Publication | Open Access
hGAAP promotes cell adhesion and migration via the stimulation of store-operated Ca2+ entry and calpain 2
64
Citations
46
References
2013
Year
Cell AdhesionCalpain 2Golgi Antiapoptotic ProteinsCell DeathCytoskeletonHgaap-dependent EffectsCellular PhysiologyAutophagySecretory PathwayCell SignalingCell PhysiologyMolecular PhysiologyCell TraffickingCell BiologySignal TransductionPhysiologyHgaap PromotesCell MigrationIntracellular TraffickingStore-operated Ca2+ EntrySystems BiologyMedicineExtracellular Matrix
Golgi antiapoptotic proteins (GAAPs) are highly conserved Golgi membrane proteins that inhibit apoptosis and promote Ca(2+) release from intracellular stores. Given the role of Ca(2+) in controlling cell adhesion and motility, we hypothesized that human GAAP (hGAAP) might influence these events. In this paper, we present evidence that hGAAP increased cell adhesion, spreading, and migration in a manner that depended on the C-terminal domain of hGAAP. We show that hGAAP increased store-operated Ca(2+) entry and thereby the activity of calpain at newly forming protrusions. These hGAAP-dependent effects regulated focal adhesion dynamics and cell migration. Indeed, inhibition or knockdown of calpain 2 abrogated the effects of hGAAP on cell spreading and migration. Our data reveal that hGAAP is a novel regulator of focal adhesion dynamics, cell adhesion, and migration by controlling localized Ca(2+)-dependent activation of calpain.
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