首页> 外文期刊>Biomechanics and modeling in mechanobiology >Cyclic strain amplitude dictates the growth response of vascular smooth muscle cells in vitro: Role in in-stent restenosis and inhibition with a sirolimus drug-eluting stent
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Cyclic strain amplitude dictates the growth response of vascular smooth muscle cells in vitro: Role in in-stent restenosis and inhibition with a sirolimus drug-eluting stent

机译:循环应变幅度决定了体外血管平滑肌细胞的生长反应:在支架内再狭窄和西罗莫司药物洗脱支架抑制中的作用

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摘要

The putative effects of changes in mean strain and cyclic strain amplitude on vascular smooth muscle cell (vSMC) growth (proliferation and apoptosis) were examined. Subsequently, a quantitative measure of vSMC growth was obtained to determine the prolonged effect of changes in mechanical burden following bare-metal stent (BMS) and sirolimus drug-eluting stent (DES) deployment in vitro. Bovine aortic vSMCs were exposed to prolonged cyclic strain using a Flexercell~(TM) Tension system and a novel Sylgard~(TM) phantom vessel following stent implantation before the level of vSMC proliferation and apoptosis was assessed by FACS analysis, cell counting, and immunocytochemistry. Physiological cyclic strain (5%) decreased vSMC proliferation and increased apoptosis in a temporal manner. There was no significant difference in cell growth following exposure to varying mean strains with similar amplitude. In contrast, exposure to varying strain amplitudes with similar mean strains resulted in significant differences in cell proliferation and apoptosis. In parallel studies, the level of vSMC proliferation and cell survival was significantly increased within low amplitude, high mean strain regions of a phantom vessel following BMS implantation when compared to regions of higher strain amplitude upstream and downstream of the stent, respectively. Moreover, the level of vSMC growth within the stented region was significantly attenuated following implantation of a sirolimus-coated DES independent of significant changes in cell survival. Cyclic strain amplitude is an important regulator of vSMC growth capacity within a stent and is a target for inhibition using a sirolimus-coated DES.
机译:研究了平均应变和循环应变振幅变化对血管平滑肌细胞(vSMC)生长(增殖和凋亡)的假定影响。随后,获得了vSMC生长的定量测定,以确定在体外裸金属支架(BMS)和西罗莫司药物洗脱支架(DES)部署后机械负荷变化的延长效果。在支架植入后,使用FlexercellTM张力系统和新型SylgardTM幻影血管将牛主动脉vSMC暴露于延长的周期性应变,然后通过FACS分析,细胞计数和免疫细胞化学评估vSMC增殖和凋亡水平。生理循环菌株(5%)以暂时的方式降低了vSMC增殖并增加了细胞凋亡。暴露于振幅相似的不同平均菌株后,细胞生长无显着差异。相反,暴露于具有相似平均应变的不同应变幅度会导致细胞增殖和凋亡的显着差异。在平行研究中,与支架上游和下游分别具有较高应变幅度的区域相比,BMS植入后,在幻影血管的低幅度,高平均应变区域内,vSMC增殖和细胞存活水平显着提高。此外,植入西罗莫司涂层的DES后,支架区域内vSMC的生长水平显着减弱,而与细胞存活率的显着变化无关。循环应变振幅是支架内vSMC生长能力的重要调节剂,并且是使用西罗莫司涂层的DES抑制的靶标。

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