Excitable Rho dynamics drive cell contractions by sequentially inducing ERM protein-mediated actin-membrane attachment and actomyosin contractility
Posted on: 12 February 2024
Preprint posted on 20 December 2023
"Unraveling cellular dance”: Rho directs edge retractions, ERMs lead the rhythm.
Selected by Vibha SINGH
Categories: cell biology
Background.
The role of the small GTPases Rac1 and Cdc42 in driving cell protrusion via actin polymerization in various contexts and cell types is well acknowledged. Rho activity, despite being a well-known regulator of cell contractility via Rho-associated kinase (ROCK), and non-muscle myosin II (NMII), has not been fully characterized, as Rho activity has also been reported in cell protrusions (possibly via downstream effector formin, mDia1). This study aimed to clarify the roles of Rho effectors ROCK/NMII and SLK/LOK/ERM in cell morphology and Rho-driven cell contractions.
Overall, the authors manage to highlight the crucial roles of ROCK and SLK/LOK in Rho-mediated cell contractions and emphasize the significance of SLK/LOK-dependent ERM activation in safeguarding cell integrity.
Key findings.
(a) Excitability of Rho Activity and its dynamics: The spatiotemporal analysis of a FRET-based RhoB sensor revealed consistently elevated Rho activity during cell edge retractions, but not during protrusions, indicative of a distinct role in mediating cell contraction via ROCK-dependent mechanisms. Rac and Cdc42 reporters displayed the expected responses to GEF translocations, with reciprocal activation upon Rho activation/inactivation.
(b) Role of MLC and Ezrin: NMII accumulation at retracting cell edges occurred with a delay relative to Rho activity, while ERM activation showed strong co-localization without a detectable delay. This indicates that ERMs act as immediate responders to Rho activity, enhancing force transmission during retractions. Rho was further shown to activate ERMs, facilitating membrane-cortex attachment during retraction initiation, while NMII exerts contractile forces to further drive edge retraction.
(c) Feedback Mechanisms: Potential positive and negative feedback mechanisms – involving Rho, ERMs, and focal adhesion dynamics, contributing to the regulation of cell edge dynamics during, and after retraction onset, indicative of an excitable Rho signaling network has been highlighted. Positive feedback loops enhance Rho activation, resulting in pulsatile behavior and propagating waves. Besides the RhoB sensor, DORA-RhoA and RhoA2G probes also exhibit pulsatile activation patterns, supporting the existence of an excitable Rho signaling network during retractions.
(d) SLK/LOK inhibition effects: Inhibition of SLK/LOK kinase resulted in morphological phenotypes similar to ROCK inhibition, underlining the importance of Rho-dependent ERM activation for cellular integrity and contractility. A SLK/LOK inhibitor (Cpd31) caused a rapid and almost complete loss of pERM signal, suggesting a high turnover rate of ERM phosphorylation. Thrombin and nocodazole, known Rho activators, induced simultaneous increases in Rho activity and pERM signals, which were suppressed by Cpd31 but not by ROCK inhibitor (Y27632). This highlights the crucial role of SLK/LOK kinases in mediating rapid ERM activation downstream of Rho, underlining the important role of the Rho-SLK/LOK-ERM signaling axis in regulating actin-membrane attachment and force transmission.
Significance and Implications:
The authors of this study have uncovered intricate spatiotemporal dynamics of Rho activity during endothelial cell edge retractions, validating pulsatile excitability and feedback mechanisms. This delineation not only improves our understanding of cellular motility, but also uncovers the roles of Ezrin-Radixin-Moesin (ERMs) and non-muscle myosin II (NMII) in governing cell shape modifications (Figure 1). The conclusions from this study have broad implications for the field of cell migration, morphogenesis, and the regulatory networks underlying dynamic cellular responses. Furthermore, the identification of Rho excitability and ERMs as early effectors unlock avenues for exploring novel therapeutic targets and allows more detailed investigations into cellular behavior across diverse contexts.
Open questions.
(1) Since RhoA activity has been reported during cell edge protrusions, could there be a spatiotemporal correlation between edge-proximal RhoA activity and ERMs in contexts where the Rho-SLK/LOK-ERM module exists?
(2) Could activated ERM also interact/activate NMII, further accelerating cell retraction?
doi: https://doi.org/10.1242/prelights.36479
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