LWBK1006-20 LWW-Govindan-Review December 12, 2011 19:4
246 DeVita, Hellman, and Rosenberg’s CANCER: Principles and Practice of Oncology ReviewQuestion 20.2.10.Mutation of which tumor suppressor gene is most frequently associated
with familial pancreatic cancer?
A. BRCA2
B. PALB2
C. K-RAS
D. TP53Question 20.2.11.Which of the following statements regarding risk factors for pancreatic
cancer is CORRECT?
A. ABO blood group is associated with increased risk for pancreatic
cancer.
B. Testing for K-RAS mutations in the pancreatic juice of patients is an
effective screening test for pancreatic cancer in high risk patients.
C. Patients with hereditary nonpolyposis colorectal cancer syndrome do
not have an increased risk for pancreatic cancer.
D. Hereditary pancreatitis is not a significant risk factor for pancreatic
cancer.Question 20.2.12.A 65-year-old male was diagnosed with metastatic pancreatic cancer and
received treatment with single-agent gemcitabine. However, he now has
disease progression and is interested in pursuing systemic therapy. Which
of the following could be considered as a second-line treatment choice?
A. FOLFOX6
B. Erlotinib
C. Paclitaxel
D. Irinotecan and raltitrexedQuestion 20.2.13.Which of the following is true about pancreatic cancer?
A. Most pancreatic cancers have mutations in KRAS, TP53, SMAD4,
p16/CDKN2A.
B. Telomere shortening is the earliest and most prevalent genetic change
identified in the precursor lesions.
C. Underexpression of TGF-is observed in few pancreatic cancers.
D. p16-mediated CDK inhibition is a protective mechanism against pan-
creatic cancer.
E. All of above.