Cargando…

DROSHA is recruited to DNA damage sites by the MRN complex to promote non-homologous end joining

The DNA damage response (DDR) is the signaling cascade that recognizes DNA double-strand breaks (DSBs) and promotes their resolution via the DNA repair pathways of non-homologous end joining (NHEJ) or homologous recombination (HR). We and others have shown that DDR activation requires DROSHA; howeve...

Descripción completa

Detalles Bibliográficos
Autores principales:	Cabrini, Matteo, Roncador, Marco, Galbiati, Alessandro, Cipolla, Lina, Maffia, Antonio, Iannelli, Fabio, Sabbioneda, Simone, d’Adda di Fagagna, Fabrizio, Francia, Sofia
Formato:	Online Artículo Texto
Lenguaje:	English
Publicado:	The Company of Biologists Ltd 2021
Materias:	Research Article
Acceso en línea:	https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8015226/ https://www.ncbi.nlm.nih.gov/pubmed/33558311 http://dx.doi.org/10.1242/jcs.249706

Ejemplares similares

DICER, DROSHA and DNA damage response RNAs are necessary for the secondary recruitment of DNA damage response factors
por: Francia, Sofia, et al.
Publicado: (2016)

Site-specific DICER and DROSHA RNA products control the DNA damage response
por: Francia, Sofia, et al.
Publicado: (2012)

A damaged genome’s transcriptional landscape through multilayered expression profiling around in situ-mapped DNA double-strand breaks
por: Iannelli, Fabio, et al.
Publicado: (2017)

Need telomere maintenance? Call 911
por: Francia, Sofia, et al.
Publicado: (2007)

A novel single‐cell method provides direct evidence of persistent DNA damage in senescent cells and aged mammalian tissues
por: Galbiati, Alessandro, et al.
Publicado: (2017)

Pharmacological boost of DNA damage response and repair by enhanced biogenesis of DNA damage response RNAs
por: Gioia, Ubaldo, et al.
Publicado: (2019)

Multiple functions of MRN in end-joining pathways during isotype class switching
por: Dinkelmann, Maria, et al.
Publicado: (2009)

CtIP and MRN promote non-homologous end-joining of etoposide-induced DNA double-strand breaks in G1
por: Quennet, Verena, et al.
Publicado: (2011)

MRE11-RAD50-NBS1 Complex Is Sufficient to Promote Transcription by RNA Polymerase II at Double-Strand Breaks by Melting DNA Ends
por: Sharma, Sheetal, et al.
Publicado: (2021)

The Regulation of DNA Damage Tolerance by Ubiquitin and Ubiquitin-Like Modifiers
por: Cipolla, Lina, et al.
Publicado: (2016)

Damage-induced lncRNAs control the DNA damage response through interaction with DDRNAs at individual double-strand breaks
por: Michelini, Flavia, et al.
Publicado: (2017)

Never-ageing cellular senescence
por: Ogrunc, Müge, et al.
Publicado: (2011)

Neural stem cells exposed to BrdU lose their global DNA methylation and undergo astrocytic differentiation
por: Schneider, Leonid, et al.
Publicado: (2012)

Detection of Telomeric DNA:RNA Hybrids Using TeloDRIP-qPCR
por: Rosso, Ilaria, et al.
Publicado: (2020)

NOTCH1 Inhibits Activation of ATM by Impairing the Formation of an ATM-FOXO3a-KAT5/Tip60 Complex
por: Adamowicz, Marek, et al.
Publicado: (2016)

A Role for Human DNA Polymerase λ in Alternative Lengthening of Telomeres
por: Mentegari, Elisa, et al.
Publicado: (2021)

DNA damage response inhibition at dysfunctional telomeres by modulation of telomeric DNA damage response RNAs
por: Rossiello, Francesca, et al.
Publicado: (2017)

Corrigendum: DNA damage response inhibition at dysfunctional telomeres by modulation of telomeric DNA damage response RNAs
por: Rossiello, Francesca, et al.
Publicado: (2017)

Stable Cellular Senescence Is Associated with Persistent DDR Activation
por: Fumagalli, Marzia, et al.
Publicado: (2014)

The spatial organization of non-homologous end joining: From bridging to end joining
por: Ochi, Takashi, et al.
Publicado: (2014)

ZNF281 is recruited on DNA breaks to facilitate DNA repair by non-homologous end joining
por: Nicolai, Sara, et al.
Publicado: (2019)

DNA damage response at telomeres boosts the transcription of SARS‐CoV‐2 receptor ACE2 during aging
por: Sepe, Sara, et al.
Publicado: (2021)

Irreparable telomeric DNA damage and persistent DDR signalling as a shared causative mechanism of cellular senescence and ageing
por: Rossiello, Francesca, et al.
Publicado: (2014)

The cohesin complex prevents Myc-induced replication stress
por: Rohban, Sara, et al.
Publicado: (2017)

The Ku-binding motif is a conserved module for recruitment and stimulation of non-homologous end-joining proteins
por: Grundy, Gabrielle J., et al.
Publicado: (2016)

Transcriptional and post-transcriptional regulation of the ionizing radiation response by ATM and p53
por: Venkata Narayanan, Ishwarya, et al.
Publicado: (2017)

SRSF3 recruits DROSHA to the basal junction of primary microRNAs
por: Kim, Kijun, et al.
Publicado: (2018)

UBR5 interacts with the replication fork and protects DNA replication from DNA polymerase η toxicity
por: Cipolla, Lina, et al.
Publicado: (2019)

MRN-dependent and independent pathways for recruitment of TOPBP1 to DNA double-strand breaks
por: Montales, Katrina, et al.
Publicado: (2022)

BRCA2 controls DNA:RNA hybrid level at DSBs by mediating RNase H2 recruitment
por: D’Alessandro, Giuseppina, et al.
Publicado: (2018)

The MRN complex promotes DNA repair by homologous recombination and restrains antigenic variation in African trypanosomes
por: Mehnert, Ann-Kathrin, et al.
Publicado: (2021)

Rad51 recruitment and exclusion of non-homologous end joining during homologous recombination at a Tus/Ter mammalian replication fork barrier
por: Willis, Nicholas A., et al.
Publicado: (2018)

Replication of Structured DNA and its implication in epigenetic stability
por: Cea, Valentina, et al.
Publicado: (2015)

Non-homologous end joining in class switch recombination: the beginning of the end
por: Kotnis, Ashwin, et al.
Publicado: (2008)

PIAS3 promotes homology-directed repair and distal non-homologous end joining
por: LIU, SHICUI, et al.
Publicado: (2013)

Telomere damage promotes vascular smooth muscle cell senescence and immune cell recruitment after vessel injury
por: Uryga, Anna K., et al.
Publicado: (2021)

The Intermediate Filament Synemin Regulates Non-Homologous End Joining in an ATM-Dependent Manner
por: Deville, Sara Sofia, et al.
Publicado: (2020)

Homology and enzymatic requirements of microhomology-dependent alternative end joining
por: Sharma, S, et al.
Publicado: (2015)

DNA non-homologous end-joining enters the resection arena
por: Jeggo, Penny A., et al.
Publicado: (2017)

Non-homologous end joining repair in Xenopus egg extract
por: Zhu, Songli, et al.
Publicado: (2016)

Cannot write session to /tmp/vufind_sessions/sess_i288ivdorug8vjhgdtoq1gjp7h