JOP. J Pancreas (Online) 2012 Mar 10; 13(2):180-181.

 

 

BRCA and Pancreatic Cancer: Selection of Chemotherapy

Highlights from the “2012 ASCO Gastrointestinal Cancers Symposium”.
San Francisco, CA, USA. January 19-21, 2012

 

 

Richard Kim¹, Jennifer Byer², Muhammad Wasif Saif³

 

¹H. Lee Moffitt Cancer Center and ²University of South Florida. Tampa, FL, USA. ³Columbia University College of Physicians and Surgeons and New York Presbyterian Hospital. New York, NY, USA

 

 

Summary

Germline mutations in BRCA genes are associated with increased risk of pancreatic cancer. There are pre clinical data which suggests that DNA cross linking agents should be used in pancreatic cancer patients with BRCA mutations. This review is an update from the 2012 American Society of Clinical Oncology (ASCO) Gastrointestinal Cancers Symposium regarding recent developments in the treatment of pancreatic cancer with BRCA mutation. Only one study (Abstracts #217) was presented and it is described here.

 

Introduction

 

There are approximately 40,000 new cases of pancreatic adenocarcinoma diagnosed in the USA each year [1]. It is well known that germline mutation in the breast cancer, early onset (BRCA) 1 and BRCA2 tumor suppressor genes are associated with increased risk of ovarian and breast cancer [2]. In pancreatic cancer most of the cases are sporadic but it has been reported that patients with BRCA2 mutations have 3.5 fold increase risk of developing pancreatic cancer [3]. Past series have found incidence of BRCA2 mutation as high as 17% in pancreatic cancer patients with strong family history of pancreatic cancer [4]. The association between BRCA1 and pancreatic cancer is not well defined. However one series from Ashkenazi Jews showed that BRCA1 and BRCA2 mutations are observed with nearly equal distribution in pancreas cancer families, suggesting that both genes are associated with pancreatic cancer risk [5].

 

What Did We Learn at the 2012 American Society of Clinical Oncology (ASCO) GI Cancers Symposium?

 

Only one of the abstracts at the 2012 GI ASCO symposium dealt with BRCA mutation and pancreatic cancer (Abstract #217 [6]). Retrospective analysis by Tran et al. looked at Ontario Pancreatic Cancer Study and pharmacy databases and identified 5 patients with BRCA mutations (4 BRCA2 and 1 BRCA1) who were treated with platinum based regimen. It was a heterogeneous population as 3 patients received platinum based regimen for advanced disease while other 2 patients had resectable and locally advanced disease. Interestingly, patient with locally advanced disease (T4N0) were downstaged after receiving platinum based regimen and eventually underwent resection. The 3 metastatic patients had a very good response to platinum based regimen as well with progression free survival of 12 and 45 months in two of the patients.

 

Discussion

 

Patients with BRCA mutations are more susceptible certain drugs such as cisplatin or poly(ADP-ribose) polymerase (PARP) inhibitors.

Pre- clinical data suggest that platinum based regimen maybe effective in BRCA mutations at it exert their cytotoxic effect by binding directly to DNA, causing crosslinking of DNA strands and thereby inducing DNA double strand breaks. However, these damages can not repaired effectively due to lacking functioning BRCA1 or BRCA2 [7].

In breast cancer patients there are data to suggest that patients with BRCA mutations are more sensitive to DNA damaging agents such as platinum based regimen [8]. However, interestingly, in ovarian cancer it was found that BRCA2 mutation was more associated with response to platinum-based therapy when compared with BRCA1 mutation carriers [9]. In pancreatic cancer, in vitro data suggest that pancreatic cancers with BRCA2 mutations are more susceptible to DNA cross liking agents [10]. However, clinically this hypothesis is yet to be validated even though there are cases of patients responding to platinum based regimen after failing multiple lines of therapy [11, 12]. The Abstract #217 presented at the 2012 ASCO GI Cancers Symposium supports the further role of using platinum based regimen in pancreatic cancer with BRCA mutation. Even though the numbers were once again small there was evidence of activity of platinum based regimen in this highly selected subset of population.

PARP inhibitors are class of drugs which can induce cell death in tumors with mutations in certain DNA repair pathways such as the BRCA pathways of double-strand break repair [13]. Similarly to the platinum based regimen, PARP inhibitors were found to have activity in population enriched for BRCA1 and BRCA2 mutations [14]. In pancreas cancer, the largest series with BRCA mutations were published from the Memorial Sloan-Kettering Cancer Center, New York, NY, USA [15]. In this series, 15 patients with BRCA mutation pancreatic cancer were identified. Three of those patients received PARP inhibitors while 6 patients received platinum based regimen. The results were promising with median survival of 27.6 months including one patient with complete response which is rare in pancreatic cancer.

