Publication | Open Access
Generation of compartmentalized pressure by a nuclear piston governs cell motility in a 3D matrix
361
Citations
19
References
2014
Year
EngineeringNuclear StructureCytoskeletonBiomedical EngineeringCellular PhysiologyBiomechanicsNucleus ForwardNuclear Piston GovernsMatrix BiologyBiophysicsMechanobiologyActomyosin ContractilityCell BiomechanicsCell BiologyDevelopmental BiologyCompartmentalized PressureCell MigrationCell MotilityCellular StructureMedicineExtracellular Matrix
Cells use actomyosin contractility to move through three-dimensional (3D) extracellular matrices. Contractility affects the type of protrusions cells use to migrate in 3D, but the mechanisms are unclear. In this work, we found that contractility generated high-pressure lobopodial protrusions in human cells migrating in a 3D matrix. In these cells, the nucleus physically divided the cytoplasm into forward and rear compartments. Actomyosin contractility with the nucleoskeleton-intermediate filament linker protein nesprin-3 pulled the nucleus forward and pressurized the front of the cell. Reducing expression of nesprin-3 decreased and equalized the intracellular pressure. Thus, the nucleus can act as a piston that physically compartmentalizes the cytoplasm and increases the hydrostatic pressure between the nucleus and the leading edge of the cell to drive lamellipodia-independent 3D cell migration.
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