Abstract

DNA double strand breaks (DSBs) are a particularly severe and mutagenic form of DNA damage as they disrupt genetic continuity. Proteins involved in prevention and repair of DSBs are associated with a variety of severe human diseases, such as breast and ovarian cancer (BRCA1 and BRCA2), Nijmegan breakage Syndrome (NBS1), Blood's syndrome (BLM), Ataxia telangiectasia (Mre11) and premature aging (WRN). In this project we aim to understand, at the molecular level, early events of DSB repair (DSBR) such as DSB recognition and processing, DSBR by non-homologous end joining (NHEJ), and DSB prevention by RecQ family helicases. Research of t he past years revealed that proteins involved in DSBR often not only interact with each other and other DNA repair proteins but exist in large super assemblies or repairosomes. The resulting complexity of protein-protein interactions and of conformational switches makes it necessary to shift efforts to understand the underlying molecular events, from the analysis of individual components, as has been successfully performed in the past, to the study of complexes and super-assemblies. For that reason, we propose to elucidate molecular events of protein-protein interactions, assembly states and conformational switching, for early events in DSBR. Tight synergies with Projects 4 (Homologous Recombination Repair) and 5 (Mismatch Repair interactions), plus collaborative efforts within this Program Project, will ensure the required experimental innovations, aided by advance technologies for protein expression and protein characterization techniques (EMB Core) and for the structure determination of larger complexes (SCB Core). We will begin to understand the complex nature of DSBR conformational switching and interactions by focusing on five Specific Aims:
Aim 1 will study functional and structural switches in the NHEJ machinery in response to phosphorylation;
Aim 2 will study the structure and function of the Rad50/BRCA1 interaction;
Aim 3 will study the modulation of end processing of the Rad50/Mre11/Nbs1 complex by RPA;
Aim 4 will study the structure and function of DSB preventive RecQ helicases;
and Aim 5 will study early temporal and spatial interaction of DSBR factors by a chromatin immunoprecipitation. The anticipated combined outcome of the proposed five specific Aims will be a molecular picture of protein-protein interactions and functional states orchestrating early events o DSBR. This picture will provide the molecular foundation for a detailed understanding of human diseases and cancer predispositions linked to DSBR proteins.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA092584-02
Application #
6652791
Study Section
Subcommittee E - Prevention &Control (NCI)
Project Start
2002-09-01
Project End
2003-08-31
Budget Start
Budget End
Support Year
2
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
Lawrence Berkeley National Laboratory
Department
Type
DUNS #
078576738
City
Berkeley
State
CA
Country
United States
Zip Code
94720

  Publications

Sung, Patrick (2018) Introduction to the Thematic Minireview Series: DNA double-strand break repair and pathway choice. J Biol Chem 293:10500-10501
Shen, Jianfeng; Ju, Zhenlin; Zhao, Wei et al. (2018) ARID1A deficiency promotes mutability and potentiates therapeutic antitumor immunity unleashed by immune checkpoint blockade. Nat Med 24:556-562
Sengupta, Shiladitya; Yang, Chunying; Hegde, Muralidhar L et al. (2018) Acetylation of oxidized base repair-initiating NEIL1 DNA glycosylase required for chromatin-bound repair complex formation in the human genome increases cellular resistance to oxidative stress. DNA Repair (Amst) 66-67:1-10
Mu, Hong; Geacintov, Nicholas E; Broyde, Suse et al. (2018) Molecular basis for damage recognition and verification by XPC-RAD23B and TFIIH in nucleotide excision repair. DNA Repair (Amst) :
Chavez, Diana A; Greer, Briana H; Eichman, Brandt F (2018) The HIRAN domain of helicase-like transcription factor positions the DNA translocase motor to drive efficient DNA fork regression. J Biol Chem 293:8484-8494
Wang, Jing L; Duboc, Camille; Wu, Qian et al. (2018) Dissection of DNA double-strand-break repair using novel single-molecule forceps. Nat Struct Mol Biol 25:482-487
Crickard, J Brooks; Kaniecki, Kyle; Kwon, Youngho et al. (2018) Meiosis-specific recombinase Dmc1 is a potent inhibitor of the Srs2 antirecombinase. Proc Natl Acad Sci U S A 115:E10041-E10048
Syed, Aleem; Tainer, John A (2018) The MRE11-RAD50-NBS1 Complex Conducts the Orchestration of Damage Signaling and Outcomes to Stress in DNA Replication and Repair. Annu Rev Biochem 87:263-294
Howes, Timothy R L; Sallmyr, Annahita; Brooks, Rhys et al. (2018) Erratum to ""Structure-activity relationships among DNA ligase inhibitors; characterization of a selective uncompetitive DNA ligase I inhibitor"" [DNA Repair 60C (2017) 29-39]. DNA Repair (Amst) 61:99
Bhattacharyya, Sudipta; Soniat, Michael M; Walker, David et al. (2018) Phage Mu Gam protein promotes NHEJ in concert with Escherichia coli ligase. Proc Natl Acad Sci U S A 115:E11614-E11622

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