Abstract
Shear flow-induced migration is an important physiological phenomenon experienced by multiple cell types, including leukocytes and cancer cells. However, molecular mechanisms by which cells sense and directionally migrate in response to mechanical perturbation are not well understood. Dictyostelium discoideum social amoeba, a well-established model for studying amoeboid-type migration, also exhibits directional motility when exposed to shear flow, and this behavior is preceded by rapid and transient activation of the same signal transduction network that is activated by chemoattractants. The initial response, which can also be observed following brief 2 s stimulation with shear flow, requires an intact actin cytoskeleton; however, what aspect of the cytoskeletal network is responsible for sensing and/or transmitting the signal is unclear. We investigated the role of actin crosslinkers filamin and α-actinin by analyzing initial shear flow-stimulated responses in cells with or without these proteins. Both filamin and α-actinin showed rapid and transient relocalization from the cytosol to the cortex following shear flow stimulation. Using spatiotemporal analysis of Ras GTPase activation as a readout of signal transduction network activity, we demonstrated that lack of α-actinin did not reduce, and, in fact, slightly improved the response to acute mechanical stimulation compared to cells expressing α-actinin. In contrast, shear flow-induced Ras activation was significantly more robust in filamin-null cells rescued with filamin compared to cells expressing empty vector. Reduced responsiveness appeared to be specific to mechanical stimuli and was not due to a change in the basal activity since response to global stimulation with a chemoattractant and random migration was comparable between cells with or without filamin. Finally, while filamin-null cells rescued with filamin efficiently migrated upstream when presented with continuous flow, cells lacking filamin were defective in directional migration. Overall, our study suggests that filamin, but not α-actinin, is involved in sensing and/or transmitting mechanical stimuli that drive directed migration; however, other components of the actin cytoskeleton likely also contribute to the initial response since filamin-null cells were still able to activate the signal transduction network. These findings could have implications for our fundamental understanding of shear flow-induced migration of leukocytes, cancer cells and other amoeboid-type cells.
Highlights
Directed migration of cells to cues from their environment plays an important role in diverse physiological and pathophysiological processes, including embryo development, inflammation and cancer metastasis (Barriga and Theveneau, 2020; SenGupta et al, 2021)
Both mCherry-tagged ddFLN and ddACTN transiently localized to the cell cortex of wild-type cells following 2 s stimulation with shear flow at 45 dyn/cm2 (Figure 1 and Supplementary Video 1)
We noticed that fln− cells tended to have increased cortical Ras-binding domain (RBD) localization following the shut-off after the initial response to shear flow stimulation, suggesting that, perhaps, these cells generate more protrusions and/or become more motile compared to cells rescued with mCherry-ddFLN following stimulation
Summary
Directed migration of cells to cues from their environment plays an important role in diverse physiological and pathophysiological processes, including embryo development, inflammation and cancer metastasis (Barriga and Theveneau, 2020; SenGupta et al, 2021). Other environmental conditions, such as substrate stiffness (durotaxis), electric fields (galvanotaxis), and physical forces, such as shear flow, can guide migration, the molecular mechanisms of these types of directed migration are not well understood (Shellard and Mayor, 2020). In addition to the shear forces experienced by cells within blood and lymphatic vessels, ranging from < 1 to 12 dyn/cm in the lymphatic system, up to 6 dyn/cm in the veins, and 10–70 dyn/cm in the arteries, most cells are subject to interstitial fluid flow caused by plasma that leaks out of the capillaries and drains through the tissue to the lymphatic system (Malek et al, 1999; Wiig and Swartz, 2012). The direction of cell migration in response to shear flow appears to be dependent on a variety of factors and migration can occur either upstream or downstream of the flow depending on the type of cells, the types of adhesion molecules they express, and the strength of the shear stress (Fache et al, 2005; Valignat et al, 2013; Dominguez et al, 2015; Artemenko et al, 2016; Buffone et al, 2018, 2019)
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