Pseudodiastrophic dysplasia expands the known phenotypic spectrum of defects in proteoglycan biosynthesis.
Alicia B ByrneShuji MizumotoPeer ArtsPatrick YapJinghua FengAndreas W SchreiberMilena BabicSarah L King-SmithChristopher P BarnettLynette MooreKazuyuki SugaharaHatice Mutlu-AlbayrakGen NishimuraJan E LiebeltShuhei YamadaRavi SavarirayanHamish S ScottPublished in: Journal of medical genetics (2020)
For the families described in this study, the PDD phenotype was caused by mutations in the known skeletal dysplasia genes B3GAT3 and CANT1, demonstrating the advantage of genomic analyses in delineating the molecular diagnosis of skeletal dysplasias. This finding expands the phenotypic spectrum of B3GAT3-related and CANT1-related skeletal dysplasias to include PDD and highlights the significant phenotypic overlap of conditions within the proteoglycan biosynthesis pathway.
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