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首页> 外文期刊>Inflammation >Regulation on RhoA in vascular smooth muscle cells under inflammatory stimulation proposes a novel mechanism mediating the multiple-beneficial action of acetylsalicylic acid
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Regulation on RhoA in vascular smooth muscle cells under inflammatory stimulation proposes a novel mechanism mediating the multiple-beneficial action of acetylsalicylic acid

机译:炎症刺激下血管平滑肌细胞中RhoA的调控提出了介导乙酰水杨酸的多种有益作用的新机制

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Recent studies have revealed the additional beneficial effects of acetylsalicylic acid (aspirin) in the medication of cardiovascular diseases. The small GTPase RhoA as an important signaling factor is implicated in a wide range of cell functions. This study aimed to investigate the regulatory effect of acetylsalicylic acid on RhoA in vascular smooth muscle cells (VSMCs). We found that aspirin at 300 μM suppressed VSMCs proliferation stimulated by LPS, and this inhibitory effect was partially mediated by inhibiting the iNOS/NO pathway. RhoA overexpression was downregulated by aspirin (both 30 and 300 μM) because of enhanced degradation of RhoA protein. The effect of LPS on increasing active RhoA level was significantly attenuated by aspirin (300 μM), which exerted no effect on RhoA translocation. The promoted RhoA phosphorylation under LPS stimulation, coupled with RhoA protein expression, was greatly decreased by aspirin treatment. No effect of aspirin was found on the expression, activation, and phosphorylation of RhoA in VSMCs devoid of inflammatory stimulation. Our investigation indicates that the regulation of RhoA by aspirin in VSMCs under inflammatory stimulus could be a novel mechanism via which aspirin, apart from the COX-dependent action, exerted the multiple beneficial effects.
机译:最近的研究表明,乙酰水杨酸(阿司匹林)在治疗心血管疾病方面具有额外的有益作用。小GTPase RhoA作为重要的信号转导因子,与多种细胞功能有关。这项研究旨在调查乙酰水杨酸对血管平滑肌细胞(VSMC)中RhoA的调节作用。我们发现300μM的阿司匹林抑制了LPS刺激的VSMC增殖,并且这种抑制作用部分是通过抑制iNOS / NO途径介导的。由于RhoA蛋白的降解增强,阿司匹林(30和300μM)下调了RhoA过表达。阿司匹林(300μM)显着减弱了LPS对增加活性RhoA水平的影响,但对RhoA易位没有影响。阿司匹林处理可大大降低LPS刺激下促进的RhoA磷酸化,并降低RhoA蛋白表达。没有阿司匹林对没有炎症刺激的VSMC中RhoA的表达,激活和磷酸化没有影响。我们的研究表明,在炎症刺激下,阿司匹林对VSMC中RhoA的调节可能是一种新的机制,通过该机制,阿司匹林除了具有COX依赖性作用外,还可以发挥多种有益作用。

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