Caveolin-1 is Associated with Tumor Progression and Confers a Multi-Modality Resistance Phenotype in Pancreatic Cancer

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作者
Moumita Chatterjee
Edgar Ben-Josef
Dafydd G. Thomas
Meredith A. Morgan
Mark M. Zalupski
Gazala Khan
Charles Andrew Robinson
Kent A. Griffith
Ching-Shih Chen
Thomas Ludwig
Tanios Bekaii-Saab
Arnab Chakravarti
Terence M. Williams
机构
[1] The Ohio State University Medical Center,
[2] Arthur G. James Comprehensive Cancer Center and Richard J. Solove Research Institute,undefined
[3] Hospital of the University of Pennsylvania,undefined
[4] University of Michigan Medical Center,undefined
[5] Henry Ford Hospital System,undefined
[6] West Bloomfield,undefined
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Caveolin-1 (Cav-1) is a 21 kDa protein enriched in caveolae and has been implicated in oncogenic cell transformation, tumorigenesis and metastasis. We explored roles for Cav-1 in pancreatic cancer (PC) prognostication, tumor progression, resistance to therapy and whether targeted downregulation could lead to therapeutic sensitization. Cav-1 expression was assessed in cell lines, mouse models and patient samples and knocked down in order to compare changes in proliferation, invasion, migration, response to chemotherapy and radiation and tumor growth. We found Cav-1 is overexpressed in human PC cell lines, mouse models and human pancreatic tumors and is associated with worse tumor grade and clinical outcomes. In PC cell lines, disruption/depletion of caveolae/Cav-1 reduces proliferation, colony formation and invasion. Radiation and chemotherapy up-regulate Cav-1 expression, while Cav-1 depletion induces both chemosensitization and radiosensitization through altered apoptotic and DNA repair signaling. In vivo, Cav-1 depletion significantly attenuates tumor initiation and growth. Finally, Cav-1 depletion leads to altered JAK/STAT, JNK and Src signaling in PC cells. Together, higher Cav-1 expression is correlated with worse outcomes, is essential for tumor growth and invasion (both in vitro and in vivo), is responsible for promoting resistance to therapies and may serve as a prognostic/predictive biomarker and target in PC.
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