Publication | Open Access
Scar/WAVE3 contributes to motility and plasticity of lamellipodial dynamics but not invasion in three dimensions
18
Citations
37
References
2012
Year
EngineeringCytoskeletonCellular PhysiologyTumor BiologyCell InteractionBiomechanicsMatrix BiologyCell SignalingBiophysicsMolecular SignalingCamp ReceptorLamellipodial DynamicsMorphogenesisPlasticityCell BiologyBiophysical AspectBiologyPattern FormationScar/wave IsoformsSignal TransductionDynamic LamellipodiaCell-matrix InteractionCell MotilitySystems BiologyMedicineExtracellular Matrix
The Scar (suppressor of cAMP receptor)/WAVE [WASP (Wiskott-Aldrich syndrome protein) verprolin homologous] complex plays a major role in the motility of cells by activating the Arp2/3 complex, which initiates actin branching and drives protrusions. Mammals have three Scar/WAVE isoforms, which show some tissue-specific expression, but their functions have not been differentiated. In the present study we show that depletion of Scar/WAVE3 in the mammalian breast cancer cells MDA-MB-231 results in larger and less dynamic lamellipodia. Scar/WAVE3-depleted cells move more slowly but more persistently on a two-dimensional matrix and they typically only show one lamellipod. However, Scar/WAVE3 appears to have no role in driving invasiveness in a three-dimensional Matrigel™ invasion assay or a three-dimensional collagen invasion assay, suggesting that lamellipodial persistence as seen in two-dimensions is not crucial in three-dimensional environments.
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