Decitabine cytotoxicity is promoted by dCMP deaminase DCTD and mitigated by SUMO-dependent E3 ligase TOPORS

Carnie, Christopher J; Götz, Maximilian J; Palma-Chaundler, Chloe S; Weickert, Pedro; Wanders, Amy; Serrano-Benitez, Almudena; Li, Hao-Yi; Gupta, Vipul; Awwad, Samah W; Blum, Christian J; Sczaniecka-Clift, Matylda; Cordes, Jacqueline; Zagnoli-Vieira, Guido; D’Alessandro, Giuseppina; Richards, Sean L; Gueorguieva, Nadia; Lam, Simon; Beli, Petra; Stingele, Julian; Jackson, Stephen P

doi:10.1038/s44318-024-00108-2

EMBO J

2024

DOI: 10.1038/s44318-024-00108-2

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Decitabine cytotoxicity is promoted by dCMP deaminase DCTD and mitigated by SUMO-dependent E3 ligase TOPORS

Christopher J Carnie,

Maximilian J Götz,

Chloe S Palma-Chaundler

et al.

Abstract: The nucleoside analogue decitabine (or 5-aza-dC) is used to treat several haematological cancers. Upon its triphosphorylation and incorporation into DNA, 5-aza-dC induces covalent DNA methyltransferase 1 DNA–protein crosslinks (DNMT1-DPCs), leading to DNA hypomethylation. However, 5-aza-dC’s clinical outcomes vary, and relapse is common. Using genome-scale CRISPR/Cas9 screens, we map factors determining 5-aza-dC sensitivity. Unexpectedly, we find that loss of the dCMP deaminase DCTD causes 5-aza-dC resistance,… Show more

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Understanding the interplay between dNTP metabolism and genome stability in cancer

Yagüe-Capilla,

Rudd

2024

Disease Models &Amp; Mechanisms

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The size and composition of the intracellular DNA precursor pool is integral to the maintenance of genome stability, and this relationship is fundamental to our understanding of cancer. Key aspects of carcinogenesis, including elevated mutation rates and induction of certain types of DNA damage in cancer cells, can be linked to disturbances in deoxynucleoside triphosphate (dNTP) pools. Furthermore, our approaches to treat cancer heavily exploit the metabolic interplay between the DNA and the dNTP pool, with a long-standing example being the use of antimetabolite-based cancer therapies, and this strategy continues to show promise with the development of new targeted therapies. In this Review, we compile the current knowledge on both the causes and consequences of dNTP pool perturbations in cancer cells, together with their impact on genome stability. We outline several outstanding questions remaining in the field, such as the role of dNTP catabolism in genome stability and the consequences of dNTP pool expansion. Importantly, we detail how our mechanistic understanding of these processes can be utilised with the aim of providing better informed treatment options to patients with cancer.

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Understanding the interplay between dNTP metabolism and genome stability in cancer

Yagüe-Capilla,

Rudd

2024

Disease Models &Amp; Mechanisms

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Decitabine cytotoxicity is promoted by dCMP deaminase DCTD and mitigated by SUMO-dependent E3 ligase TOPORS

Cited by 1 publication

References 90 publications

Understanding the interplay between dNTP metabolism and genome stability in cancer

Understanding the interplay between dNTP metabolism and genome stability in cancer

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