| Literature DB >> 28139197 |
Janusz Franco-Barraza1, Ralph Francescone1, Tiffany Luong1, Neelima Shah1, Raj Madhani1, Gil Cukierman1, Essel Dulaimi2, Karthik Devarajan3, Brian L Egleston4, Emmanuelle Nicolas5, R Katherine Alpaugh6, Ruchi Malik1, Robert G Uzzo1,7, John P Hoffman7, Erica A Golemis4, Edna Cukierman1.
Abstract
Desmoplasia, a fibrotic mass including cancer-associated fibroblasts (CAFs) and self-sustaining extracellular matrix (D-ECM), is a puzzling feature of pancreatic ductal adenocarcinoma (PDACs). Conflicting studies have identified tumor-restricting and tumor-promoting roles of PDAC-associated desmoplasia, suggesting that individual CAF/D-ECM protein constituents have distinguishable tumorigenic and tumor-repressive functions. Using 3D culture of normal pancreatic versus PDAC-associated human fibroblasts, we identified a CAF/D-ECM phenotype that correlates with improved patient outcomes, and that includes CAFs enriched in plasma membrane-localized, active α5β1-integrin. Mechanistically, we established that TGFβ is required for D-ECM production but dispensable for D-ECM-induced naïve fibroblast-to-CAF activation, which depends on αvβ5-integrin redistribution of pFAK-independent active α5β1-integrin to assorted endosomes. Importantly, the development of a simultaneous multi-channel immunofluorescence approach and new algorithms for computational batch-analysis and their application to a human PDAC panel, indicated that stromal localization and levels of active SMAD2/3 and α5β1-integrin distinguish patient-protective from patient-detrimental desmoplasia and foretell tumor recurrences, suggesting a useful new prognostic tool.Entities:
Keywords: alpha5beta1 integrin; alphavbeta5 integrin; cancer biology; cancer-associated fibroblasts; desmoplasia; extracellular matrix; human; human biology; medicine; mouse; myofibroblasts; pancreatic ductal adenocarcinoma
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Year: 2017 PMID: 28139197 PMCID: PMC5283834 DOI: 10.7554/eLife.20600
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140