Apoptosis of adherent cells by recruitment of caspase-8 to unligated integrins

Author:

Stupack Dwayne G.1,Puente Xose S.1,Boutsaboualoy Souphaphone1,Storgard Chris M.1,Cheresh David A.1

Affiliation:

1. Department of Immunology and Department of Vascular Biology, The Scripps Research Institute, La Jolla, CA 92037

Abstract

Integrin-mediated adhesion promotes cell survival in vitro, whereas integrin antagonists induce apoptosis of adherent cells in vivo. Here, we demonstrate that cells adherent within a three-dimensional extracellular matrix undergo apoptosis due to expression of unligated integrins, the β subunit cytoplasmic domain, or its membrane proximal sequence KLLITIHDRKEF. Integrin-mediated death requires initiator, but not stress, caspase activity and is distinct from anoikis, which is caused by the loss of adhesion per se. Surprisingly, unligated integrin or β integrin tails recruit caspase-8 to the membrane, where it becomes activated in a death receptor–independent manner. Integrin ligation disrupts this integrin–caspase containing complex and increases survival, revealing an unexpected role for integrins in the regulation of apoptosis and tissue remodeling.

Publisher

Rockefeller University Press

Subject

Cell Biology

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