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    Near-complete Middle Eastern genomes refine autozygosity and enhance disease-causing and population-specific variant discovery

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    s41588-025-02173-7.pdf (7.195Mb)
    Date
    2025-05-05
    Author
    Ghorbani, Mohammadmersad
    Moosa, Shabir
    Siddig, Zenab
    Farhad, Radi
    Naeem, Haroon
    Harvey, William T.
    Mastrorosa, Francesco Kumara
    Munson, Katherine M.
    Mohamad Razali, Rozaimi
    Aliyev, Elbay
    Diboun, Ilhame
    Abouelhassan, Rawan
    Tauro, Melissa
    Hassan, Sondoss
    Mathew, Rebecca
    Al Hashmi, Muna
    Mathew, Lisa S.
    Wang, Kun
    Salhab, Abdul Rahman
    Vempalli, Fazulur Rehaman
    El Khouly, Ahmed
    Tatari, Zohreh
    Suhre, Karsten
    Puthen, Jithesh V.
    Fakhro, Khalid
    Estivill, Xavier
    Chouchane, Lotfi
    Badii, Ramin
    Alshafai, Mashael
    Al-Khodor, Souhaila
    Albagha, Omar
    Al-Ali, Rashid
    Poolat, Shafeeq
    Pathare, Tushar
    Zaid, Tariq Abu
    Hamza, Mehshad
    Khatib, Mohammedhusen
    Saqri, Tariq Abu
    Temanni, Ramzi
    Almabrazi, Hakeem
    Syed, Najeeb
    Lorenz, Stephan
    Liu, Wei
    Afifi, Nahla
    Alkhayat, Eiman
    Qafoud, Fatima
    Fethnou, Eleni
    Althani, Asmaa
    Saad, Chadi
    Al-Sarraj, Yasser
    Alvi, Muhammad
    Alkuwari, Fatima
    Abdellatif, Rania
    Ennaifar, Maryem
    Yasin, Heba
    Fadl, Tasnim
    Darwish, Dima
    Mbarek, Hamdi
    Badji, Radja
    Al-Muftah, Wadha
    Ismail, Said I.
    Alazwani, Iman
    Tomei, Sara
    Fakhro, Khalid A.
    Satti, Alia
    Benini, Ruba
    Rhie, Arang
    Eichler, Evan E.
    Mokrab, Younes
    ...show more authors ...show less authors
    Metadata
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    Abstract
    Advances in long-read sequencing have enabled routine complete assembly of human genomes, but much remains to be done to represent broader populations and show impact on disease-gene discovery. Here, we report highly accurate, near-complete and phased genomes from six Middle Eastern (ME) family trios (n = 18) with neurodevelopmental conditions, representing ancestries from Sudan, Jordan, Syria, Qatar and Afghanistan. These genomes revealed 42.2 Mb of new sequence (13.8% impacting known genes), 75 new HLA/KIR alleles and strong signals of inbreeding, with ROH covering up to one-third of chromosomes 6 and 12 in one individual. Using assembly-based variant calling, we identified 23 de novo and recessive variants as strong candidates for causing previously unresolved symptoms in the probands. The ME genomes revealed unique variation relative to existing references, showing enhanced mappability and variant calling. These results underscore the value of de novo assembly for disease variant discovery and the need for sampled ME-specific references to better characterize population-relevant variation.
    URI
    https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=105004360655&origin=inward
    DOI/handle
    http://dx.doi.org/10.1038/s41588-025-02173-7
    http://hdl.handle.net/10576/65537
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    • Biomedical Sciences [‎832‎ items ]

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