 

Conclusion

 

The incidence of BRCA mutations in pancreatic cancer is small. However, these subsets of patients are clinically important as they may potentially benefit from “targeted therapy”. The abstract presented at 2012 ASCO GI Cancers Symposium supports the hypothesis of using platinum based regimen in pancreatic cancer patients with BRCA mutations. However, the numbers are still very small and further prospective studies are need to be done to validate the potential use of platinum based regimen or PARP inhibitors in pancreatic cancer with BRCA mutations.

 

Key words Drug Therapy; Genes, BRCA1; Genes, BRCA2; Mutation; Pancreatic Neoplasms

 

Abbreviations PARP: poly(ADP-ribose) polymerase

 

Conflict of interest The authors have no potential conflicts of interest

 

Correspondence
Richard Kim
H. Lee Moffitt Cancer Center
12902 Magnolia Drive FOB-2
Tampa, FL 33612
Phone: +1-813.745.1277
Fax: +1-813.745.7229
E-mail: richard.kim@moffitt.org

 

References

1.    Jemal A, Siegel R, Xu J, Ward E. Cancer statistics, 2010. CA Cancer J Clin 2010;60:277-300. (More details: [1]).

2.    Narod SA, Foulkes WD. Brca1 and brca2: 1994 and beyond. Nat Rev Cancer 2004;4:665-76. (More details: [2]).

3.    Cancer risks in brca2 mutation carriers. The breast cancer linkage consortium. J Natl Cancer Inst 1999;91:1310-6. (More details: [3]).

4.    Murphy KM, Brune KA, Griffin C, Sollenberger JE, Petersen GM, Bansal R, et al. Evaluation of candidate genes map2k4, madh4, acvr1b, and brca2 in familial pancreatic cancer: Deleterious brca2 mutations in 17%. Cancer Res 2002;62:3789-93. (More details: [4]).

5.    Stadler ZK, Salo-Mullen E, Patil SM, Pietanza MC, Vijai J, Saloustros E, et al. Prevalence of brca1 and brca2 mutations in ashkenazi jewish families with breast and pancreatic cancer. Cancer 2012;118:493-9. (More details: [5]).

6.    Tran B MS, Zogopoulos G, Borgida A, Holter S, Gallinger S et al. Platinum-based chemotherapy (pt-chemo) in pancreatic adenocarcinoma (pc) associated with brca mutations: A translational case series. J Clin Oncol 2012;30:Abstract 217. (More details: [6]).

7.    McCabe N, Lord CJ, Tutt AN, Martin NM, Smith GC, Ashworth A. Brca2-deficient capan-1 cells are extremely sensitive to the inhibition of poly (adp-ribose) polymerase: An issue of potency. Cancer Biol Ther 2005;4:934-6. (More details: [7]).

8.    Byrski T, Gronwald J, Huzarski T, Grzybowska E, Budryk M, Stawicka M, et al. Pathologic complete response rates in young women with brca1-positive breast cancers after neoadjuvant chemotherapy. J Clin Oncol 2010;28:375-9. (More details: [8]).

9.    Yang D, Khan S, Sun Y, Hess K, Shmulevich I, Sood AK, et al. Association of brca1 and brca2 mutations with survival, chemotherapy sensitivity, and gene mutator phenotype in patients with ovarian cancer. JAMA 2011;306:1557-65. (More details: [9]).

10. van der Heijden MS, Brody JR, Dezentje DA, Gallmeier E, Cunningham SC, Swartz MJ, et al. In vivo therapeutic responses contingent on fanconi anemia/brca2 status of the tumor. Clin Cancer Res 2005;11:7508-15. (More details: [10]).

11. Chalasani P, Kurtin S, Dragovich T. Response to a third-line mitomycin c (mmc)-based chemotherapy in a patient with metastatic pancreatic adenocarcinoma carrying germline brca2 mutation. JOP 2008;9:305-8. (More details: [11]).

12. James E, Waldron-Lynch MG, Saif MW. Prolonged survival in a patient with brca2 associated metastatic pancreatic cancer after exposure to camptothecin: A case report and review of literature. Anti-Cancer Drugs 2009;20:634-8. (More details: [12]).

13. Farmer H, McCabe N, Lord CJ, Tutt ANJ, Johnson DA, Richardson TB, et al. Targeting the DNA repair defect in brca mutant cells as a therapeutic strategy. Nature 2005;434:917-21. (More details: [13]).

14. Fong PC, Boss DS, Yap TA, Tutt A, Wu PJ, Mergui-Roelvink M, et al. Inhibition of poly(adp-ribose) polymerase in tumors from brca mutation carriers. New England Journal of Medicine 2009;361:123-34. (More details: [14]).

15. Lowery MA, Kelsen DP, Stadler ZK, Yu KH, Janjigian YY, Ludwig E, et al. An emerging entity: Pancreatic adenocarcinoma associated with a known brca mutation: Clinical descriptors, treatment implications, and future directions. Oncologist 2011;16:1397-402. (More details: [15]).