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  1. Article: Analysis of genetic variability in Turner syndrome linked to long-term clinical features.

    Suntharalingham, Jenifer P / Ishida, Miho / Cameron-Pimblett, Antoinette / McGlacken-Byrne, Sinead M / Buonocore, Federica / Del Valle, Ignacio / Madhan, Gaganjit Kaur / Brooks, Tony / Conway, Gerard S / Achermann, John C

    Frontiers in endocrinology

    2023  Volume 14, Page(s) 1227164

    Abstract: Background: Women with Turner syndrome (TS) (45,X and related karyotypes) have an increased prevalence of conditions such as diabetes mellitus, obesity, hypothyroidism, autoimmunity, hypertension, and congenital cardiovascular anomalies (CCA). Whilst ... ...

    Abstract Background: Women with Turner syndrome (TS) (45,X and related karyotypes) have an increased prevalence of conditions such as diabetes mellitus, obesity, hypothyroidism, autoimmunity, hypertension, and congenital cardiovascular anomalies (CCA). Whilst the risk of developing these co-morbidities may be partly related to haploinsufficiency of key genes on the X chromosome, other mechanisms may be involved. Improving our understanding of underlying processes is important to develop personalized approaches to management.
    Objective: We investigated whether: 1) global genetic variability differs in women with TS, which might contribute to co-morbidities; 2) common variants in X genes - on the background of haploinsufficiency - are associated with phenotype (a "two-hit" hypothesis); 3) the previously reported association of autosomal
    Methods: Whole exome sequencing was undertaken in leukocyte DNA from 134 adult women with TS and compared to 46,XX controls (n=23), 46,XX women with primary ovarian insufficiency (n=101), and 46,XY controls (n=11). 1) Variability in autosomal and X chromosome genes was analyzed for all individuals; 2) the relation between common X chromosome variants and the long-term phenotypes listed above was investigated in a subgroup of women with monosomy X; 3)
    Results: Standard filtering identified 6,457,085 autosomal variants and 126,335 X chromosome variants for the entire cohort, whereas a somatic variant pipeline identified 16,223 autosomal and 477 X chromosome changes. 1) Overall exome variability of autosomal genes was similar in women with TS and control/comparison groups, whereas X chromosome variants were proportionate to the complement of X chromosome material; 2) when adjusted for multiple comparisons, no X chromosome gene/variants were strongly enriched in monosomy X women with key phenotypes compared to monosomy X women without these conditions, although several variants of interest emerged; 3) an association between
    Conclusions: Women with TS do not have an excess of genetic variability in exome analysis. No obvious X-chromosome variants driving phenotype were found, but several possible genes/variants of interest emerged. A reported association between autosomal
    MeSH term(s) Adult ; Humans ; Female ; Turner Syndrome/genetics ; Diabetes Mellitus ; Karyotyping ; Autoimmunity ; Phenotype
    Language English
    Publishing date 2023-09-20
    Publishing country Switzerland
    Document type Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 2592084-4
    ISSN 1664-2392
    ISSN 1664-2392
    DOI 10.3389/fendo.2023.1227164
    Database MEDical Literature Analysis and Retrieval System OnLINE

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  2. Article ; Online: Variants of IL6, IL10, FCN2, RNASE3, IL12B and IL17B loci are associated with Schistosoma mansoni worm burden in the Albert Nile region of Uganda.

    Nyangiri, Oscar Asanya / Mulindwa, Julius / Namulondo, Joyce / Kitibwa, Anna / Nassuuna, Jacent / Elliott, Alison / Kimuda, Magambo Phillip / Boobo, Alex / Nerima, Barbara / Adriko, Moses / Dunton, Nathan J / Madhan, Gaganjit Kaur / Kristiansen, Mark / Casacuberta-Partal, Miriam / Noyes, Harry / Matovu, Enock

    PLoS neglected tropical diseases

    2023  Volume 17, Issue 11, Page(s) e0011796

    Abstract: Background: Individuals genetically susceptible to high schistosomiasis worm burden may contribute disproportionately to transmission and could be prioritized for control. Identifying genes involved may guide development of therapy.: Methodology/ ... ...

    Abstract Background: Individuals genetically susceptible to high schistosomiasis worm burden may contribute disproportionately to transmission and could be prioritized for control. Identifying genes involved may guide development of therapy.
    Methodology/principal findings: A cohort of 606 children aged 10-15 years were recruited in the Albert Nile region of Uganda and assessed for Schistosoma mansoni worm burden using the Up-Converting Particle Lateral Flow (UCP-LF) test detecting circulating anodic antigen (CAA), point-of-care Circulating Cathodic Antigen (POC-CCA) and Kato-Katz tests. Whole genome genotyping was conducted on 326 children comprising the top and bottom 25% of worm burden. Linear models were fitted to identify variants associated with worm burden in preselected candidate genes. Expression quantitative trait locus (eQTL) analysis was conducted for candidate genes with UCP-LF worm burden included as a covariate. Single Nucleotide Polymorphism loci associated with UCP-LF CAA included IL6 rs2066992 (OR = 0.43, p = 0.0006) and rs7793163 (OR = 2.0, p = 0.0007); IL21 SNP kgp513476 (OR 1.79, p = 0.0025) and IL17B SNP kgp708159 (OR = 0.35, p = 0.0028). A haplotype in the IL10 locus was associated with lower worm burden (OR = 0.53, p = 0.015) and overlapped SNPs rs1800896, rs1800871 and rs1800872. Significant haplotypes (p<0.05, overlapping significant SNP) associated with worm burden were observed in IL6 and the Th17 pathway IL12B and IL17B genes. There were significant eQTL in the IL6, IL5, IL21, IL25 and IFNG regions.
    Conclusions: Variants associated with S. mansoni worm burden were in IL6, FCN2, RNASE3, IL10, IL12B and IL17B gene loci. However only eQTL associations remained significant after Bonferroni correction. In summary, immune balance, pathogen recognition and Th17 pathways may play a role in modulating Schistosoma worm burden. Individuals carrying risk variants may be targeted first in allocation of control efforts to reduce the burden of schistosomiasis in the community.
    MeSH term(s) Adolescent ; Animals ; Child ; Humans ; Antigens, Helminth ; Eosinophil Cationic Protein ; Feces/chemistry ; Interleukin-10 ; Interleukin-12 Subunit p40 ; Interleukin-6/genetics ; Schistosoma mansoni/genetics ; Schistosomiasis/diagnosis ; Schistosomiasis mansoni/epidemiology ; Schistosomiasis mansoni/diagnosis ; Sensitivity and Specificity ; Uganda/epidemiology
    Chemical Substances Antigens, Helminth ; Eosinophil Cationic Protein (EC 3.1.27.-) ; FCN2 protein, human ; IL10 protein, human ; IL12B protein, human ; IL17B protein, human ; Interleukin-10 (130068-27-8) ; Interleukin-12 Subunit p40 ; Interleukin-6 ; RNASE3 protein, human (EC 3.1.27.-) ; IL6 protein, human
    Language English
    Publishing date 2023-11-30
    Publishing country United States
    Document type Journal Article
    ZDB-ID 2429704-5
    ISSN 1935-2735 ; 1935-2735
    ISSN (online) 1935-2735
    ISSN 1935-2735
    DOI 10.1371/journal.pntd.0011796
    Database MEDical Literature Analysis and Retrieval System OnLINE

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