We identified miR-21 and miR-224 as cell-specific and compartment-specific regulators in PanINs and PDA.  miR-21 is overexpressed in tumor epithelial cells of premalignant ducts, while miR-224 is overexpressed in cancer-associated fibroblasts in PDA stroma.  Inhibition of miR-21 reverted pro-tumorigenic functionalities to baseline levels.  Overexpression of miR-224 induced activated phenotypes in normal fibroblasts.  miR-21 inhibition downregulated MAPK, mTOR and actin cytoskeleton pathways downstream of KRAS activation in tumor cells.  In vivo miR-21 inhibition improved survival in established PDA, while early systemic miR-21 inhibition intercepted premalignant progression. SOURCE: Jacquelyn,W,Zimmerman (jzimme27@jhmi.edu, jackiezimm133@gmail.com) -  Johns Hopkins Sidney Kimmel Comp. Cancer Center

Pluto Bioinformatics

GSE143326: Inhibition of miR-21 regulates mutant KRAS effector pathways and intercepts pancreatic ductal adenocarcinoma development