Streptozotocin (STZ)-based chemotherapy is the first-line chemotherapy recommended for advanced pancreatic neuroendocrine tumors (pNETs), while targeted therapies, including mTOR inhibitors, are available in second-line treatment. Unfortunately objective response rates to both treatments are limited. Since mTOR pathway activation, commonly observed in pNETs, has been reported as one of the major mechanisms accounting for chemoresistance, we investigated the potential benefit of mTOR inhibition combined with STZ treatment in a subset of pNETs, namely insulinomas. To evaluate the potential of mTOR inhibition in combination with STZ, we selected four different inhibitors acting at various levels of the pathway (everolimus: inhibition of mTORC1, MK-2206: inhibition of AKT, BKM120: inhibition of PI3K, mTORC1 and mTORC2, and BEZ235: inhibition of mTORC1 and mTORC2). Effects on cell viability and apoptosis were assessed in insulinoma cell lines INS-1E (rat) and MIN6 (mouse) in vitro and were confirmed in vivo by using a mouse model of hepatic tumor dissemination after intrasplenic xenograft. In vitro, all four combinations display synergistic effects. These combinations lead to heterogeneous mTOR pathway inhibition, in agreement with their respective target, and increased apoptosis. In vivo, tumor growth in the liver was significantly inhibited by combining STZ with everolimus (P=0.0014), BKM120 (P=0.0092) or BEZ235 (P=0.008) as compared to each agent alone. These results suggest that targeting the mTOR pathway in combination with STZ could be of potential benefit for insulinomas and pNET patients and thus support further clinical investigations.
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