Identifying Actionable Alterations in KRAS Wild-Type Pancreatic Cancer

Overview

Journal Target Oncol

Specialty Oncology

Date 2024 Aug 9

PMID 39123077

Authors

Ahmed Elhariri

Jaydeepbhai Patel

Himil Mahadevia

Douaa Albelal

Ahmed K Ahmed

Jeremy C Jones

Mitesh J Borad

Hani Babiker

Affiliations

Soon will be listed here.

Abstract

The 5-year relative survival rate for pancreatic cancer is currently the lowest among all cancer types with a dismal 13%. A Kirsten rat sarcoma virus (KRAS) gene mutation is present in approximately 90% of patients with pancreatic cancer; however, KRAS-specific drugs are not yet widely used in clinical practice for pancreatic cancer, specifically the KRAS variant. Advances in genomic testing revealed an opportunity to detect genetic alterations in a subset of patients with no KRAS mutation termed KRAS wild-type. Patients with KRAS wild-type tumors have a propensity to express driver alterations, hence paving the way for utilizing a targeted therapy approach either via clinical trials or standard-of-care drugs. These alterations include fusions, amplifications, translocations, rearrangements and microsatellite instability-high tumors and can be as high as 11% in some studies. Here, we discuss some of the most notable alterations in KRAS wild-type and highlight promising clinical trials.

Citing Articles

PARP Inhibitors in Pancreatic Cancer with Homologous Recombination Repair Gene Mutations: A Single-Institution Experience.

Miao R, Blue K, Sommerer K, Shah A, Bottiglieri S, Cueto A Cancers (Basel). 2024; 16(20).

PMID: 39456541 PMC: 11505755. DOI: 10.3390/cancers16203447.

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