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Genomic hallmarks and therapeutic implications of G0 cell cycle arrest in cancer

Abstract:
Background: Therapy resistance in cancer is often driven by a subpopulation of cells that are temporarily arrested in a non-proliferative G0 state, which is difficult to capture and whose mutational drivers remain largely unknown. Results: We develop methodology to robustly identify this state from transcriptomic signals and characterise its prevalence and genomic constraints in solid primary tumours. We show that G0 arrest preferentially emerges in the context of more stable, less mutated genomes which maintain TP53 integrity and lack the hallmarks of DNA damage repair deficiency, while presenting increased APOBEC mutagenesis. We employ machine learning to uncover novel genomic dependencies of this process and validate the role of the centrosomal gene CEP89 as a modulator of proliferation and G0 arrest capacity. Lastly, we demonstrate that G0 arrest underlies unfavourable responses to various therapies exploiting cell cycle, kinase signalling and epigenetic mechanisms in single-cell data. Conclusions: We propose a G0 arrest transcriptional signature that is linked with therapeutic resistance and can be used to further study and clinically track this state
Publication status:
Published
Peer review status:
Peer reviewed

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Publisher copy:
10.1186/s13059-023-02963-4
Publication website:
https://escholarship.org/content/qt93q6k9ht/qt93q6k9ht.pdf

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Role:
Author
ORCID:
0000-0002-2750-0932
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Role:
Author
ORCID:
0000-0003-4919-2384
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Role:
Author
ORCID:
0000-0002-2025-0256
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Role:
Author
ORCID:
0000-0003-3923-670X


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Funder identifier:
10.13039/501100000289
Grant:
C63833/A25729
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Funder identifier:
10.13039/100010269
Grant:
215296/Z/19/Z
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Funder identifier:
10.13039/501100009187
Grant:
MR/N013867/1
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Funder identifier:
10.13039/501100000691
Grant:
SBF004\1042
More from this funder
Funder identifier:
10.13039/501100000268
Grant:
BB/R01356X/1


Publisher:
BioMed Central
Journal:
Genome Biology More from this journal
Volume:
24
Issue:
1
Pages:
128-128
Article number:
128
Publication date:
2023-05-23
DOI:
EISSN:
1474-760X
ISSN:
1474-7596


Language:
English
Keywords:
Pubs id:
1344749
Local pid:
pubs:1344749
Source identifiers:
W4377940884
Deposit date:
2026-05-08
ARK identifier:
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