BMC Medical Genetics (Jun 2009)

Mild forms of hypophosphatasia mostly result from dominant negative effect of severe alleles or from compound heterozygosity for severe and moderate alleles

  • Fauvert Delphine,
  • Brun-Heath Isabelle,
  • Lia-Baldini Anne-Sophie,
  • Bellazi Linda,
  • Taillandier Agnès,
  • Serre Jean-Louis,
  • de Mazancourt Philippe,
  • Mornet Etienne

DOI
https://doi.org/10.1186/1471-2350-10-51
Journal volume & issue
Vol. 10, no. 1
p. 51

Abstract

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Abstract Background Mild hypophosphatasia (HPP) phenotype may result from ALPL gene mutations exhibiting residual alkaline phosphatase activity or from severe heterozygous mutations exhibiting a dominant negative effect. In order to determine the cause of our failure to detect a second mutation by sequencing in patients with mild HPP and carrying on a single heterozygous mutation, we tested the possible dominant effect of 35 mutations carried by these patients. Methods We tested the mutations by site-directed mutagenesis. We also genotyped 8 exonic and intronic ALPL gene polymorphisms in the patients and in a control group in order to detect the possible existence of a recurrent intronic mild mutation. Results We found that most of the tested mutations exhibit a dominant negative effect that may account for the mild HPP phenotype, and that for at least some of the patients, a second mutation in linkage disequilibrium with a particular haplotype could not be ruled out. Conclusion Mild HPP results in part from compound heterozygosity for severe and moderate mutations, but also in a large part from heterozygous mutations with a dominant negative effect.