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DNA damage response inhibition at dysfunctional telomeres by modulation of telomeric DNA damage response RNAs

The DNA damage response (DDR) involves site-specific small non-coding RNAs. Here the authors show that telomere dysfunction induces transcription of telomeric DNA damage response RNAs that are necessary for DDR activation, which can be specifically muted by antisense inhibitory oligonucleotides.

Francesca Rossiello
Julio Aguado
Fabrizio d’Adda di Fagagna
ResearchOpen Access27 Feb 2017
Nature Communications

Volume: 8, P: 1-14
Correction: Corrigendum: DNA damage response inhibition at dysfunctional telomeres by modulation of telomeric DNA damage response RNAs

Francesca Rossiello
Julio Aguado
Fabrizio d’Adda di Fagagna
Amendments and CorrectionsOpen Access13 Apr 2017
Nature Communications

Volume: 8, P: 1-2
Erratum: Telomeric DNA damage is irreparable and causes persistent DNA-damage-response activation

Marzia Fumagalli
Francesca Rossiello
Fabrizio d'Adda di Fagagna
Amendments and Corrections02 May 2012
Nature Cell Biology

Volume: 14, P: 555
Inhibition of DNA damage response at telomeres improves the detrimental phenotypes of Hutchinson–Gilford Progeria Syndrome

Hutchinson–Gilford progeria syndrome causes premature aging. Here the authors show that activation of the DNA damage response at dysfunctional telomeres and transcription of telomeric non-coding RNAs contributes to the pathogenesis, which can be ameliorated by treatment with sequence-specific telomeric antisense oligonucleotides.

Julio Aguado
Agustin Sola-Carvajal
Fabrizio d’Adda di Fagagna
ResearchOpen Access18 Nov 2019
Nature Communications

Volume: 10, P: 1-11
Telomeric DNA damage is irreparable and causes persistent DNA-damage-response activation

D’Adda di Fagagna and colleagues observe that, after genotoxic treatment of cells and mice, unrepaired DNA-damage foci and DNA-damage signalling persist at telomeres. They show that introducing the telomeric protein TRF2 near a double-strand break elsewhere on the chromosomes prevents repair. Unrepaired foci are also observed at telomeres of ageing animals, suggesting a role for TRF2 in senescence establishment.

Marzia Fumagalli
Francesca Rossiello
Fabrizio d’Adda di Fagagna
Research18 Mar 2012
Nature Cell Biology

Volume: 14, P: 355-365
Telomere dysfunction in ageing and age-related diseases

Rossiello et al. review the contributions of telomere shortening and/or dysfunction to ageing and a broad spectrum of age-associated human diseases.

Francesca Rossiello
Diana Jurk
Fabrizio d’Adda di Fagagna
Reviews14 Feb 2022
Nature Cell Biology

Volume: 24, P: 135-147
Alternative lengthening of telomeres (ALT) cells viability is dependent on C-rich telomeric RNAs

ALT cells use an alternative lengthening mechanism of telomeres and bear telomeric DNA damage with increased levels of damage-induced long non-coding RNA. Here the AUs show that antisense oligonucleotides (ASO) targeting such RNAs can induce ALT cancer cells selective cell death.

Ilaria Rosso
Corey Jones-Weinert
Fabrizio d’Adda di Fagagna
ResearchOpen Access04 Nov 2023
Nature Communications

Volume: 14, P: 1-16
RNase A treatment and reconstitution with DNA damage response RNA in living cells as a tool to study the role of non-coding RNA in the formation of DNA damage response foci

RATaR (RNase A treatment and reconstitution) enables users to study the role of DNA damage response RNA (DDRNA) in the assembly of DNA damage response foci.

Flavia Michelini
Francesca Rossiello
Sofia Francia
Protocols08 Apr 2019
Nature Protocols

Volume: 14, P: 1489-1508
Telomere damage promotes vascular smooth muscle cell senescence and immune cell recruitment after vessel injury

Anna Uryga and Mandy Grootaert et al. combine cell culture and animal models to examine how senescence of human vascular smooth muscle cells (VSMCs) and persistent telomere damage drive inflammation. Their results suggest that telomere injury can be the primary cause of premature senescence in VSMCs, and that DNA damage can be a major cause of persistent inflammation in vascular disease.

Anna K. Uryga
Mandy O. J. Grootaert
Martin R. Bennett
ResearchOpen Access21 May 2021
Communications Biology

Volume: 4, P: 1-16
Target-enrichment sequencing for detailed characterization of small RNAs

This protocol describes a method to sequence small RNAs by target enrichment (TEsR). By enriching for sRNAs, TEsR allows the quantitative detection of not only small RNAs but also their precursors and intermediate and mature forms.

Quan Nguyen
Julio Aguado
Piero Carninci
Protocols22 Mar 2018
Nature Protocols

Volume: 13, P: 768-786

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