Publication | Open Access
The secreted Ipa complex of Shigella flexneri promotes entry into mammalian cells.
201
Citations
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References
1996
Year
Protein SecretionMicrobial PathogensCell AdhesionImmunologyMolecular BiologyCytoskeletonBacterial PathogensCellular PhysiologyCell InteractionMatrix BiologySecretory PathwayCell SignalingEpithelial CellsSecreted Ipa ComplexShigella FlexneriProtein FunctionVirulence FactorGene ExpressionMammalian CellsCell BiologySignal TransductionNatural SciencesIpa ComplexLong Actin FilamentsMicrobiologyIntracellular TraffickingCellular BiochemistryMedicineExtracellular Matrix
The bacterial pathogen Shigella flexneri causes bacillary dysentery in humans by invading coloncytes. Upon contact with epithelial cells, S. flexneri elicits localized plasma membrane projections sustained by long actin filaments which engulf the microorganism. The products necessary for Shigella entry include three secretory proteins: IpaB, IpaC, and IpaD. Extracellular IpaB and IpaC associate in a soluble complex, the Ipa complex. We have immunopurified this Ipa complex on latex beads and found that they were efficiently internalized into HeLa cells. Like S. flexneri entry, uptake of the beads bearing the Ipa complex was associated with membrane projections and polymerization of actin at the site of cell-bead interaction and was dependent on small Rho GTPases. These results indicate that a secreted factor can promote S. flexneri entry into epithelial cells.
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