Tracking Telomere Fusions Through Crisis Reveals Conflict Between DNA Transcription and the DNA Damage Response

Overview

Journal NAR Cancer

Publisher Oxford University Press

Specialty Oncology

Date 2021 Jan 15

PMID 33447828

Citations 4

Authors

Kate Liddiard

Julia W Grimstead

Kez Cleal

Anna Evans

Duncan M Baird

Affiliations

Soon will be listed here.

Abstract

Identifying attributes that distinguish pre-malignant from senescent cells provides opportunities for targeted disease eradication and revival of anti-tumour immunity. We modelled a telomere-driven crisis in four human fibroblast lines, sampling at multiple time points to delineate genomic rearrangements and transcriptome developments that characterize the transition from dynamic proliferation into replicative crisis. Progression through crisis was associated with abundant intra-chromosomal telomere fusions with increasing asymmetry and reduced microhomology usage, suggesting shifts in DNA repair capacity. Eroded telomeres also fused with genomic loci actively engaged in transcription, with particular enrichment in long genes. Both gross copy number alterations and transcriptional responses to crisis likely underpin the elevated frequencies of telomere fusion with chromosomes 9, 16, 17, 19 and most exceptionally, chromosome 12. Juxtaposition of crisis-regulated genes with loci undergoing recombination exposes the collusive contributions of cellular stress responses to the evolving cancer genome.

Citing Articles

Telomeres as hotspots for innate immunity and inflammation.

Nassour J, Przetocka S, Karlseder J DNA Repair (Amst). 2023; 133:103591.

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Long-read sequencing of diagnosis and post-therapy medulloblastoma reveals complex rearrangement patterns and epigenetic signatures.

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Regulator of telomere elongation helicase 1 gene and its association with malignancy.

Hassani M, Murid J, Yan J Cancer Rep (Hoboken). 2022; 6(1):e1735.

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POLQ suppresses genome instability and alterations in DNA repeat tract lengths.

Liddiard K, Aston-Evans A, Cleal K, Hendrickson E, Baird D NAR Cancer. 2022; 4(3):zcac020.

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