G protein-coupled receptor kinase 2 moderates recruitment of THP-1 cells to the endothelium by limiting histamine-invoked Weibel-Palade body exocytosis.

Journal of thrombosis and haemostasis : JTH Pub Date : 2014-02-01

N L Stevenson, B Martin-Martin, J Freeman, J Kriston-Vizi, R Ketteler, D F Cutler

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Abstract

Background: G protein-coupled receptors (GP-CRs) are a major family of signaling molecules, central to the regulation of inflammatory responses. Their activation upon agonist binding is attenuated by GPCR kinases (GRKs), which desensitize the receptors through phosphorylation. G protein-coupled receptor kinase 2(GRK2) down-regulation in leukocytes has been closely linked to the progression of chronic inflammatory disorders such as rheumatoid arthritis and multiple sclerosis. Because leukocytes must interact with the endothelium to infiltrate inflamed tissues, we hypothesized that GRK2 down-regulation in endothelial cells would also be pro-inflammatory.

Objectives: To determine whether GRK2 down-regulation in endothelial cells is pro-inflammatory.

Methods: siRNA-mediated ablation of GRK2 in human umbilical vein endothelial cells (HUVECs) was used in analyses of the role of this kinase. Microscopic and biochemical analyses of Weibel-Palade body (WPB) formation and functioning, live cell imaging of calcium concentrations and video analyses of adhesion of monocyte-like THP-1 cells provide clear evidence of GRK2 function in histamine activation of endothelial cells.

Results: G protein-coupled receptor kinase 2 depletion in HUVECs increases WPB exocytosis and P-selectin-dependent adhesion of THP-1 cells to the endothelial surface upon histamine stimulation, relative to controls. Further, live imaging of intracellular calcium concentrations reveals amplified histamine receptor signaling in GRK2-depleted cells, suggesting GRK2 moderates WPB exocytosis through receptor desensitization.

Conclusions: G protein-coupled receptor kinase 2 deficiency in endothelial cells results in increased pro-inflammatory signaling and enhanced leukocyte recruitment to activated endothelial cells. The ability of GRK2 to modulate initiation of inflammatory responses in endothelial cells as well as leukocytes now places GRK2 at the apex of control of this finely balanced process.

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G蛋白偶联受体激酶2通过限制组胺引起的Weibel-Palade体胞外分泌来调节THP-1细胞向内皮的募集。

背景：G蛋白偶联受体（GP-CRs）是一个重要的信号分子家族，在炎症反应的调节中起着重要作用。它们在激动剂结合后的激活被GPCR激酶（GRKs）减弱，GRKs通过磷酸化使受体脱敏。白细胞中G蛋白偶联受体激酶2（GRK2）的下调与慢性炎性疾病（如类风湿关节炎和多发性硬化症）的进展密切相关。由于白细胞必须与内皮相互作用才能浸润炎症组织，我们假设内皮细胞中GRK2的下调也可能是促炎的。目的：探讨内皮细胞中GRK2的下调是否具有促炎作用。方法：采用sirna介导的人脐静脉内皮细胞（HUVECs）中GRK2消融的方法来分析该激酶的作用。webel - palade小体（WPB）形成和功能的显微镜和生化分析、钙浓度的活细胞成像和单核细胞样THP-1细胞粘附的视频分析清楚地证明了GRK2在内皮细胞组胺激活中的作用。结果：与对照组相比，在组胺刺激下，huvec中G蛋白偶联受体激酶2的缺失增加了WPB胞分泌和p选择素依赖性THP-1细胞与内皮表面的粘附。此外，细胞内钙浓度的实时成像显示，GRK2缺失的细胞中组胺受体信号增强，表明GRK2通过受体脱敏调节WPB胞外分泌。结论：内皮细胞G蛋白偶联受体激酶2缺乏导致促炎信号增加，白细胞向活化的内皮细胞募集增加。GRK2调节内皮细胞和白细胞炎症反应起始的能力现在使GRK2处于控制这一精细平衡过程的顶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Journal of thrombosis and haemostasis : JTH

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