Your search keyword '"Jan Murken"' showing total 2 results

1. A gene (PEX) with homologies to endopeptidases is mutated in patients with X–linked hypophosphatemic rickets

Author

A.-M. Poustka, Ewa Pronicka, J. L. H. O'Riordan, Tina C. Summerfield, Klaus Mohnike, Thomas Meitinger, Michael J. Econs, J. Goulding, Tim M. Strom, Teresa Nesbitt, Steffen Hennig, Hans Lehrach, Marc K. Drezner, C. Oudet, André Hanauer, Jan Murken, Andrew P. Read, P. de Jong, Richard Reinhardt, Ewa Popowska, Bettina Lorenz, Peter S. N. Rowe, Bernhard Korn, Alfons Meindl, B. Cagnoli, Solange Pannetier, Kay E. Davies, Fiona Francis, and Roger Mountford

Subjects

Familial Hypophosphatemic Rickets, Genetics, Candidate gene, Hypophosphatemic Rickets, Positional cloning, PHEX, Autosomal dominant hypophosphatemic rickets, medicine, Biology, Renal phosphate excretion, medicine.disease, X-linked hypophosphatemia

Abstract

X–linked hypophosphatemic rickets (HYP) is a dominant disorder characterised by impaired phosphate uptake in the kidney, which is likely to be caused by abnormal regulation of sodium phosphate cotransport in the proximal tubules. By positional cloning, we have isolated a candidate gene from the HYP region in Xp22.1. This gene exhibits homology to a family of endopeptidase genes, members of which are involved in the degradation or activation of a variety of peptide hormones. This gene (which we have called PEX) is composed of multiple exons which span at least five cosmids. Intragenic non–overlapping deletions from four different families and three mutations (two splice sites and one frameshift) have been detected in HYP patients, which suggest that the PEX gene is involved in the HYP disorder.

Published

1995

2. Molecular modelling of the Norrie disease protein predicts a cystine knot growth factor tertiary structure

Author

Burkhart Rost, Thomas Meitinger, Alfons Meindl, Peer Bork, Jan Murken, Martina Haasemann, and Chris Sander

Subjects

Genetics, Models, Molecular, X Chromosome, Growth factor, medicine.medical_treatment, Cystine knot, Molecular Sequence Data, Biology, Deafness, medicine.disease, Blindness, Protein tertiary structure, Protein Structure, Tertiary, Intellectual Disability, von Willebrand Factor, medicine, Extracellular, Humans, Norrie disease, Amino Acid Sequence, Peptide sequence, Gene, Sex Chromosome Aberrations, Transforming growth factor

Abstract

The X-lined gene for Norrie disease, which is characterized by blindness, deafness and mental retardation has been cloned recently. This gene has been thought to code for a putative extracellular factor; its predicted amino acid sequence is homologous to the C-terminal domain of diverse extracellular proteins. Sequence pattern searches and three-dimensional modelling now suggest that the Norrie disease protein (NDP) has a tertiary structure similar to that of transforming growth factor beta (TGF beta). Our model identifies NDP as a member of an emerging family of growth factors containing a cystine knot motif, with direct implications for the physiological role of NDP. The model also sheds light on sequence related domains such as the C-terminal domain of mucins and of von Willebrand factor.

Published

1993