Fig. 1

Antitumor activity of the combination of PTX, bevacizumab and MEK162 in MNHOC124 PDX model. Xenograft MNHOC124 was transplanted subcutaneously and when tumor masses reached 100-150mg, mice were randomized to receive vehicle (CTR,-♦-), or bevacizumab and MEK162 (BEV/MEK,-■-), paclitaxel and MEK162 (PTX/MEK,-▲-), paclitaxel and bevacizumab (PTX/BEV, -●-), or paclitaxel and bevacizumab and MEK162 (PTX/BEV/MEK,-x-). Data are the mean ± SE of tumor masses, as described in Materials and Methods; each group consisted of 8-10 mice