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    TRAIP resolves DNA replication-transcription conflicts during the S-phase of unperturbed cells

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    Authors
    Scaramuzza, Shaun
    Jones, R. M.
    Sadurni, M. M.
    Reynolds-Winczura, A.
    Poovathumkadavil, D.
    Farrell, A.
    Natsume, T.
    Rojas, P.
    Cuesta, C. F.
    Kanemaki, M. T.
    Saponaro, M.
    Gambus, A.
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    Affiliation
    Institute of Cancer and Genomic Sciences, Birmingham Centre for Genome Biology, University of Birmingham, Birmingham, UK
    Issue Date
    2023
    
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    Abstract
    Cell division is the basis for the propagation of life and requires accurate duplication of all genetic information. DNA damage created during replication (replication stress) is a major cause of cancer, premature aging and a spectrum of other human disorders. Over the years, TRAIP E3 ubiquitin ligase has been shown to play a role in various cellular processes that govern genome integrity and faultless segregation. TRAIP is essential for cell viability, and mutations in TRAIP ubiquitin ligase activity lead to primordial dwarfism in patients. Here, we have determined the mechanism of inhibition of cell proliferation in TRAIP-depleted cells. We have taken advantage of the auxin induced degron system to rapidly degrade TRAIP within cells and to dissect the importance of various functions of TRAIP in different stages of the cell cycle. We conclude that upon rapid TRAIP degradation, specifically in S-phase, cells cease to proliferate, arrest in G2 stage of the cell cycle and undergo senescence. Our findings reveal that TRAIP works in S-phase to prevent DNA damage at transcription start sites, caused by replication-transcription conflicts.
    Citation
    Scaramuzza S, Jones RM, Sadurni MM, Reynolds-Winczura A, Poovathumkadavil D, Farrell A, et al. TRAIP resolves DNA replication-transcription conflicts during the S-phase of unperturbed cells. Nature communications. 2023 Aug 21;14(1):5071. PubMed PMID: 37604812. Epub 2023/08/22. eng.
    Journal
    Nature Communications
    URI
    http://hdl.handle.net/10541/626523
    DOI
    10.1038/s41467-023-40695-y
    PubMed ID
    37604812
    Additional Links
    https://dx.doi.org/10.1038/s41467-023-40695-y
    Type
    Article
    Language
    en
    ae974a485f413a2113503eed53cd6c53
    10.1038/s41467-023-40695-y
    Scopus Count
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    All Paterson Institute for Cancer Research

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