Genetics and biology of pancreatic ductal adenocarcinoma

Author:

Ying Haoqiang,Dey Prasenjit,Yao Wantong,Kimmelman Alec C.,Draetta Giulio F.,Maitra AnirbanORCID,DePinho Ronald A.

Abstract

With 5-year survival rates remaining constant at 6% and rising incidences associated with an epidemic in obesity and metabolic syndrome, pancreatic ductal adenocarcinoma (PDAC) is on track to become the second most common cause of cancer-related deaths by 2030. The high mortality rate of PDAC stems primarily from the lack of early diagnosis and ineffective treatment for advanced tumors. During the past decade, the comprehensive atlas of genomic alterations, the prominence of specific pathways, the preclinical validation of such emerging targets, sophisticated preclinical model systems, and the molecular classification of PDAC into specific disease subtypes have all converged to illuminate drug discovery programs with clearer clinical path hypotheses. A deeper understanding of cancer cell biology, particularly altered cancer cell metabolism and impaired DNA repair processes, is providing novel therapeutic strategies that show strong preclinical activity. Elucidation of tumor biology principles, most notably a deeper understanding of the complexity of immune regulation in the tumor microenvironment, has provided an exciting framework to reawaken the immune system to attack PDAC cancer cells. While the long road of translation lies ahead, the path to meaningful clinical progress has never been clearer to improve PDAC patient survival.

Funder

Sheikh Ahmed Center for Pancreatic Cancer Research

Pancreatic Cancer Moon Shot at the University of Texas MD Anderson Cancer Center

University of Texas Star Award

Department of Defense

Odyssey Fellowship

University of Texas MD Anderson Cancer Center

American Cancer Society

National Institutes of Health

American Association for Cancer Research

Publisher

Cold Spring Harbor Laboratory

Subject

Developmental Biology,Genetics

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