eLife (Jun 2014)

Symmetric exchange of multi-protein building blocks between stationary focal adhesions and the cytosol

  • Jan-Erik Hoffmann,
  • Yessica Fermin,
  • Ruth LO Stricker,
  • Katja Ickstadt,
  • Eli Zamir

DOI
https://doi.org/10.7554/eLife.02257
Journal volume & issue
Vol. 3

Abstract

Read online

How can the integrin adhesome get self-assembled locally, rapidly, and correctly as diverse cell-matrix adhesion sites? Here, we investigate this question by exploring the cytosolic state of integrin-adhesome components and their dynamic exchange between adhesion sites and cytosol. Using fluorescence cross-correlation spectroscopy (FCCS) and fluorescence recovery after photobleaching (FRAP) we found that the integrin adhesome is extensively pre-assembled already in the cytosol as multi-protein building blocks for adhesion sites. Stationary focal adhesions release symmetrically the same types of protein complexes that they recruit, thereby keeping the cytosolic pool of building blocks spatiotemporally uniform. We conclude a model in which multi-protein building blocks enable rapid and modular self-assembly of adhesion sites and symmetric exchange of these building blocks preserves their specifications and thus the assembly logic of the system.

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