Beta 1-integrin-c-Met cooperation reveals an inside-in survival signalling on autophagy-related endomembranes.
Rachel Barrow-McGeeNaoki KishiCarine JoffreLudovic MénardAlexia HervieuBakhouche A BakhoucheAlejandro J NovalAnja MaiCamilo GuzmánLuisa Robbez-MassonXavier IturriozJames HulitCaroline H BrennanIan R HartPeter J ParkerJohanna IvaskaStéphanie KermorgantPublished in: Nature communications (2016)
Receptor tyrosine kinases (RTKs) and integrins cooperate to stimulate cell migration and tumour metastasis. Here we report that an integrin influences signalling of an RTK, c-Met, from inside the cell, to promote anchorage-independent cell survival. Thus, c-Met and β1-integrin co-internalize and become progressively recruited on LC3B-positive 'autophagy-related endomembranes' (ARE). In cells growing in suspension, β1-integrin promotes sustained c-Met-dependent ERK1/2 phosphorylation on ARE. This signalling is dependent on ATG5 and Beclin1 but not on ATG13, suggesting ARE belong to a non-canonical autophagy pathway. This β1-integrin-dependent c-Met-sustained signalling on ARE supports anchorage-independent cell survival and growth, tumorigenesis, invasion and lung colonization in vivo. RTK-integrin cooperation has been assumed to occur at the plasma membrane requiring integrin 'inside-out' or 'outside-in' signalling. Our results report a novel mode of integrin-RTK cooperation, which we term 'inside-in signalling'. Targeting integrin signalling in addition to adhesion may have relevance for cancer therapy.
Keyphrases
- cell migration
- cell adhesion
- cancer therapy
- signaling pathway
- cell death
- tyrosine kinase
- endoplasmic reticulum stress
- stem cells
- mass spectrometry
- drug delivery
- mesenchymal stem cells
- cell proliferation
- escherichia coli
- single cell
- cell therapy
- bone marrow
- preterm infants
- protein kinase
- liquid chromatography
- preterm birth
- solid phase extraction