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    Burden of Mendelian disorders in a large Middle Eastern biobank

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    Date
    2024-12
    Author
    Aamer, Waleed
    Al-Maraghi, Aljazi
    Syed, Najeeb
    Gandhi, Geethanjali Devadoss
    Aliyev, Elbay
    Al-Kurbi, Alya A.
    Al-Saei, Omayma
    Kohailan, Muhammad
    Krishnamoorthy, Navaneethakrishnan
    Palaniswamy, Sasirekha
    Al-Malki, Khulod
    Abbasi, Saleha
    Agrebi, Nourhen
    Abbaszadeh, Fatemeh
    Akil, Ammira S.Al Shabeeb
    Badii, Ramin
    Ben-Omran, Tawfeg
    Lo, Bernice
    Mokrab, Younes
    Fakhro, Khalid A.
    ...show more authors ...show less authors
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    Abstract
    Background: Genome sequencing of large biobanks from under-represented ancestries provides a valuable resource for the interrogation of Mendelian disease burden at world population level, complementing small-scale familial studies. Methods: Here, we interrogate 6045 whole genomes from Qatar—a Middle Eastern population with high consanguinity and understudied mutational burden—enrolled at the national Biobank and phenotyped for 58 clinically-relevant quantitative traits. We examine a curated set of 2648 Mendelian genes from 20 panels, annotating known and novel pathogenic variants and assessing their penetrance and impact on the measured traits. Results: We find that 62.5% of participants are carriers of at least 1 known pathogenic variant relating to recessive conditions, with homozygosity observed in 1 in 150 subjects (0.6%) for which Peninsular Arabs are particularly enriched versus other ancestries (5.8-fold). On average, 52.3 loss-of-function variants were found per genome, 6.5 of which affect a known Mendelian gene. Several variants annotated in ClinVar/HGMD as pathogenic appeared at intermediate frequencies in this cohort (1–3%), highlighting Arab founder effect, while others have exceedingly high frequencies (> 5%) prompting reconsideration as benign. Furthermore, cumulative gene burden analysis revealed 56 genes having gene carrier frequency > 1/50, including 5 ACMG Tier 3 panel genes which would be candidates for adding to newborn screening in the country. Additionally, leveraging 58 biobank traits, we systematically assess the impact of novel/rare variants on phenotypes and discover 39 candidate large-effect variants associating with extreme quantitative traits. Furthermore, through rare variant burden testing, we discover 13 genes with high mutational load, including 5 with impact on traits relevant to disease conditions, including metabolic disorder and type 2 diabetes, consistent with the high prevalence of these conditions in the region. Conclusions: This study on the first phase of the growing Qatar Genome Program cohort provides a comprehensive resource from a Middle Eastern population to understand the global mutational burden in Mendelian genes and their impact on traits in seemingly healthy individuals in high consanguinity settings.
    URI
    https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85189641836&origin=inward
    DOI/handle
    http://dx.doi.org/10.1186/s13073-024-01307-6
    http://hdl.handle.net/10576/59784
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