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Novel mode of action of c-kit tyrosine kinase inhibitors leading to NK cell-dependent antitumor effects |
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| Authors: | Borg Christophe Terme Magali Taïeb Julien Ménard Cédric Flament Caroline Robert Caroline Maruyama Koji Wakasugi Hiro Angevin Eric Thielemans Kris Le Cesne Axel Chung-Scott Véronique Lazar Vladimir Tchou Isabelle Crépineau Florent Lemoine François Bernard Jacky Fletcher Jonhantan A Turhan Ali Blay Jean-Yves Spatz Alain Emile Jean-François Heinrich Michael C Mécheri Salah Tursz Thomas Zitvogel Laurence |
| Affiliation: | Department of Clinical Biology, Equipe de Recherche Mixte 0208, INSERM, Institut Gustave Roussy, Villejuif, France. |
| Abstract: | Mutant isoforms of the KIT or PDGF receptors expressed by gastrointestinal stromal tumors (GISTs) are considered the therapeutic targets for STI571 (imatinib mesylate; Gleevec), a specific inhibitor of these tyrosine kinase receptors. Case reports of clinical efficacy of Gleevec in GISTs lacking the typical receptor mutations prompted a search for an alternate mode of action. Here we show that Gleevec can act on host DCs to promote NK cell activation. DC-mediated NK cell activation was triggered in vitro and in vivo by treatment of DCs with Gleevec as well as by a loss-of-function mutation of KIT. Therefore, tumors that are refractory to the antiproliferative effects of Gleevec in vitro responded to Gleevec in vivo in an NK cell-dependent manner. Longitudinal studies of Gleevec-treated GIST patients revealed a therapy-induced increase in IFN-gamma production by NK cells, correlating with an enhanced antitumor response. These data point to a novel mode of antitumor action for Gleevec. |
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