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

Hoffmann, Jan‐Erik; Fermin, Yessica; Stricker, Ruth Lo; Ickstadt, Katja; Zamir, Eli

doi:10.7554/elife.02257

Cited by 63 publications

(63 citation statements)

References 42 publications

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“…(legend on next page) on integrin endocytosis for their proper turnover at MASs has been reported , while recent findings have shown that focal adhesion-interacting proteins display similar kinetics (Hoffmann et al, 2014). Thus, the talin-GFP exchange rate is increased in Parvin mutants; however, the mys b58 GOF allele is sufficient to restore it.…”

Section: Discussionmentioning

confidence: 88%

IPP Complex Reinforces Adhesion by Relaying Tension-Dependent Signals to Inhibit Integrin Turnover

et al. 2016

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Cytoskeleton-mediated forces regulate the assembly and function of integrin adhesions; however, the underlying mechanisms remain unclear. The tripartite IPP complex, comprising ILK, Parvin, and PINCH, mediates the integrin-actin link at Drosophila embryo muscle attachment sites (MASs). Here, we demonstrate a developmentally earlier function for the IPP complex: to reinforce integrin-extracellular matrix (ECM) adhesion in response to tension. In IPP-complex mutants, the integrin-ECM linkage at MASs breaks in response to intense muscle contractility. Mechanistically, the IPP complex is required to relay force-elicited signals that decelerate integrin turnover at the plasma membrane so that the integrin immobile fraction is adequate to withstand tension. Epistasis analysis shows that alleviation of muscle contractility, downregulation of endocytosis, and enhanced integrin binding to the ECM are sufficient to restore integrin-ECM adhesion and maintain integrin-adhesome organization in IPP-complex mutants. Our findings reveal a role for the IPP complex as an essential mechanosensitive regulatory switch of integrin turnover in vivo.

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Section: Discussionmentioning

confidence: 88%

IPP Complex Reinforces Adhesion by Relaying Tension-Dependent Signals to Inhibit Integrin Turnover

et al. 2016

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“…In contrast, individual proteins exchange between the adhesion and cytoplasm within seconds, highlighting the dynamic nature of the adhesion (26,69,70). Again, the exchange rates correlate with myosin forces, and many critical components exchange more slowly and less extensively in the presence of blebbistatin (e.g., paxillin), whereas others exchange more readily (e.g., vinculin) (26).…”

Section: Stabilization and Maturation Of Adhesions By Forcementioning

confidence: 88%

Early Events in Cell Spreading as a Model for Quantitative Analysis of Biomechanical Events

Wolfenson

Iskratsch

Sheetz

2014

Biophysical Journal

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In this review, we focus on the early events in the process of fibroblast spreading on fibronectin matrices of different rigidities. We present a focused position piece that illustrates the many different tests that a cell makes of its environment before it establishes mature matrix adhesions. When a fibroblast is placed on fibronectin-coated glass surfaces at 37°C, it typically spreads and polarizes within 20-40 min primarily through αvβ3 integrin binding to fibronectin. In that short period, the cell goes through three major phases that involve binding, integrin activation, spreading, and mechanical testing of the surface. The advantage of using the model system of cell spreading from the unattached state is that it is highly reproducible and the stages that the cell undergoes can thus be studied in a highly quantitative manner, in both space and time. The mechanical and biochemical parameters that matter in this example are often surprising because of both the large number of tests that occur and the precision of the tests. We discuss our current understanding of those tests, the decision tree that is involved in this process, and an extension to the behavior of the cells at longer time periods when mature adhesions develop. Because many other matrices and integrins are involved in cell-matrix adhesion, this model system gives us a limited view of a subset of cellular behaviors that can occur. However, by defining one cellular process at a molecular level, we know more of what to expect when defining other processes. Because each cellular process will involve some different proteins, a molecular understanding of multiple functions operating within a given cell can lead to strategies to selectively block a function.

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“…By contrast, candidate-based microscopy studies have focused on the architecture, interactions, and dynamics of adhesion complex assembly and disassembly [34,36,37]. For example, recent studies have identified that many adhesome components are pre-assembled as multi-protein building blocks in the cytosol, allowing rapid adhesion complex maturation and turnover [34]. Together these studies have contributed to our understanding of integrin signalling, force generation, and actin regulation and their impact on numerous downstream cellular processes.…”

mentioning

confidence: 95%

“…Proteomic analyses also suggest the existence of a large number of non-canonical adhesome components. By contrast, candidate-based microscopy studies have focused on the architecture, interactions, and dynamics of adhesion complex assembly and disassembly [34,36,37]. For example, recent studies have identified that many adhesome components are pre-assembled as multi-protein building blocks in the cytosol, allowing rapid adhesion complex maturation and turnover [34].…”

mentioning

confidence: 95%

Emerging properties of adhesion complexes: what are they and what do they do?

Humphries

Paul

Morgan

2015

Trends in Cell Biology

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

Cited by 63 publications

References 42 publications

IPP Complex Reinforces Adhesion by Relaying Tension-Dependent Signals to Inhibit Integrin Turnover

IPP Complex Reinforces Adhesion by Relaying Tension-Dependent Signals to Inhibit Integrin Turnover

Early Events in Cell Spreading as a Model for Quantitative Analysis of Biomechanical Events

Emerging properties of adhesion complexes: what are they and what do they do?

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