Trypsin stimulates proteinase-activated receptor-2-dependent and -independent activation of mitogen-activated protein kinases

Alan D. PEMBERTON; Christopher M. BELHAM; Gwyn W. GOULD; Hugh R. P. MILLER; Pamela H. SCOTT; Robin PLEVIN; Roger M. WADSWORTH; Rothwelle J. TATE

摘要

pWe have examined protease-mediated activation of the mitogen-activated protein (MAP) kinase cascade in rat aortic smooth-muscle cells and bovine pulmonary arterial fibroblasts. Exposure of smooth-muscle cells to trypsin evoked rapid and transient activation of c-Raf-1, MAP kinase kinase 1 and 2 and MAP kinase that was sensitive to inhibition by soybean trypsin inhibitor. The actions of trypsin were closely mimicked by the proteinase-activated receptor 2 (PAR-2)-activating peptide sequence SLIGRL but not LSIGRL. Peak MAP kinase activation in response to both trypsin and SLIGRL was also dependent on concentration, with ECsub50/sub values of 12.1±3.4 nM and 62.5±4.5 iμ/iM respectively. Under conditions where MAP kinase activation by SLIGRL was completely desensitized by prior exposure of smooth-muscle cells to the peptide, trypsin-stimulated MAP kinase activity was markedly attenuated (78.9±15.1% desensitization), whereas the response to thrombin was only marginally affected (16.6±12.1% desensitization). Trypsin and SLIGRL also weakly stimulated the activation of the MAP kinase homologue p38 in smooth-muscle cells without any detectable activation of c-Jun N-terminal kinase. Strong activation of the MAP kinase cascade and modest activation of p38 by trypsin were also observed in fibroblasts, although in this cell type these effects were not mimicked by SLIGRL nor by the thrombin receptor-activating peptide SFLLRNPNDKYEPF. Reverse transcriptase–PCR analysis confirmed the presence of PAR-2 mRNA in smooth-muscle cells but not fibroblasts. Our results suggest that in vascular smooth-muscle cells, trypsin stimulates the activation of the MAP kinase cascade relatively selectively, in a manner consistent with an interaction with the recently described PAR-2. Activation of MAP kinase by trypsin in vascular fibroblasts, however, seems to be independent of PAR-2 and occurs by an undefined mechanism possibly involving novel receptor species./p

机译：>我们检查了大鼠主动脉平滑肌细胞和牛肺动脉成纤维细胞中蛋白酶介导的丝裂原活化蛋白（MAP）激酶级联反应的活化。平滑肌细胞暴露于胰蛋白酶引起对大豆胰蛋白酶抑制剂抑制敏感的c-Raf-1，MAP激酶激酶1和2和MAP激酶的快速和瞬时活化。蛋白酶激活的受体2（PAR-2）激活肽序列SLIGRL与LSIGRL紧密模仿了胰蛋白酶的作用。胰蛋白酶和SLIGRL响应的峰值MAP激酶活化也取决于浓度，EC _{50 值分别为12.1±3.4 nM和62.5±4.5 μM。在先于平滑肌细胞暴露于肽的情况下，SLIGRL激活的MAP激酶激活完全脱敏的条件下，胰蛋白酶刺激的MAP激酶活性显着减弱（脱敏78.9±15.1％），而对凝血酶的反应仅受到轻微影响（ 16.6±12.1％的脱敏）。胰蛋白酶和SLIGRL还弱刺激了平滑肌细胞中MAP激酶同源物p38的激活，而未检测到c-Jun N端激酶的激活。在成纤维细胞中也观察到了MAP激酶级联的强活化和胰蛋白酶对p38的适度活化，尽管在这种细胞类型中，SLIGRL或凝血酶受体活化肽SFLLRNPNDKYEPF都没有模仿这些作用。逆转录-PCR分析证实，平滑肌细胞中存在PAR-2 mRNA，而成纤维细胞中没有。我们的结果表明，在血管平滑肌细胞中，胰蛋白酶以与最近描述的PAR-2相互作用相一致的方式相对选择性地刺激MAP激酶级联反应的激活。胰蛋白酶在血管成纤维细胞中激活MAP激酶似乎与PAR-2无关，并且可能是由一种不确定的机制引起的，可能涉及新的受体种类。}

Trypsin stimulates proteinase-activated receptor-2-dependent and -independent activation of mitogen-activated protein kinases

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