Mechanical force regulates integrin turnover in Drosophila in vivo

Author:  ["Mary Pines","Raibatak Das","Stephanie J. Ellis","Alexander Morin","Stefan Czerniecki","Lin Yuan","Markus Klose","Daniel Coombs","Guy Tanentzapf"]

Publication:  Nature Cell Biology

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Tags:  Integrins   Mechanotransduction   Biological

Abstract

Tanentzapf and colleagues use genetic mutations that alter tensile force at the Drosophila myotendinous junction to demonstrate that mechanical force controls in vivo turnover of integrin and intracellular adhesion complexes. Regulated assembly and disassembly, or turnover, of integrin-mediated cell–extracellular matrix (ECM) adhesions is essential for dynamic cell movements and long-term tissue maintenance. For example, in Drosophila, misregulation of integrin turnover disrupts muscle–tendon attachment at myotendinous junctions (MTJs). We demonstrate that mechanical force, which modulates integrin activity, also regulates integrin and intracellular adhesion complex (IAC) turnover in vivo. Using conditional mutants to alter the tensile force on MTJs, we found that the proportion of IAC components undergoing turnover inversely correlated with the force applied on MTJs. This effect was disrupted by point mutations in β-integrin that interfere with ECM-induced conformational changes and activation of β-integrin or integrin-mediated cytoplasmic signalling. These mutants also disrupted integrin dynamics at MTJs during larval development. Together, these data suggest that specific β-integrin-mediated signals regulate adhesion turnover in response to tension during tissue formation. We propose that integrin–ECM adhesive stability is continuously controlled by force in vivo through integrin-dependent auto-regulatory feedback mechanisms so that tissues can quickly adapt to and withstand mechanical stresses.

Cite this article

Pines, M., Das, R., Ellis, S. et al. Mechanical force regulates integrin turnover in Drosophila in vivo. Nat Cell Biol 14, 935–943 (2012). https://doi.org/10.1038/ncb2555

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