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. 2015 Nov;116(3):215-20.
doi: 10.1016/j.ymgme.2015.09.010. Epub 2015 Sep 30.

Molecular diagnosis of hypophosphatasia and differential diagnosis by targeted Next Generation Sequencing

Agnès Taillandier  1 Christelle Domingues  2 Clémence De Cazanove  3 Valérie Porquet-Bordes  4 Sophie Monnot  5 Tina Kiffer-Moreira  6 Agnès Rothenbuhler  7 Pascal Guggenbuhl  8 Catherine Cormier  9 Geneviève Baujat  10 Françoise Debiais  11 Yline Capri  12 Martine Cohen-Solal  13 Philippe Parent  14 Jean Chiesa  15 Anne Dieux  16 Florence Petit  17 Joelle Roume  18 Monica Isnard  19 Valérie Cormier-Daire  20 Agnès Linglart  21 José Luis Millán  22 Jean-Pierre Salles  23 Christine Muti  24 Brigitte Simon-Bouy  25 Etienne Mornet  26
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Molecular diagnosis of hypophosphatasia and differential diagnosis by targeted Next Generation Sequencing

Agnès Taillandier et al. Mol Genet Metab. 2015 Nov.

Abstract

Hypophosphatasia (HPP) is a rare inherited skeletal dysplasia due to loss of function mutations in the ALPL gene. The disease is subject to an extremely high clinical heterogeneity ranging from a perinatal lethal form to odontohypophosphatasia affecting only teeth. Up to now genetic diagnosis of HPP is performed by sequencing the ALPL gene by Sanger methodology. Osteogenesis imperfecta (OI) and campomelic dysplasia (CD) are the main differential diagnoses of severe HPP, so that in case of negative result for ALPL mutations, OI and CD genes had often to be analyzed, lengthening the time before diagnosis. We report here our 18-month experience in testing 46 patients for HPP and differential diagnosis by targeted NGS and show that this strategy is efficient and useful. We used an array including ALPL gene, genes of differential diagnosis COL1A1 and COL1A2 that represent 90% of OI cases, SOX9, responsible for CD, and 8 potentially modifier genes of HPP. Seventeen patients were found to carry a mutation in one of these genes. Among them, only 10 out of 15 cases referred for HPP carried a mutation in ALPL and 5 carried a mutation in COL1A1 or COL1A2. Interestingly, three of these patients were adults with fractures and/or low BMD. Our results indicate that HPP and OI may be easily misdiagnosed in the prenatal stage but also in adults with mild symptoms for these diseases.

Keywords: Differential diagnosis; Hypophosphatasia; NGS; Osteogenesis imperfecta.

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References

    1. Mornet E. Hypophosphatasia Best Pract Res Clin Rheumatol. 2008;22:113–127. - PubMed
    1. Whyte M. Hypophosphatasia. Elsevier (Academic Press); San Diego, CA: 2013.
    1. Moore CA, Curry CJ, Henthorn PS, Smith JA, Smith JC, O'Lague P, Coburn SP, Weaver DD, Whyte MP. Mild autosomal dominant hypophosphatasia: in utero presentation in two families. Am J Med Genet. 1999;86:410–415. - PubMed
    1. Pauli RM, Modaff P, Sipes SL, Whyte MP. Mild hypophosphatasia mimicking severe osteogenesis imperfecta in utero: bent but not broken. Am J Med Genet. 1999;86:434–438. - PubMed
    1. Wenkert D, McAlister WH, Coburn SP, Zerega JA, Ryan LM, Ericson KL, Hersh JH, Mumm S, Whyte MP. Hypophosphatasia: nonlethal disease despite skeletal presentation in utero (17 new cases and literature review) J Bone Miner Res. 2011;26:2389–2398. - PubMed

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