Assembly and Reorientation of Stress Fibers Drives Morphological Changes to Endothelial Cells Exposed to Shear Stress

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Assembly and Reorientation of Stress Fibers Drives Morphological Changes to Endothelial Cells Exposed to Shear Stress

Sabrena Noria^*, Feng Xu^*, Shannon McCue^*, Mara Jones^*, Avrum I. Gotlieb^* and B. Lowell Langille^*

From the Toronto General Research Institute,^* University Health Network, Toronto; and the Department of Laboratory Medicine and Pathobiology, University of Toronto, Toronto, Canada

Fluid shear stress greatly influences the biology of vascularendothelial cells and the pathogenesis of atherosclerosis. Endothelialcells undergo profound shape change and reorientation in responseto physiological levels of fluid shear stress. These morphologicalchanges influence cell function; however, the processes thatproduce them are poorly understood. We have examined how actinassembly is related to shear-induced endothelial cell shapechange. To do so, we imposed physiological levels of shear stresson cultured endothelium for up to 96 hours and then permeabilizedthe cells and exposed them briefly to fluorescently labeledmonomeric actin at various time points to assess actin assembly.Alternatively, monomeric actin was microinjected into cellsto allow continuous monitoring of actin distribution. Actinassembly occurred primarily at the ends of stress fibers, whichsimultaneously reoriented to the shear axis, frequently fusedwith neighboring stress fibers, and ultimately drove the polesof the cells in the upstream and/or downstream directions. Actinpolymerization occurred where stress fibers inserted into focaladhesion complexes, but usually only at one end of the stressfiber. Neither the upstream nor downstream focal adhesion complexwas preferred. Changes in actin organization were accompaniedby translocation and remodeling of cell-substrate adhesion complexesand transient formation of punctate cell-cell adherens junctions.These findings indicate that stress fiber assembly and realignmentprovide a novel mode by which cell morphology is altered bymechanical signals.

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