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Zoledronate upregulates MMP-9 and -13 in rat vascular smooth muscle cells by inducing oxidative stress

机译:唑来膦酸盐通过诱导氧化应激上调大鼠血管平滑肌细胞中的MMP-9和-13

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Background: Bisphosphonates, including zoledronate, target osteoclasts and are widely used in the treatment of osteoporosis and other bone resorption diseases, despite side effects that include damaging the stomach epithelium. Beneficial and adverse effects on other organ systems, including the cardiovascular system, have also been described and could impact on the use of bisphosphonates as therapeutic agents. Vascular smooth muscle cells (VSMCs) are major constituents of the normal vascular wall and have a key role in intimal thickening and atherosclerosis, in part by secreting MMPs that remodel the extracellular matrix and cleave cell surface proteins or secreted mediators. In this study, we investigated the effects of zoledronate on MMP expression. Methods: Rat VSMCs were stimulated by PDGF (50 ng/mL) plus TNF-α (10 ng/mL) or left unstimulated for a further 24 hours in serum-free medium. In other series of experiments, cells were pre-treated either with SC-514 (50 μM) or with apocynin (20 nM) for 2 hours, then zoledronate (100 μM) was added into 2% fetal calf serum containing medium for 24 hours. Results and discussion: Using isolated rat VSMCs in culture, zoledronate (100 μM) increased MMP-9 and -13 mRNA expressions but inhibited MMP-2 expression. MMP-9 and MMP-13 up-regulation was shown to depend on the NF-κB pathway; and this was activated by zoledronate. Furthermore, zoledronate elevated the levels of reactive oxygen species detected by either dichlorofluorescein in isolated VSMCs or lucigenin enhanced chemiluminescence in rat aortic rings in vitro. Apocynin, an inhibitor of NADPH oxidase, reversed NF-κB activation and MMP-9 and MMP-13 up-regulation by zoledronate. Conclusion: We conclude that zoledronate increases MMP-9 and MMP-13 expressions in rat VSMCs dependent upon stimulation of the NF-κB pathway by reactive oxygen species. Effects on MMP expression may contribute to the pharmacologic profile of bisphosphonates.
机译:背景:双膦酸盐(包括唑来膦酸盐)靶向破骨细胞,尽管副作用包括损害胃上皮,但仍广泛用于治疗骨质疏松症和其他骨吸收疾病。还已经描述了对其他器官系统(包括心血管系统)的有利和不利影响,这些影响可能会影响双膦酸盐作为治疗剂的使用。血管平滑肌细胞(VSMC)是正常血管壁的主要成分,在内膜增厚和动脉粥样硬化中起关键作用,部分原因是通过分泌MMP来重塑细胞外基质并裂解细胞表面蛋白或分泌的介体。在这项研究中,我们调查了唑来膦酸盐对MMP表达的影响。方法:PDGF(50 ng / mL)加TNF-α(10 ng / mL)刺激大鼠VSMC,或在无血清培养基中再刺激24小时。在其他系列实验中,将细胞用SC-514(50μM)或载脂蛋白(20 nM)预处理2小时,然后将唑来膦酸盐(100μM)加入含2%胎牛血清的培养基中24小时。结果与讨论:在培养物中使用分离的大鼠VSMC,唑来膦酸盐(100μM)增加MMP-9和-13 mRNA表达,但抑制MMP-2表达。 MMP-9和MMP-13的上调依赖于NF-κB通路。并被唑来膦酸盐激活。此外,唑来膦酸盐可提高离体VSMC中的二氯荧光素检测到的活性氧种类的水平,或在体外大鼠主动脉环中通过荧光黄素增强的化学发光作用。 Apocynin,NADPH氧化酶的抑制剂,通过唑来膦酸逆转了NF-κB的活化以及MMP-9和MMP-13的上调。结论:我们得出的结论是唑来膦酸盐增加了大鼠VSMC中MMP-9和MMP-13的表达,这取决于活性氧对NF-κB途径的刺激。对MMP表达的影响可能有助于双膦酸盐的药理作用。

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