Deleterious Germline Mutations in Patients With Apparently Sporadic Pancreatic Adenocarcinoma

Author:

Shindo Koji1,Yu Jun1,Suenaga Masaya1,Fesharakizadeh Shahriar1,Cho Christy1,Macgregor-Das Anne1,Siddiqui Abdulrehman1,Witmer P. Dane1,Tamura Koji1,Song Tae Jun1,Navarro Almario Jose Alejandro1,Brant Aaron1,Borges Michael1,Ford Madeline1,Barkley Thomas1,He Jin1,Weiss Matthew J.1,Wolfgang Christopher L.1,Roberts Nicholas J.1,Hruban Ralph H.1,Klein Alison P.1,Goggins Michael1

Affiliation:

1. All authors: The Sol Goldman Pancreatic Cancer Research Center, Johns Hopkins University, Baltimore, MD.

Abstract

Purpose Deleterious germline mutations contribute to pancreatic cancer susceptibility and are well documented in families in which multiple members have had pancreatic cancer. Methods To define the prevalence of these germline mutations in patients with apparently sporadic pancreatic cancer, we sequenced 32 genes, including known pancreatic cancer susceptibility genes, in DNA prepared from normal tissue obtained from 854 patients with pancreatic ductal adenocarcinoma, 288 patients with other pancreatic and periampullary neoplasms, and 51 patients with non-neoplastic diseases who underwent pancreatic resection at Johns Hopkins Hospital between 2000 and 2015. Results Thirty-three (3.9%; 95% CI, 3.0% to 5.8%) of 854 patients with pancreatic cancer had a deleterious germline mutation, 31 (3.5%) of which affected known familial pancreatic cancer susceptibility genes: BRCA2 (12 patients), ATM (10 patients), BRCA1 (3 patients), PALB2 (2 patients), MLH1 (2 patients), CDKN2A (1 patient), and TP53 (1 patient). Patients with these germline mutations were younger than those without (mean ± SD, 60.8 ± 10.6 v 65.1 ± 10.5 years; P = .03). Deleterious germline mutations were also found in BUB1B (1) and BUB3 (1). Only three of these 33 patients had reported a family history of pancreatic cancer, and most did not have a cancer family history to suggest an inherited cancer syndrome. Five (1.7%) of 288 patients with other periampullary neoplasms also had a deleterious germline mutation. Conclusion Germline mutations in pancreatic cancer susceptibility genes are commonly identified in patients with pancreatic cancer without a significant family history of cancer. These deleterious pancreatic cancer susceptibility gene mutations, some of which are therapeutically targetable, will be missed if current family history guidelines are the main criteria used to determine the appropriateness of gene testing.

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

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