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Significant difference between sirolimus and paclitaxel nanoparticles in anti-proliferation effect in normoxia and hypoxia: The basis of better selection of atherosclerosis treatment

机译:西罗莫司和紫杉醇纳米粒子在常氧和缺氧中抗扩散作用中的显着差异:更好地选择动脉粥样硬化处理的基础

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Compared with paclitaxel, sirolimus has been more used in the treatment of vascular restenosis gradually as an anti-proliferative drug, but few basic studies have elucidated its mechanism. The anti-proliferative effects of sirolimus or paclitaxel have been demonstrated by numerous studies under normoxia, but few studies have been achieved focusing hypoxia. In this study, porcine carotid artery injury model and classical cobalt chloride hypoxia cell model were established. Sirolimus nanoparticles (SRM-NPs), paclitaxel nanoparticles (PTX-NPs) and blank nanoparticles (Blank-NPs) were prepared respectively. The effect of RPM-NPs on the degree of stenosis, proliferative index and the expression of PCNA after 28 days of porcine carotid artery injury model was evaluated. Compared with saline group and SRM groups, SRM-NPs group suppressed vascular stenosis, proliferative index and the expression of PCNA ( P ?0.01 and P ?0.05). Endothelial cell (EC) and smooth muscle cell (SMC) were pre-treated with cobaltous chloride, followed by SRM-NPs, PTX-NPs, Blank-NPs or PBS control treating, the effects on cell proliferation, HIF-1 expression and glycolysis were detected. SRM-NPs could inhibit EC and SMC proliferation under hypoxia, while PTX-NPs couldn't ( P ?0.001). Significant differences between sirolimus and paclitaxel NPs in anti-proliferation effect under normoxia and hypoxia may due to the different inhibitory effects on HIF-1α expression and glycolysis. In conclusion, these results suggest that sirolimus can inhibit the proliferation of hypoxic cells more effectively than paclitaxel. These observations may provide a basis for understanding clinical vascular stenosis therapeutic differences between rapamycin and paclitaxel.
机译:与紫杉醇相比,西罗莫司逐渐被用作血管再狭窄的治疗逐渐作为抗增殖药物,但少数基本研究阐明了其机制。通过常氧的许多研究证明了西罗莫司或紫杉醇的抗增殖作用,但缺氧缺氧很少有研究。在该研究中,建立了猪颈动脉损伤模型和典型氯化钴缺氧细胞模型。分别制备西罗司纳米颗粒(SRM-NPS),紫杉醇纳米颗粒(PTX-NPS)和坯料纳米颗粒(BALLB-NPS)。评估了RPM-NP对猪颈动脉损伤28天后狭窄,增殖指数和PCNA表达的影响。与盐碱组和SRM组相比,SRM-NPS组抑制血管狭窄,增殖指数和PCNA的表达(P <0.01和P&?0.05)。用氯化钴预处理内皮细胞(EC)和平滑肌细胞(SMC),其次是SRM-NPS,PTX-NPS,BALKED-NPS或PBS治疗,对细胞增殖的影响,HIF-1表达和糖酵解被发现了。 SRM-NPS可以抑制缺氧下的EC和SMC增殖,而PTX-NPS不能(P <0.001)。由于对HIF-1α的表达和糖溶解的不同抑制作用,西罗莫司和紫杉醇NPS在抗扩散效应中的显着差异可能是由于对HIF-1α表达和糖酵解的不同抑制作用。总之,这些结果表明西罗莫司可以比紫杉醇更有效地抑制缺氧细胞的增殖。这些观察结果可以为了解雷帕霉素和紫杉醇之间的临床血管狭窄治疗差异提供依据。

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