Precision medicine in pancreatic cancer: treating every patient as an exception
- PMID: 31511204
- PMCID: PMC9516437
- DOI: 10.1016/S2468-1253(19)30175-X
Precision medicine in pancreatic cancer: treating every patient as an exception
Abstract
Patients with pancreatic cancer have not benefited from recent improvements in overall survival brought about by precision medicine in other malignancies. This failure is not due to a dearth of precision-medicine research in pancreatic ductal adenocarcinoma (PDAC), the main type of pancreatic cancer. In fact, the stalled progress in precision therapies for this type of cancer is due to the absence of agents that are able to target the common genetic alterations in PDAC. Several studies have attempted to phenotypically stratify PDAC at the transcriptional level. However, the value of such classifications will only be revealed through prospective studies and, crucially, only after development of new treatment options for this disease. Therefore, it is essential to learn from breakthrough discoveries in other cancer types that could benefit subpopulations of patients with PDAC and convert them from ordinary to exceptional responders. Identifying these exceptional patients will help to bring PDAC in line with other cancer types in terms of availability of precision therapies. Thus, the true challenge to precision medicine for PDAC might be the poor consensus on which genetic and phenotypic alterations across the spectrum of this disease are actionable; not the absence of actionable variables themselves. To reach consensus, knowledge and tools must be developed and disseminated for individuals who provide pancreatic cancer care, to enable the real-time identification of exceptional patients, more precise subgroup classifications, and effective disease management strategies; all informed by immediate feedback from clinical outcome data.
Copyright © 2019 Elsevier Ltd. All rights reserved.
Conflict of interest statement
Declaration of interests
LZ reports grants from Bristol-Myers Squibb, Merck, iTeos, Amgen, Gradalis, and Halozyme; personal fees from Merck, AstraZeneca, Oncorus, Alphamab, Sound Biologics, Biosion, Fosun Biopharmaceutical, Foundation Medicine, and Mingruizhiyao; and shares from Alphamab (a biopharmaceutical not currently in the field of pancreatic cancer drug development) and Mingruizhiyao (a contracted preclinical research provider that does not have its own research and development). LZ has a patent for Annexin A2 as a pancreatic cancer target pending, a patent for Sema3D/PlexinD1 as a pancreatic cancer target pending, a patent for vaccine in combination with immune checkpoint inhibitors as cancer treatment strategy pending, a patent for vaccine in combination with IDO inhibitor as cancer treatment strategy pending, and a patent for colon cancer GVAX vaccine with royalties paid. BH declares no competing interests.
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