Journal ArticleDOI
Sensing DNA Damage Through ATRIP Recognition of RPA-ssDNA Complexes
Lee Zou,Stephen J. Elledge +1 more
Reads0
Chats0
TLDR
The data suggest that RPA-coated ssDNA is the critical structure at sites of DNA damage that recruits the ATR-ATRIP complex and facilitates its recognition of substrates for phosphorylation and the initiation of checkpoint signaling.Abstract:
The function of the ATR (ataxia-telangiectasia mutated- and Rad3-related)-ATRIP (ATR-interacting protein) protein kinase complex is crucial for the cellular response to replication stress and DNA damage. Here, we show that replication protein A (RPA), a protein complex that associates with single-stranded DNA (ssDNA), is required for the recruitment of ATR to sites of DNA damage and for ATR-mediated Chk1 activation in human cells. In vitro, RPA stimulates the binding of ATRIP to ssDNA. The binding of ATRIP to RPA-coated ssDNA enables the ATR-ATRIP complex to associate with DNA and stimulates phosphorylation of the Rad17 protein that is bound to DNA. Furthermore, Ddc2, the budding yeast homolog of ATRIP, is specifically recruited to double-strand DNA breaks in an RPA-dependent manner. A checkpoint-deficient mutant of RPA, rfa1-t11, is defective for recruiting Ddc2 to ssDNA both in vivo and in vitro. Our data suggest that RPA-coated ssDNA is the critical structure at sites of DNA damage that recruits the ATR-ATRIP complex and facilitates its recognition of substrates for phosphorylation and the initiation of checkpoint signaling.read more
Citations
More filters
Journal ArticleDOI
Mantle cell lymphomas with low levels of cyclin D1 long mRNA transcripts are highly proliferative and can be discriminated by elevated cyclin A2 and cyclin B1
Birgitta Sander,Jenny Flygare,Anna Porwit-MacDonald,C. I. Edvard Smith,Emma K. Emanuelsson,Eva Kimby,Johan Lidén,Birger Christensson +7 more
TL;DR: Identification of MCL with low cyclin D1 3′UTR is important because it seems to be associated with shorter overall survival, and several of the upregulated genes, such as TOP2A, AURORA A and RRM2 may influence a response to therapy.
Journal ArticleDOI
Radiation-induced double-strand breaks require ATM but not Artemis for homologous recombination during S-phase
Sabrina Köcher,Thorsten Rieckmann,Gabor Rohaly,Wael Y. Mansour,Ekkehard Dikomey,Irena Dornreiter,Jochen Dahm-Daphi +6 more
TL;DR: It is shown that during S-phase Artemis but not ATM is dispensable for HR of radiation-induced DSBs, and it is demonstrated that in AT cells loading of Rad51 depends on functional ATR/Chk1.
Journal ArticleDOI
Stalled replication forks: Making ends meet for recognition and stabilization
TL;DR: Elucidation of the structural basis for recognition of arrested forks by PriA should provide useful insight into how stalled forks are recognized in eukaryotes.
Journal ArticleDOI
Cell Cycle and DNA Repair Regulation in the Damage Response: Protein Phosphatases Take Over the Reins.
TL;DR: Recent progress in the characterization of DDR-related protein phosphatases during the response to a DNA lesion is reviewed, focusing mainly on their ability to modulate the DNA damage checkpoint and the repair of the damaged DNA.
Journal ArticleDOI
Therapeutic targeting of PGBD5-induced DNA repair dependency in pediatric solid tumors.
Anton G. Henssen,Casie Reed,Eileen Jiang,Heathcliff Dorado Garcia,Jennifer von Stebut,Ian C. MacArthur,Patrick Hundsdoerfer,Jun Hyun Kim,Elisa de Stanchina,Yasumichi Kuwahara,Hajime Hosoi,Neil J. Ganem,Filemon S. Dela Cruz,Andrew L. Kung,Johannes H. Schulte,John H.J. Petrini,Alex Kentsis +16 more
TL;DR: A drug is identified that inhibits this DNA repair pathway and is therefore active against many pediatric tumor types, particularly when combined with chemotherapy, while sparing surrounding nontumor tissues and delineate a therapeutically actionable synthetic dependency induced in PGBD5-expressing solid tumors.
References
More filters
Journal ArticleDOI
The DNA damage response: putting checkpoints in perspective
TL;DR: The inability to repair DNA damage properly in mammals leads to various disorders and enhanced rates of tumour development, and this work has shown that direct activation of DNA repair networks is needed to correct this problem.
Journal ArticleDOI
Cell cycle checkpoint signaling through the ATM and ATR kinases
TL;DR: These checkpoints contain, as their most proximal signaling elements, sensor proteins that scan chromatin for partially replicated DNA, DNA strand breaks, or other abnormalities, and translate these DNA-derived stimuli into biochemical signals that modulate the functions of specific downstream target proteins.
Journal ArticleDOI
Chk1 is an essential kinase that is regulated by Atr and required for the G2/M DNA damage checkpoint
Qinghua Liu,Saritha Guntuku,Xian Shu Cui,Shuhei Matsuoka,David Cortez,Katsuyuki Tamai,Guangbin Luo,Sandra Carattini-Rivera,Francisco J. DeMayo,Allan Bradley,Lawrence A. Donehower,Stephen J. Elledge +11 more
TL;DR: It is shown that in human cells, Chk1 is phosphorylated on serine 345 (S345) in response to UV, IR, and hydroxyurea (HU).
Journal ArticleDOI
Human DNA Repair Genes
TL;DR: Modulation of DNA repair should lead to clinical applications including improvement of radiotherapy and treatment with anticancer drugs and an advanced understanding of the cellular aging process.
Journal ArticleDOI
REPLICATION PROTEIN A: A Heterotrimeric, Single-Stranded DNA-Binding Protein Required for Eukaryotic DNA Metabolism
TL;DR: Replication protein A (RPA) is a single-stranded DNA-binding protein that is required for multiple processes in eukaryotic DNA metabolism, including DNA replication, DNA repair, and recombination.