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TGF-β and αvβ6 integrin act in a common pathway to suppress pancreatic cancer progression.

Cancer research (2012-07-13)
Aram F Hezel, Vikram Deshpande, Stephanie M Zimmerman, Gianmarco Contino, Brinda Alagesan, Michael R O'Dell, Lee B Rivera, Jay Harper, Scott Lonning, Rolf A Brekken, Nabeel Bardeesy
RÉSUMÉ

The TGF-β pathway is under active consideration as a cancer drug target based on its capacity to promote cancer cell invasion and to create a protumorigenic microenvironment. However, the clinical application of TGF-β inhibitors remains uncertain as genetic studies show a tumor suppressor function of TGF-β in pancreatic cancer and other epithelial malignancies. Here, we used genetically engineered mouse models to investigate the therapeutic impact of global TGF-β inhibition in pancreatic cancer in relation to tumor stage, genetic profile, and concurrent chemotherapy. We found that αvβ6 integrin acted as a key upstream activator of TGF-β in evolving pancreatic cancers. In addition, TGF-β or αvβ6 blockade increased tumor cell proliferation and accelerated both early and later disease stages. These effects were dependent on the presence of Smad4, a central mediator of TGF-β signaling. Therefore, our findings indicate that αvβ6 and TGF-β act in a common tumor suppressor pathway whose pharmacologic inactivation promotes pancreatic cancer progression.

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Anticorps anti-protéoglycane NG2 de type sulfate de chondroïtine, Chemicon®, from rabbit