The UDP-sugar-sensing P2Y14receptor promotes Rho-mediated signaling and chemotaxis in human neutrophils

罗亚 HL60型 细胞生物学 趋化性 信号转导 促炎细胞因子 生物 运动性 受体 化学 生物化学 细胞 炎症 免疫学
作者
Juliana I. Sesma,Silvia M. Kreda,Natacha Steinckwich-Besançon,Hong Dang,Rafael Garcı́a-Mata,T. Kendall Harden,Eduardo R. Lazarowski
出处
期刊:American Journal of Physiology-cell Physiology [American Physiological Society]
卷期号:303 (5): C490-C498 被引量:57
标识
DOI:10.1152/ajpcell.00138.2012
摘要

The G i -coupled P2Y 14 receptor (P2Y 14 -R) is potently activated by UDP-sugars and UDP. Although P2Y 14 -R mRNA is prominently expressed in circulating neutrophils, the signaling pathways and functional responses associated with this receptor are undefined. In this study, we illustrate that incubation of isolated human neutrophils with UDP-glucose resulted in cytoskeleton rearrangement, change of cell shape, and enhanced cell migration. We also demonstrate that UDP-glucose promotes rapid, robust, and concentration-dependent activation of RhoA in these cells. Ecto-nucleotidases expressed on neutrophils rapidly hydrolyzed extracellular ATP, but incubation with UDP-glucose for up to 1 h resulted in negligible metabolism of the nucleotide-sugar. HL60 human promyelocytic leukemia cells do not express the P2Y 14 -R, but neutrophil differentiation of HL60 cells with DMSO resulted in markedly enhanced P2Y 14 -R expression. Accordingly, UDP-glucose, UDP-galactose, and UDP- N-acetylglucosamine promoted Rho activation in differentiated but not in undifferentiated HL60 cells. Stable expression of recombinant human P2Y 14 -R conferred UDP-sugar-promoted responses to undifferentiated HL60 cells. UDP-glucose-promoted RhoA activation also was accompanied by enhanced cell migration in differentiated HL60 cells, and these responses were blocked by Rho kinase inhibitors. These results support the notion that UDP-glucose is a stable and potent proinflammatory mediator that promotes P2Y 14 -R-mediated neutrophil motility via Rho/Rho kinase activation.
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