PIP₃abundance overcomes PI3K signaling selectivity in invadopodia

Abstract: PI3Kβ is required for invadopodia‐mediated matrix degradation by breast cancer cells. Invadopodia maturation requires GPCR activation of PI3Kβ and its coupling to SHIP2 to produce PI(3,4)P2. We now test whether selectivity for PI3Kβ is preserved under conditions of mutational increases in PI3K activity. In breast cancer cells where PI3Kβ is inhibited, short‐chain diC8‐PIP3 rescues gelatin degradation in a SHIP2‐dependent manner; rescue by diC8‐PI(3,4)P2 is SHIP2‐independent. Surprisingly, the expression of eit… Show more