Chemerin is an adipokine associated with increased blood pressure, and may link obesity with hypertension. We tested the hypothesis that chemerin-induced contraction of the vasculature occurs via calcium flux in smooth muscle cells. Isometric contraction of rat aortic rings was performed in parallel with calcium kinetics of rat aortic smooth muscle cells to assess the possible signaling pathway. Chemerin-9 (nonapeptide of the chemerin S157 isoform) caused a concentration-dependent contraction of isolated aorta (EC50 100 nM) and elicited a concentration-dependent intracellular calcium response (EC50 10 nM). Pertussis toxin (Gi inhibitor), verapamil (L-type Ca2+ channel inhibitor), PP1 (Src inhibitor), and Y27632 (Rho kinase inhibitor) reduced both calcium influx and isometric contraction to chemerin-9 but PD098059 (Erk MAPK inhibitor) and (PLC inhibitor) had little to no effect on either measure of chemerin signaling. Although our primary aim was to examine chemerin signaling, we also highlight differences in the mechanisms of chemerin-9 and recombinant chemerin S157. These data support a chemerin-induced contractile mechanism in vascular smooth muscle that functions through Gi proteins to activate L-type Ca2+ channels, Src, and Rho kinase. There is mounting evidence linking chemerin to hypertension and this mechanism brings us closer to targeting chemerin as a form of therapy.
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机译:Chemerin是一种与血压升高相关的脂肪因子,可能将肥胖与高血压联系起来。我们测试了一种假设,即凯莫瑞诱导的血管收缩是通过平滑肌细胞中的钙流量发生的。大鼠主动脉环的等距收缩与大鼠主动脉平滑肌细胞的钙动力学同时进行,以评估可能的信号通路。 Chemerin-9(chemerin S 157 异构体的九肽)引起离体主动脉的浓度依赖性收缩(EC50 100 nM),并引起浓度依赖性的细胞内钙反应(EC50 10 nM)。百日咳毒素(Gi抑制剂),维拉帕米(L型Ca 2 + 通道抑制剂),PP1(Src抑制剂)和Y27632(Rho激酶抑制剂)减少了钙流入和等轴收缩至凯莫瑞9但是PD098059(Erk MAPK抑制剂)和(PLC抑制剂)对凯莫瑞信号传导的两种测量几乎没有影响。尽管我们的主要目的是检查chemerin信号传导,但我们也强调了chemerin-9和重组chemerin S 157 的机制差异。这些数据支持凯莫瑞诱导的血管平滑肌收缩机制,该机制通过Gi蛋白激活L型Ca 2 + 通道,Src和Rho激酶。越来越多的证据表明凯莫瑞与高血压有关,并且这种机制使我们更接近于将凯莫瑞作为一种治疗手段。
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