4.4 Article

Distinct Recycling of Active and Inactive ß1 Integrins

Journal

TRAFFIC
Volume 13, Issue 4, Pages 610-625

Publisher

WILEY-BLACKWELL
DOI: 10.1111/j.1600-0854.2012.01327.x

Keywords

conformation; endocytosis; integrin; recycling; trafficking

Categories

Funding

  1. Academy of Finland
  2. ERC
  3. Sigrid Juselius Foundation
  4. Finnish Cancer Organizations
  5. V-S cultural foundation
  6. Ida Montin foundation
  7. Orion-Farmos foundation
  8. K. Albin Johanssons foundation
  9. Instrumentarium foundation
  10. Alexander von Humboldt foundation
  11. EMBO
  12. Turku Graduate School for Biomedical Sciences

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Integrin trafficking plays an important role in cellular motility and cytokinesis. Integrins undergo constant endo/exocytic shuttling to facilitate the dynamic regulation of cell adhesion. Integrin activity toward the components of the extracellular matrix is regulated by the ability of these receptors to switch between active and inactive conformations. Several cellular signalling pathways have been described in the regulation of integrin traffic under different conditions. However, the interrelationship between integrin activity conformations and their endocytic fate have remained incompletely understood. Here, we have investigated the endocytic trafficking of active and inactive beta 1 integrins in cancer cells. Both conformers are endocytosed in a clathrin- and dynamin-dependent manner. The net endocytosis rate of the active beta 1 integrins is higher, whereas endocytosis of the inactive beta 1 integrin is counteracted by rapid recycling back to the plasma membrane via an ARF6- and early endosome antigen 1-positive compartment in an Rab4a- and actin-dependent manner. Owing to these distinct trafficking routes, the two receptor pools display divergent subcellular localization. At steady state, the inactive beta 1 integrin is mainly on the plasma membrane, whereas the active receptor is predominantly intracellular. These data provide new insights into the endocytic traffic of integrins and imply the possibility of a previously unappreciated crosstalk between pathways regulating integrin activity and traffic.

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