fraser(University of Liverpool), J. L. H. O’Riordan(North Middlesex Hospital), Michael J. Econs(Indiana University Bloomington), Andrew Read(University of Manchester), J.N. Goulding(North Middlesex Hospital)
Human Genetics
March 1, 1996
10.1007/bf02185769
Cited by 57

Related Papers

A global reference for human genetic variation
|Nature|2015|19.9k
A gene (PEX) with homologies to endopeptidases is mutated in patients with X–linked hypophosphatemic rickets
|Nature Genetics|1995|1.1k
A complete genomic screen for multiple sclerosis underscores a role for the major histocompatability complex
|Nature Genetics|1996|654
A homozygous missense mutation in human KLOTHO causes severe tumoral calcinosis
|Journal of Clinical Investigation|2007|476
Molecular dissection of colorectal cancer in pre-clinical models identifies biomarkers predicting sensitivity to EGFR inhibitors
|Nature Communications|2017|348