The rapid reorganization of the actin cytoskeleton in response to external stimuli is an essential property of many motile eukaryotic cells. Here, we report evidence that the actin machinery of chemotactic Dictyostelium cells operates close to an oscillatory instability. When averaging the actin response of many cells to a short pulse of the chemoattractant cAMP, we observed a transient accumulation of cortical actin reminiscent of a damped oscillation. At the single-cell level, however, the response dynamics ranged from short, strongly damped responses to slowly decaying, weakly damped oscillations. Furthermore, in a small subpopulation, we observed self-sustained oscillations in the cortical F-actin concentration. To substantiate that an oscillatory mechanism governs the actin dynamics in these cells, we systematically exposed a large number of cells to periodic pulse trains of different frequencies. Our results indicate a resonance peak at a stimulation period of around 20 s. We propose a delayed feedback model that explains our experimental findings based on a time-delay in the regulatory network of the actin system. To test the model, we performed stimulation experiments with cells that express GFP-tagged fusion proteins of Coronin and actin-interacting protein 1, as well as knockout mutants that lack Coronin and actin-interacting protein 1. These actin-binding proteins enhance the disassembly of actin filaments and thus allow us to estimate the delay time in the regulatory feedback loop. Based on this independent estimate, our model predicts an intrinsic period of 20 s, which agrees with the resonance observed in our periodic stimulation experiments.Dictyostelium discoideum | microfluidics | caged cAMP | delay-differential equation T he actin cytoskeleton provides the basis for shape dynamics and motility of eukaryotic cells. Essential biological processes like wound healing, embryonic morphogenesis, or cancer metastasis rely on the rapid rearrangement of the actin cytoskeleton in response to external chemical cues (1). Many of the underlying actin-driven processes have been investigated in cells of the social amoeba Dictyostelium discoideum. Under starvation, the singlecelled amoeba expresses a chemotactic signaling system to aggregate into a multicellular structure, mediated by the chemoattractant cAMP. The corresponding receptor signaling pathway and the downstream cytoskeletal machinery show remarkable similarities to motile cells of higher organisms, in particular neutrophils (2), making Dictyostelium one of the most popular models for eukaryotic cell motility and chemotaxis (3, 4).In earlier studies, it was observed that the actin system of chemotactic Dictyostelium cells shows a complex, nonmonotonic response when exposed to a sudden increase in the extracellular chemoattractant concentration (5-7). Between 5 and 10 s after the stimulus, a first maximum in the filamentous actin content is observed, followed by a second, less intense but prolonged maximum that starts about 30 s after the stimulus and...
