Citation

  • Authors: Shitomi, Y., Thogersen, I. B., Ito, N., Leitinger, B., Enghild, J. J., Itoh, Y.
  • Year: 2015
  • Journal: Mol Biol Cell 26 659-73
  • Applications: in vitro / siRNA / INTERFERin
  • Cell types:
    1. Name: A431
    2. Name: HEK-293
      Description: Human embryonic kidney Fibroblast
      Known as: HEK293, 293

Method

Transfections were performed in 24-well plates (3.5 × 10^4 cells/well for A431 , 2.5 × 104 cells/well for HEK-293) together with 20 nM siRNA using 3 μl of INTERFERin in a total reaction volume of 0.6 ml/well (reverse transfection protocol).

Abstract

Discoidin domain receptor 1 (DDR1) is a receptor tyrosine kinase that binds and transmits signals from various collagens in epithelial cells. However, how DDR1-dependent signaling is regulated has not been understood. Here we report that collagen binding induces ADAM10-dependent ectodomain shedding of DDR1. DDR1 shedding is not a result of an activation of its signaling pathway, since DDR1 mutants defective in signaling were shed in an efficient manner. DDR1 and ADAM10 were found to be in a complex on the cell surface, but shedding did not occur unless collagen bound to DDR1. Using a shedding-resistant DDR1 mutant, we found that ADAM10-dependent DDR1 shedding regulates the half-life of collagen-induced phosphorylation of the receptor. Our data also revealed that ADAM10 plays an important role in regulating DDR1-mediated cell adhesion to achieve efficient cell migration on collagen matrices.

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