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Molecular Characterization of KRAS Wild-type Tumors in Patients with Pancreatic Adenocarcinoma

Authors :
Philip, Philip A
Azar, Ibrahim
Xiu, Joanne
Hall, Michael J
Hendifar, Andrew Eugene
Lou, Emil
Hwang, Jimmy J
Gong, Jun
Feldman, Rebecca
Ellis, Michelle
Stafford, Phil
Spetzler, David
Khushman, Moh'd M
Sohal, Davendra
Lockhart, A Craig
Weinberg, Benjamin A
El-Deiry, Wafik S
Marshall, John
Shields, Anthony F
Korn, W Michael
Source :
Clinical cancer research : an official journal of the American Association for Cancer Research, vol 28, iss 12
Publication Year :
2022
Publisher :
eScholarship, University of California, 2022.

Abstract

PurposeKRAS mutation (MT) is a major oncogenic driver in pancreatic ductal adenocarcinoma (PDAC). A small subset of PDACs harbor KRAS wild-type (WT). We aim to characterize the molecular profiles of KRAS WT PDAC to uncover new pathogenic drivers and offer targeted treatments.Experimental designTumor tissue obtained from surgical or biopsy material was subjected to next-generation DNA/RNA sequencing, microsatellite instability (MSI) and mismatch repair status determination.ResultsOf the 2,483 patients (male 53.7%, median age 66 years) studied, 266 tumors (10.7%) were KRAS WT. The most frequently mutated gene in KRAS WT PDAC was TP53 (44.5%), followed by BRAF (13.0%). Multiple mutations within the DNA-damage repair (BRCA2, ATM, BAP1, RAD50, FANCE, PALB2), chromatin remodeling (ARID1A, PBRM1, ARID2, KMT2D, KMT2C, SMARCA4, SETD2), and cell-cycle control pathways (CDKN2A, CCND1, CCNE1) were detected frequently. There was no statistically significant difference in PD-L1 expression between KRAS WT (15.8%) and MT (17%) tumors. However, KRAS WT PDAC were more likely to be MSI-high (4.7% vs. 0.7%; P < 0.05), tumor mutational burden-high (4.5% vs. 1%; P < 0.05), and exhibit increased infiltration of CD8+ T cells, natural killer cells, and myeloid dendritic cells. KRAS WT PDACs exhibited gene fusions of BRAF (6.6%), FGFR2 (5.2%), ALK (2.6%), RET (1.3%), and NRG1 (1.3%), as well as amplification of FGF3 (3%), ERBB2 (2.2%), FGFR3 (1.8%), NTRK (1.8%), and MET (1.3%). Real-world evidence reveals a survival advantage of KRAS WT patients in overall cohorts as well as in patients treated with gemcitabine/nab-paclitaxel or 5-FU/oxaliplatin.ConclusionsKRAS WT PDAC represents 10.7% of PDAC and is enriched with targetable alterations, including immuno-oncologic markers. Identification of KRAS WT patients in clinical practice may expand therapeutic options in a clinically meaningful manner.

Details

Database :
OpenAIRE
Journal :
Clinical cancer research : an official journal of the American Association for Cancer Research, vol 28, iss 12
Accession number :
edsair.od.......325..eaafc85abbe37805926f1b8f8a8bebee