MicroRNA-135b Promotes Cancer Progression by Acting as a Downstream Effector of Oncogenic Pathways in Colon Cancer.

Valeri, N; Braconi, C; Gasparini, P; Murgia, C; Lampis, A; Paulus Hock, V; Hart, Jr; Ueno, L; Grivennikov, Si; Lovat, F; Paone, A; Cascione, L; Sumani, Km; Veronese, A; Fabbri, M; Carasi, S; Alder, H; Lanza, G; Gafa', R; Moyer, Mp; Ridgway, Ra; Cordero, J; Nuovo, Gj; Frankel, Wl; Rugge, Massimo; Fassan, Matteo; Groden, J; Vogt, Pk; Karin, M; Sansom, Oj; Croce, Cm

doi:10.1016/j.ccr.2014.03.006

MicroRNA deregulation is frequent in human colorectal cancers (CRCs), but little is known as to whether it represents a bystander event or actually drives tumor progression in vivo. We show that miR-135b overexpression is triggered in mice and humans by APC loss, PTEN/PI3K pathway deregulation, and SRC overexpression and promotes tumor transformation and progression. We show that miR-135b upregulation is common in sporadic and inflammatory bowel disease-associated human CRCs and correlates with tumor stage and poor clinical outcome. Inhibition of miR-135b in CRC mouse models reduces tumor growth by controlling genes involved in proliferation, invasion, and apoptosis. We identify miR-135b as a key downsteam effector of oncogenic pathways and a potential target for CRC treatmen