Lidington Elaine A, Steinberg Rivka, Kinderlerer Anne R, Landis R Clive, Ohba Motoi, Samarel Allen, Haskard Dorian O, Mason Justin C
Cardiovascular Medicine Unit, Imperial College, Hammersmith Hospital, DuCane Road, London W12 ONN, UK.
Am J Physiol Cell Physiol. 2005 Dec;289(6):C1437-47. doi: 10.1152/ajpcell.00502.2004. Epub 2005 Aug 3.
Thrombin, an important mediator of thrombosis and inflammation, may also enhance vascular cytoprotection. Thus thrombin induces expression of the complement-inhibitory protein decay-accelerating factor (DAF) in human umbilical vein endothelial cells (HUVECs), thus increasing protection against complement-mediated injury. Using PKC isozyme-specific peptide antagonists and adenoviral constructs, we have shown in the present study that PKC-epsilon is the primary isozyme involved in DAF induction by thrombin. Experiments with proteinase-activated receptor-1 (PAR1) and PAR2 activating peptides (APs) showed that DAF expression induced by PAR1-AP was PKC-alpha-dependent; in contrast, PAR2-AP induction of DAF required activation of PKC-epsilon. PAR1-AP and PAR2-AP in combination exerted an additive effect on DAF protein expression, which was equivalent to that observed with thrombin alone. These data implied a specific role for PAR2 in DAF induction, which was supported by the observation that upregulation of endothelial cell (EC) PAR2-enhanced DAF induction by thrombin. ERK1/2, p38, and JNK MAPK were also involved in thrombin-induced DAF upregulation, with evidence of interdependence between ERK1/2 and JNK. A role for transactivation of PAR2 by PAR1 was suggested by partial inhibition of thrombin-induced DAF expression by the PAR1 signaling antagonists BMS-200261 and SCH79797, whereas inhibition of thrombin-induced cleavage of PAR1 by specific MAbs or hirudin completely abrogated the response. Together, these data imply that the predominant pathway for thrombin-induced DAF expression involves transactivation of PAR2 by PAR1 and signaling via PKC-epsilon/MAPK. This may represent an important, novel pathway for endothelial cytoprotection during inflammation and angiogenesis and suggests that PAR2 may play a central role in some thrombin-induced responses.
凝血酶是血栓形成和炎症反应的重要介质,它也可能增强血管细胞保护作用。因此,凝血酶可诱导人脐静脉内皮细胞(HUVECs)中补体抑制蛋白衰变加速因子(DAF)的表达,从而增强对补体介导损伤的保护作用。在本研究中,我们使用蛋白激酶C(PKC)同工酶特异性肽拮抗剂和腺病毒构建体,证明PKC-ε是凝血酶诱导DAF表达所涉及的主要同工酶。用蛋白酶激活受体-1(PAR1)和PAR2激活肽(APs)进行的实验表明,PAR1-AP诱导的DAF表达依赖于PKC-α;相反,PAR2-AP诱导DAF需要激活PKC-ε。PAR1-AP和PAR2-AP联合对DAF蛋白表达具有累加效应,这与单独使用凝血酶时观察到的效应相当。这些数据暗示PAR2在DAF诱导中具有特定作用,内皮细胞(EC)PAR2上调增强凝血酶诱导的DAF诱导这一观察结果支持了这一点。细胞外信号调节激酶1/2(ERK1/2)、p38和应激活化蛋白激酶(JNK)丝裂原活化蛋白激酶(MAPK)也参与凝血酶诱导的DAF上调,有证据表明ERK1/2和JNK之间存在相互依赖性。PAR1信号拮抗剂BMS-200261和SCH79797对凝血酶诱导的DAF表达有部分抑制作用,提示PAR1对PAR2有反式激活作用,而特异性单克隆抗体或水蛭素抑制凝血酶诱导的PAR1裂解则完全消除了该反应。总之,这些数据表明凝血酶诱导DAF表达的主要途径涉及PAR1对PAR2的反式激活以及通过PKC-ε/ MAPK的信号传导。这可能代表了炎症和血管生成过程中内皮细胞保护的一条重要的新途径,并提示PAR2可能在某些凝血酶诱导的反应中起核心作用。
