Karolinska Institutet
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Compound heterozygosity for two variants in BMP5 in human skeletal dysostosis with atrioventricular septal defect.

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posted on 2025-01-08, 13:53 authored by Pernille Axél Gregersen, Anna Hammarsjö, Lise Graversen, Nis Brix, Hillevi Lindelöf, Uffe Birk Jensen, Stense Farholt, Sune Rubak, Jesper Bjerre, Serena G Piticchio, Thorkild Terkelsen, Gen Nishimura, Michel Bach Hellfritzsch, Giedre GrigelionieneGiedre Grigelioniene
The growth and development of the skeleton is regulated by bone morphogenetic proteins of which several are linked to genetic skeletal disorders. So far, no human skeletal malformations have been associated with variants in BMP5. Here, we report a patient with biallelic loss of function variants in BMP5 and a syndromic phenotype including skeletal dysostosis, dysmorphic features, hypermobility, laryngo-tracheo-bronchomalacia and atrioventricular septal defect. We discuss the phenotype in relation to the known tissue-specific expression of Bmp5 and similar morphological abnormalities previously reported in experimental animal models. Our findings suggest a new association between BMP5 variants and a range of developmental anomalies, involving ears, heart and skeleton, thereby increasing understanding of BMP5's role in human development.

History

File version

  • Published

Publication status

Published

Sub type

Case Reports

Journal

Clin Genet

ISSN

0009-9163

eISSN

1399-0004

Volume

107

Issue

1

Pagination

78-82

Language

  • eng

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