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Craniofacial dysmorphology in Down syndrome is caused by increased dosage of Dyrk1a and at least three other genes

Yushi Redhead, Dorota Gibbins, Eva Lana‐Elola, Sheona Watson-Scales, Lisa Dobson, Matthias Krause, Karen Liu, Elizabeth Fisher, Jeremy Green, Victor L. J. Tybulewicz

2023Development26 citationsDOIOpen Access PDF

Abstract

Down syndrome (DS), trisomy of human chromosome 21 (Hsa21), occurs in 1 in 800 live births and is the most common human aneuploidy. DS results in multiple phenotypes, including craniofacial dysmorphology, which is characterised by midfacial hypoplasia, brachycephaly and micrognathia. The genetic and developmental causes of this are poorly understood. Using morphometric analysis of the Dp1Tyb mouse model of DS and an associated mouse genetic mapping panel, we demonstrate that four Hsa21-orthologous regions of mouse chromosome 16 contain dosage-sensitive genes that cause the DS craniofacial phenotype, and identify one of these causative genes as Dyrk1a. We show that the earliest and most severe defects in Dp1Tyb skulls are in bones of neural crest (NC) origin, and that mineralisation of the Dp1Tyb skull base synchondroses is aberrant. Furthermore, we show that increased dosage of Dyrk1a results in decreased NC cell proliferation and a decrease in size and cellularity of the NC-derived frontal bone primordia. Thus, DS craniofacial dysmorphology is caused by an increased dosage of Dyrk1a and at least three other genes.

Topics & Concepts

BiologyCraniofacialTrisomyMicrocephalyDown syndromeGeneticsGene dosageDYRK1AChromosome 21HypoplasiaAneuploidyCraniofacial abnormalityPhenotypeCranial vaultNeural crestSkullGeneChromosomeAnatomyGene expressionDown syndrome and intellectual disability researchGenetics and Neurodevelopmental DisordersGenomics and Rare Diseases
Craniofacial dysmorphology in Down syndrome is caused by increased dosage of Dyrk1a and at least three other genes | Litcius