Publication | Open Access
Domain and Functional Analysis of a Novel Platelet-Endothelial Cell Surface Protein, SCUBE1
107
Citations
31
References
2008
Year
SclerostinCell AdhesionImmunologyCytoskeletonBrain MorphogenesisFunctional AnalysisCellular PhysiologyInflammationThrombosisAngiogenesisBone Morphogenic ProteinFibroblast Growth FactorMatrix BiologyCell SignalingVascular BiologyNeovascularizationCell BiologyCub DomainCell Surface GlycoproteinThrombopoiesisSignal TransductionDevelopmental BiologyBlood PlateletEndothelial DysfunctionMedicineExtracellular Matrix
SCUBE1 (signal peptide-CUB-EGF domain-containing protein 1) is a novel, secreted, cell surface glycoprotein expressed during early embryogenesis and found in platelet and endothelial cells. This protein is composed of an N-terminal signal peptide sequence followed by nine tandemly arranged epidermal growth factor (EGF)-like repeats, a spacer region, three cysteine-rich repeat motifs, and one CUB domain at the C terminus. However, little is known about its domain and biological function. Here, we generated a comprehensive panel of domain deletion constructs and a new genetic mouse model with targeted disruption of Scube1 (Scube1(Delta cub/Delta cub)) to investigate the domain function and biological significance. A number of cell-based assays were utilized to define the critical role of the spacer region for membrane association and establish that the EGF-like repeats 7-9 are sufficient for the formation of SCUBE1-mediated homophilic adhesions in a calcium-dependent fashion. Biochemical and molecular analyses showed that the C-terminal cysteine-rich motifs and CUB domain could directly bind and antagonize the bone morphogenetic protein activity. Furthermore, genetic ablation of this C-terminal region resulted in brain malformation in the Scube1(Delta cub/Delta cub) embryos. Together, our results support the dual roles of SCUBE1 on brain morphogenesis and cell-cell adhesions through its distinct domain function.
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