Rural Clinical School - Research Publications

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Author: Hutson, John × Author: Sinclair, Andrew × End date: 2019 × Start date: 2010 ×

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    Copy Number Variation in Patients with Disorders of Sex Development Due to 46,XY Gonadal Dysgenesis
    White, S ; Ohnesorg, T ; Notini, A ; Roeszler, K ; Hewitt, J ; Daggag, H ; Smith, C ; Turbitt, E ; Gustin, S ; van den Bergen, J ; Miles, D ; Western, P ; Arboleda, V ; Schumacher, V ; Gordon, L ; Bell, K ; Bengtsson, H ; Speed, T ; Hutson, J ; Warne, G ; Harley, V ; Koopman, P ; Vilain, E ; Sinclair, A ; Orban, L (PUBLIC LIBRARY SCIENCE, 2011-03-07)
    Disorders of sex development (DSD), ranging in severity from mild genital abnormalities to complete sex reversal, represent a major concern for patients and their families. DSD are often due to disruption of the genetic programs that regulate gonad development. Although some genes have been identified in these developmental pathways, the causative mutations have not been identified in more than 50% 46,XY DSD cases. We used the Affymetrix Genome-Wide Human SNP Array 6.0 to analyse copy number variation in 23 individuals with unexplained 46,XY DSD due to gonadal dysgenesis (GD). Here we describe three discrete changes in copy number that are the likely cause of the GD. Firstly, we identified a large duplication on the X chromosome that included DAX1 (NR0B1). Secondly, we identified a rearrangement that appears to affect a novel gonad-specific regulatory region in a known testis gene, SOX9. Surprisingly this patient lacked any signs of campomelic dysplasia, suggesting that the deletion affected expression of SOX9 only in the gonad. Functional analysis of potential SRY binding sites within this deleted region identified five putative enhancers, suggesting that sequences additional to the known SRY-binding TES enhancer influence human testis-specific SOX9 expression. Thirdly, we identified a small deletion immediately downstream of GATA4, supporting a role for GATA4 in gonad development in humans. These CNV analyses give new insights into the pathways involved in human gonad development and dysfunction, and suggest that rearrangements of non-coding sequences disturbing gene regulation may account for significant proportion of DSD cases.
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    Disorders of sex development: insights from targeted gene sequencing of a large international patient cohort
    Eggers, S ; Sadedin, S ; van den Bergen, JA ; Robevska, G ; Ohnesorg, T ; Hewitt, J ; Lambeth, L ; Bouty, A ; Knarston, IM ; Tiong, YT ; Cameron, F ; Werther, G ; Hutson, J ; O'Connell, M ; Grover, SR ; Heloury, Y ; Zacharin, M ; Bergman, P ; Kimber, C ; Brown, J ; Webb, N ; Hunter, MF ; Srinivasan, S ; Titmuss, A ; Verge, CF ; Mowat, D ; Smith, G ; Smith, J ; Ewans, L ; Shalhoub, C ; Crock, P ; Cowell, C ; Leong, GM ; Ono, M ; Lafferty, AR ; Huynh, T ; Visser, U ; Choong, CS ; McKenzie, F ; Pachter, N ; Thompson, EM ; Couper, J ; Baxendale, A ; Gecz, J ; Wheeler, BJ ; Jefferies, C ; MacKenzie, K ; Hofman, P ; Carter, P ; King, RI ; Krausz, C ; van Ravenswaaij-Arts, CMA ; Looijenga, L ; Drop, S ; Riedl, S ; Cools, M ; Dawson, A ; Juniarto, AZ ; Khadilkar, V ; Khadilkar, A ; Bhatia, V ; Vu, CD ; Atta, I ; Raza, J ; Nguyen, TDC ; Tran, KH ; Harley, V ; Koopman, P ; Warne, G ; Faradz, S ; Oshlack, A ; Ayers, KL ; Sinclair, AH (BIOMED CENTRAL LTD, 2016-11-29)
    BACKGROUND: Disorders of sex development (DSD) are congenital conditions in which chromosomal, gonadal, or phenotypic sex is atypical. Clinical management of DSD is often difficult and currently only 13% of patients receive an accurate clinical genetic diagnosis. To address this we have developed a massively parallel sequencing targeted DSD gene panel which allows us to sequence all 64 known diagnostic DSD genes and candidate genes simultaneously. RESULTS: We analyzed DNA from the largest reported international cohort of patients with DSD (278 patients with 46,XY DSD and 48 with 46,XX DSD). Our targeted gene panel compares favorably with other sequencing platforms. We found a total of 28 diagnostic genes that are implicated in DSD, highlighting the genetic spectrum of this disorder. Sequencing revealed 93 previously unreported DSD gene variants. Overall, we identified a likely genetic diagnosis in 43% of patients with 46,XY DSD. In patients with 46,XY disorders of androgen synthesis and action the genetic diagnosis rate reached 60%. Surprisingly, little difference in diagnostic rate was observed between singletons and trios. In many cases our findings are informative as to the likely cause of the DSD, which will facilitate clinical management. CONCLUSIONS: Our massively parallel sequencing targeted DSD gene panel represents an economical means of improving the genetic diagnostic capability for patients affected by DSD. Implementation of this panel in a large cohort of patients has expanded our understanding of the underlying genetic etiology of DSD. The inclusion of research candidate genes also provides an invaluable resource for future identification of novel genes.
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    Human sex reversal is caused by duplication or deletion of core enhancers upstream of SOX9
    Croft, B ; Ohnesorg, T ; Hewitt, J ; Bowles, J ; Quinn, A ; Tan, J ; Corbin, V ; Pelosi, E ; van den Bergen, J ; Sreenivasan, R ; Knarston, I ; Robevska, G ; Dung, CV ; Hutson, J ; Harley, V ; Ayers, K ; Koopman, P ; Sinclair, A (NATURE PUBLISHING GROUP, 2018-12-14)
    Disorders of sex development (DSDs) are conditions affecting development of the gonads or genitalia. Variants in two key genes, SRY and its target SOX9, are an established cause of 46,XY DSD, but the genetic basis of many DSDs remains unknown. SRY-mediated SOX9 upregulation in the early gonad is crucial for testis development, yet the regulatory elements underlying this have not been identified in humans. Here, we identified four DSD patients with overlapping duplications or deletions upstream of SOX9. Bioinformatic analysis identified three putative enhancers for SOX9 that responded to different combinations of testis-specific regulators. All three enhancers showed synergistic activity and together drive SOX9 in the testis. This is the first study to identify SOX9 enhancers that, when duplicated or deleted, result in 46,XX or 46,XY sex reversal, respectively. These enhancers provide a hitherto missing link by which SRY activates SOX9 in humans, and establish SOX9 enhancer mutations as a significant cause of DSD.