Myosin cluster dynamics determines epithelial wound ring constriction.

Collection of myosin motors and actin filaments can self-assemble into submicrometric clusters under the regulation of RhoA. Emergent dynamics of these clusters have been reported in a variety of morphogenetic systems, ranging from Drosophila to actomyosin assays in vitro. In single-cell cytokinetic rings, actomyosin clusters contribute to stress generation when their dynamics are radial, and they facilitate transport when their dynamics are tangential to the direction of ring closure. Here, we show that these phenomena hold true for actomyosin multi-cellular rings during wound closure in epithelial monolayers. We assessed the activity of RhoA using FRET sensors, and we report that cluster dynamics does not correlate with RhoA activity. Nevertheless, we show that bursts of RhoA activation precede recruitment of myosin. Altogether myosin clusters dynamics is conserved between single and multi-cellular systems, and this suggests that they could be used as generic read-outs for mapping and predicting stress generation and shape changes in morphogenesis.