Document Type
Article
Publication Date
6-30-2015
Abstract
Pancreatic ductal adenocarcinoma (PDA) harbors an exceedingly poor prognosis, and is generally considered a therapy-recalcitrant disease due to poor response to conventional chemotherapy coupled with non-actionable genetic drivers (e.g. KRAS mutations). However, PDA frequently loses p16ink4a, thereby leading to deregulation of CDK4/6. Surprisingly, in established cell models and xenografts, CDK4/6 inhibition has a modest effect on proliferation and resistance develops rapidly. To determine if such weak response was an intrinsic feature of PDA, we developed primary tumor explants that maintain the tumor environment and recapitulate feuture of primary PDA. The CDK4/6 inhibitor PD-0332991 was highly efficient at suppressing proliferation in 14 of the 15 explants. In the single resistant explant, we identified the rare loss of the RB tumor suppressor as the basis for resistance. Patient-derived xenografts (PDXs) were developed in parallel, and unlike the xenografts emerging from established cell lines, the PDXs maintained the histoarchitecture of the primary tumor. These PDXs were highly sensitive to CDK4/6 inhibition, yielding a complete suppression of PDA proliferation. Together, these data indicate that primary PDA is sensitive to CDK4/6 inhibition, that specific biomarkers can delineate intrinsic resistance, and that established cell line models may not represent an adequate means for evaluating therapeutic sensitivities.
Recommended Citation
Witkiewicz, Agnieszka K; Borja, Nicholas A; Franco, Jorge; Brody, MD, Jonathan; Yeo, Charles; Mansour, John; Choti, Michael A; McCue, Peter; and Knudsen, Erik S, "Selective impact of CDK4/6 suppression on patient-derived models of pancreatic cancer." (2015). Department of Pathology, Anatomy, and Cell Biology Faculty Papers. Paper 169.
https://jdc.jefferson.edu/pacbfp/169
PubMed ID
26158861
Comments
This article has been peer reviewed. It was published in: Oncotarget.
Volume 6, Issue 18, 2015, Pages 15788-15801.
The published version is available at http://www.impactjournals.com/oncotarget/index.php?journal=oncotarget&page=article&op=view&path[]=3819&pubmed-linkout=1
Copyright © 2015 the authors