ROCK1及其相关信号分子参与张应变调控的血管平滑肌细胞增殖
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国家自然科学基金项目(J1210047,11222223)


ROCK1 and the relative signal molecules participate in proliferation of vascular smooth muscle cells induced by cyclic strain
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    摘要:

    目的 探讨Rho相关卷曲蛋白激酶1(rho-associated coiled-coil containing protein kinase 1, ROCK1)及其相关信号分子在感受张应变机械刺激、调控血管平滑肌细胞(vascular smooth muscle cells,VSMCs)增殖功能中的作用。方法 应用张应变加载系统对体外培养VSMCs施加牵张幅度10%、频率1.25 Hz生理性周向张应变;Brdu检测VSMCs增殖水平;Western blotting检测力学加载后VSMCs的ROCK1表达水平以及蛋白激酶C(protein kinase C, PKC)α/β II、蛋白激酶D(protein kinase D, PKD)、胞外信号调节激酶(extracellular regulated protein kinase, ERK)磷酸化水平;采用RNA干扰技术(RNA interference, RNAi)检测ROCK1对VSMC增殖和PKCα/βII、PKD、ERK磷酸化的调控作用。结果 10%生理性张应变加载12、24 h显著抑制VSMCs的ROCK1表达,并显著抑制PKD和ERK的磷酸化;10%生理性张应变加载12 h显著抑制PKCα/βⅡ 的磷酸化,但加载24 h PKCα/βⅡ 的磷酸化与静止对照组相比无显著差异。RNAi抑制VSMCs的ROCK1表达后,VSMCs增殖水平显著降低,同时PKCα/βⅡ 和PKD磷酸化水平显著降低,但ERK磷酸化无明显变化。结论 10%生理性张应变可能通过抑制ROCK1表达调控PKCα/βⅡ 和PKD的磷酸化水平,从而影响VSMCs增殖,维持血管稳定性。探讨张应变力学刺激调控血管细胞功能的细胞内信号转导网络,对心血管生理和疾病病理机制研究具有一定意义。

    Abstract:

    Objective To investigate the role of rho-associated coiled-coil containing protein kinase 1 (ROCK1) and the relative signal molecules in sensing the mechanical stimulation from tensile strain and regulating the proliferation of vascular smooth muscle cells (VSMCs). Methods Physiological cyclic strain with magnitude of 10% and at frequency of 1.25 Hz was applied to VSMCs in vitro by using strain loading system. The proliferation level of VSMCs was analyzed by BrdU ELISA; the expression level of ROCK1, phosphorylations of protein kinase C (PKC) α/β II, protein kinase D (PKD) and extracellular regulated protein kinase (ERK) in VSMCs modulated by cyclic strain were detected with Western blotting; the expression of ROCK1 was specifically repressed by using RNA interference (RNAi). Results Compared with the static control, 10% cyclic strain significantly decreased the expression of ROCK1 and phosphorylations of PKD and ERK. The phosphorylation of PKCα/βII was decreased significantly under 10% cyclic strain for 12 h, but returned to normal level after 24 h-loading. Repressed expression of ROCK1 with RNAi significantly down-regulated VSMC proliferation, suppressed phosphorylations of PKCα/βII and PKD, but no obvious change was found in phosphorylation of ERK. Conclusions Physiological cyclic strain with magnitude of 10% may repress the phosphorylation of PKCα/βII and PKD via inhibiting the expression of ROCK1, which subsequently affect VSMC proliferation and maintain vascular hemostasis. The investigation on intracellular mechanotransduction network of VSMCs under mechanical stimulation of cyclic strain may contribute to the physiological and pathological mechanisms of cardiovascular diseases.

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王立意,郭东铭,庞景之,杨煜晨,沈宝荣,齐颖新. ROCK1及其相关信号分子参与张应变调控的血管平滑肌细胞增殖[J].医用生物力学,2017,32(3):205-212

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  • 收稿日期:2016-06-23
  • 最后修改日期:2016-10-12
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  • 在线发布日期: 2017-06-28
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