Endosomes: Emerging Platforms for Integrin-Mediated FAK Signalling

Integrins are vital cell adhesion receptors with the ability to transmit extracellular matrix (ECM) cues to intracellular signalling pathways. ECM–integrin signalling regulates various cellular functions such as cell survival and movement. Integrin signalling has been considered to occur exclusively from adhesion sites at the plasma membrane (PM). However, recent data demonstrates integrin signalling also from endosomes. Integrin-mediated focal adhesion kinase (FAK) signalling is strongly dependent on integrin endocytosis, and endosomal FAK signalling facilitates cancer metastasis by supporting anchorage-independent growth and anoikis resistance. Here we discuss the possible mechanisms and functions of endosomal FAK signalling compared with its previously known roles in other cellular locations and discuss the potential of endosomal FAK as novel target for future cancer therapies.

TrendsActive integrins signal from endosomes to activate focal adhesion kinase (FAK).Integrin endosomal signalling contributes to FAK-dependent anoikis suppression.Integrin trafficking is thoroughly linked to cellular signalling.FAK targeting to endosomes is distinct from focal adhesion recruitment.Signalling from integrin-containing ‘endoadhesomes’ supports cancer metastasis.