Abstract

Pancreatic ductal adenocarcinoma is the 4th leading cause of cancer death in the United States and it has the lowest survival rate for any solid cancer. The goal of personalized cancer therapy is to identify molecular defects that predict drug responses or to test the cancers themselves for drug sensitivities and treat the patient with the optimal drug regimen. The pancreatic cancer genome project identified heterogeneity in the molecular alterations of pancreatic cancers indicating the need for personalized cancer therapy. To this end, we have identified molecular predictors of pancreatic cancer chemotherapy responses. We know that the majority of genes mutated in patients with familial pancreatic cancer are in the homologous DNA repair including BRCA2/BRCA1/PALB2/Fanconi Anemia pathway mutations. Pancreatic and other cancers with defects in homologous DNA repair are exquisitely sensitive to Parp inhibitors and to other drugs that cause double-strand DNA breaks. The Parp inhibitor, olaparib, now in phase 2 clinical trials, has shown a 44% response rate in patients with ovarian cancer. Therefore, we propose a clinical trial randomizing patients to a low-dose DNA strand break regimen of monthly cycles of chemotherapy (irinotecan, cisplatin, bleomycin and mitomycin C) with or without the oral Parp inhibitor, olarparib. We will target patients most likely to respond to this protocol including patients with known BRCA mutations, familial pancreatic cancer, or Ashkenazi ancestry as well as patients with usual pancreatic cancer. Patients and their cancer samples will undergo gene testing to identify gene defects in homologous DNA repair to determine if gene testing can identify patients most likely to respond to Parp inhibitor based therapy. Cell lines will be developed from patient samples to correlate clinical responses to therapy with responses in the laboratory. Circulating mutant DNA will be measured to determine how well it predicts response to therapy.

Public Health Relevance

Pancreatic cancer is the deadliest of the common cancers and the 4th commonest cause of cancer death. Clinical trials that utilize personalized cancer therapy are needed for this disease. We propose a randomized phase 2 trial using a very promising therapy, the oral Parp inhibitor, olarparib, combined with therapies for patients with pancreatic cancer predicted to respond to these drugs based on their genetic profiles and in vitro responses to these agents.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
High Impact Research and Research Infrastructure Programs (RC2)
Project #
5RC2CA148346-02
Application #
7943946
Study Section
Special Emphasis Panel (ZCA1-RPRB-J (O9))
Program Officer
Agarwal, Rajeev K
Project Start
2009-09-30
Project End
2013-08-31
Budget Start
2010-09-01
Budget End
2013-08-31
Support Year
2
Fiscal Year
2010
Total Cost
$962,168
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Pediatrics
Type
Schools of Medicine
DUNS #
001910777
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Yarchoan, Mark; Myzak, Melinda C; Johnson 3rd, Burles A et al. (2017) Olaparib in combination with irinotecan, cisplatin, and mitomycin C in patients with advanced pancreatic cancer. Oncotarget 8:44073-44081
Li, Ang; Yu, Jun; Kim, Haeryoung et al. (2013) MicroRNA array analysis finds elevated serum miR-1290 accurately distinguishes patients with low-stage pancreatic cancer from healthy and disease controls. Clin Cancer Res 19:3600-10
Kanda, Mitsuro; Sadakari, Yoshihiko; Borges, Michael et al. (2013) Mutant TP53 in duodenal samples of pancreatic juice from patients with pancreatic cancer or high-grade dysplasia. Clin Gastroenterol Hepatol 11:719-30.e5
Li, Ang; Yu, Jun; Kim, Haeryoung et al. (2013) Serum miR-1290 as a marker of pancreatic cancer--response. Clin Cancer Res 19:5252-3
Kanda, Mitsuro; Knight, Spencer; Topazian, Mark et al. (2013) Mutant GNAS detected in duodenal collections of secretin-stimulated pancreatic juice indicates the presence or emergence of pancreatic cysts. Gut 62:1024-33
O'Sullivan, Eileen; Goggins, Michael (2013) DNA methylation analysis in human cancer. Methods Mol Biol 980:131-56
Dinnen, Richard D; Mao, Yuehua; Qiu, Wanglong et al. (2013) Redirecting apoptosis to aponecrosis induces selective cytotoxicity to pancreatic cancer cells through increased ROS, decline in ATP levels, and VDAC. Mol Cancer Ther 12:2792-803
Kanda, Mitsuro; Matthaei, Hanno; Wu, Jian et al. (2012) Presence of somatic mutations in most early-stage pancreatic intraepithelial neoplasia. Gastroenterology 142:730-733.e9
Hong, Seung-Mo; Omura, Noriyuki; Vincent, Audrey et al. (2012) Genome-wide CpG island profiling of intraductal papillary mucinous neoplasms of the pancreas. Clin Cancer Res 18:700-12
Yu, Jun; Li, Ang; Hong, Seung-Mo et al. (2012) MicroRNA alterations of pancreatic intraepithelial neoplasias. Clin Cancer Res 18:981-92

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