Paediatrics (RCH) - Research Publications

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Start date: 2000 × Author: Bagheri-Fam, Stefan ×

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    Genome-Wide ENU Mutagenesis in Combination with High Density SNP Analysis and Exome Sequencing Provides Rapid Identification of Novel Mouse Models of Developmental Disease
    Caruana, G ; Farlie, PG ; Hart, AH ; Bagheri-Fam, S ; Wallace, MJ ; Dobbie, MS ; Gordon, CT ; Miller, KA ; Whittle, B ; Abud, HE ; Arkell, RM ; Cole, TJ ; Harley, VR ; Smyth, IM ; Bertram, JF ; Veitia, RA (PUBLIC LIBRARY SCIENCE, 2013-03-01)
    BACKGROUND: Mice harbouring gene mutations that cause phenotypic abnormalities during organogenesis are invaluable tools for linking gene function to normal development and human disorders. To generate mouse models harbouring novel alleles that are involved in organogenesis we conducted a phenotype-driven, genome-wide mutagenesis screen in mice using the mutagen N-ethyl-N-nitrosourea (ENU). METHODOLOGY/PRINCIPAL FINDINGS: ENU was injected into male C57BL/6 mice and the mutations transmitted through the germ-line. ENU-induced mutations were bred to homozygosity and G3 embryos screened at embryonic day (E) 13.5 and E18.5 for abnormalities in limb and craniofacial structures, skin, blood, vasculature, lungs, gut, kidneys, ureters and gonads. From 52 pedigrees screened 15 were detected with anomalies in one or more of the structures/organs screened. Using single nucleotide polymorphism (SNP)-based linkage analysis in conjunction with candidate gene or next-generation sequencing (NGS) we identified novel recessive alleles for Fras1, Ift140 and Lig1. CONCLUSIONS/SIGNIFICANCE: In this study we have generated mouse models in which the anomalies closely mimic those seen in human disorders. The association between novel mutant alleles and phenotypes will lead to a better understanding of gene function in normal development and establish how their dysfunction causes human anomalies and disease.
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    The gene encoding the ketogenic enzyme HMGCS2 displays a unique expression during gonad development in mice.
    Bagheri-Fam, S ; Chen, H ; Wilson, S ; Ayers, K ; Hughes, J ; Sloan-Bena, F ; Calvel, P ; Robevska, G ; Puisac, B ; Kusz-Zamelczyk, K ; Gimelli, S ; Spik, A ; Jaruzelska, J ; Warenik-Szymankiewicz, A ; Faradz, S ; Nef, S ; Pié, J ; Thomas, P ; Sinclair, A ; Wilhelm, D ; Yenugu, S (Public Library Science, 2020)
    Disorders/differences of sex development (DSD) cause profound psychological and reproductive consequences for the affected individuals, however, most are still unexplained at the molecular level. Here, we present a novel gene, 3-hydroxy-3-methylglutaryl coenzyme A synthase 2 (HMGCS2), encoding a metabolic enzyme in the liver important for energy production from fatty acids, that shows an unusual expression pattern in developing fetal mouse gonads. Shortly after gonadal sex determination it is up-regulated in the developing testes following a very similar spatial and temporal pattern as the male-determining gene Sry in Sertoli cells before switching to ovarian enriched expression. To test if Hmgcs2 is important for gonad development in mammals, we pursued two lines of investigations. Firstly, we generated Hmgcs2-null mice using CRISPR/Cas9 and found that these mice had gonads that developed normally even on a sensitized background. Secondly, we screened 46,XY DSD patients with gonadal dysgenesis and identified two unrelated patients with a deletion and a deleterious missense variant in HMGCS2 respectively. However, both variants were heterozygous, suggesting that HMGCS2 might not be the causative gene. Analysis of a larger number of patients in the future might shed more light into the possible association of HMGCS2 with human gonadal development.