Abstract

One of the most difficult problems in the treatment of cancer is acquired resistance to chemotherapy. Defects in DNA repair are likely to play a critical role in the sensitivity of cancer cells to chemotherapeutic drugs, many of which are DNA-damaging agents. Fanconi Anemia (FA) is a genetic disorder characterized by cancer susceptibility and cellular hypersensitivity to DNA crosslinking agents, such as cisplatin and melphalan. FA proteins and breast/ovarian cancer susceptibility gene products (BRCA1 and BRCA2) cooperate in a common DNA damage-activated signaling pathway (the FA-BRCA pathway), which controls DNA repair. We hypothesize that integrity of the FA-BRCA pathway is a critical determinant of resistance of tumor cells to chemotherapy with DNA crosslinking agents. The goals of our proposed research are 1) to elucidate the role of the FA-BRCA pathway in cisplatin sensitivity/resistance of cancer cells, 2) to determine if the sensitivity of tumor cells to DNA crosslinking agents can be increased by modulating the FA- BRCA pathway using small molecule inhibitors of the pathway, and 3) to further elucidate the mechanism of regulation of the FA-BRCA pathway. We plan to determine the role of one of the FA genes, BRCA2/FANCD1, in acquired resistance to cisplatin by analyzing BRCA2-deficient cancer cell lines and clinical samples of ovarian cancer. We also plan to identify small molecule inhibitors of the FA-BRCA pathway which sensitize tumor cells to DNA crosslinking agents. Several candidate chemicals including cyclin dependent kinase inhibitors and proteasome inhibitors have already emerged from our initial screens. We plan to test if these inhibitors sensitize cancer cells to cisplatin and ultimately to elucidate the mechanism of actions of these drugs. We also plan to elucidate involvement of cyclin-dependent kinases and the proteasome in the regulation of the FA-BRCA pathway using the inhibitors we identified. These studies will lead to discovery of potential drugs that can be used as chemo-sensitizers in the treatment of cancer, provide new insights about the signaling of the FA-BRCA pathway, and may eventually lead to establishment of a strategy to overcome chemo-resistance of cancer. Relevance: Our studies are intended to clarify why some cancers can be effectively treated with drugs that cause DNA damage and others become resistant. They should also lead to a discovery of ways to make cancer chemotherapy more effective. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA125636-01A1
Application #
7318026
Study Section
Basic Mechanisms of Cancer Therapeutics Study Section (BMCT)
Program Officer
Arya, Suresh
Project Start
2007-07-01
Project End
2012-05-31
Budget Start
2007-07-01
Budget End
2008-05-31
Support Year
1
Fiscal Year
2007
Total Cost
$317,289
Indirect Cost

  Institution

Name
Fred Hutchinson Cancer Research Center
Department
Type
DUNS #
078200995
City
Seattle
State
WA
Country
United States
Zip Code
98109

  Publications

Calses, Philamer C; Dhillon, Kiranjit K; Tucker, Nyka et al. (2017) DGCR8 Mediates Repair of UV-Induced DNA Damage Independently of RNA Processing. Cell Rep 19:162-174
Cheung, Ronald S; Castella, Maria; Abeyta, Antonio et al. (2017) Ubiquitination-Linked Phosphorylation of the FANCI S/TQ Cluster Contributes to Activation of the Fanconi Anemia I/D2 Complex. Cell Rep 19:2432-2440
Drost, Rinske; Dhillon, Kiranjit K; van der Gulden, Hanneke et al. (2016) BRCA1185delAG tumors may acquire therapy resistance through expression of RING-less BRCA1. J Clin Invest 126:2903-18
Castella, Maria; Jacquemont, Celine; Thompson, Elizabeth L et al. (2015) FANCI Regulates Recruitment of the FA Core Complex at Sites of DNA Damage Independently of FANCD2. PLoS Genet 11:e1005563
Wang, Yemin; Huang, Jen-Wei; Castella, Maria et al. (2014) p53 is positively regulated by miR-542-3p. Cancer Res 74:3218-27
Huang, Jen-Wei; Wang, Yemin; Dhillon, Kiranjit K et al. (2013) Systematic screen identifies miRNAs that target RAD51 and RAD51D to enhance chemosensitivity. Mol Cancer Res 11:1564-73
Wang, Yemin; Taniguchi, Toshi (2013) MicroRNAs and DNA damage response: implications for cancer therapy. Cell Cycle 12:32-42
Jacquemont, CĂ©line; Simon, Julian A; D'Andrea, Alan D et al. (2012) Non-specific chemical inhibition of the Fanconi anemia pathway sensitizes cancer cells to cisplatin. Mol Cancer 11:26
Swisher, Elizabeth M; Taniguchi, Toshiyasu; Karlan, Beth Y (2012) Molecular scores to predict ovarian cancer outcomes: a worthy goal, but not ready for prime time. J Natl Cancer Inst 104:642-5
Wang, Yemin; Huang, Jen-Wei; Calses, Philamer et al. (2012) MiR-96 downregulates REV1 and RAD51 to promote cellular sensitivity to cisplatin and PARP inhibition. Cancer Res 72:4037-46

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