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Adenovirus-Mediated Gene Transfer of microRNA-21 Sponge Inhibits Neointimal Hyperplasia in Rat Vein Grafts

机译:腺病毒介导的microRNA-21海绵基因转移抑制大鼠静脉移植物中的新内膜增生。

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摘要

>Background:Vein graft failure due to neointimal hyperplasia remains an important and unresolved complication of cardiovascular surgery. microRNA-21 (miR-21) plays a major role in regulating vascular smooth muscle cell (VSMC) proliferation and phenotype transformation. Thus, the purpose of this study was to determine whether adenovirus-mediated miR-21 sponge gene therapy was able to inhibit neointimal hyperplasia in rat vein grafts.>Methods:Adenovirus-mediated miR-21 sponge was used to inhibit VSMC proliferation in vitro and neointimal formation in vivo. To improve efficiency of delivery gene transfer to the vein grafts, 20% poloxamer F-127 gel was used to increase virus contact time and 0.25% trypsin to increase virus penetration. Morphometric analyses and cellular proliferation were assessed for neointimal hyperplasia and VSMC proliferation.>Results:miR-21 sponge can significantly decrease the expression of miR-21 and proliferation in cultured VSMCs. Cellular proliferation rates were significantly reduced in miR-21 sponge-treated grafts compared with controls at 28 days after bypass surgery (14.6±9.4 vs 34.9±10.8%, P=0.0032). miR-21 sponge gene transfer therapy reduced the intimal/media area ratio in vein grafts compared with the controls (1.38±0.08 vs. 0.6±0.10, P<0.0001). miR-21 sponge treatment also improved vein graft hemodynamics. We further identified that phosphatase and tensin homolog (PTEN) is a potential target gene that was involved in the miR-21-mediated effect on neointimal hyperplasia in vein grafts.>Conclusions:Adenovirus-mediated miR-21 sponge gene therapy effectively reduced neointimal formation in vein grafts. These results suggest that there is potential for miR-21 sponge to be used to prevent vein graft failure.
机译:>背景:由于新内膜增生引起的静脉移植物衰竭仍然是心血管手术的重要且尚未解决的并发症。 microRNA-21(miR-21)在调节血管平滑肌细胞(VSMC)增殖和表型转化中起主要作用。因此,本研究的目的是确定腺病毒介导的miR-21海绵基因疗法是否能够抑制大鼠静脉移植物中的新内膜增生。>方法:采用腺病毒介导的miR-21海绵用于在体外抑制VSMC增殖和在体内抑制新内膜形成。为了提高将基因传递到静脉移植物的效率,使用了20%的泊洛沙姆F-127凝胶来增加病毒接触时间,并使用0.25%的胰蛋白酶来增加病毒渗透。对新内膜增生和VSMC增殖进行形态计量学分析和细胞增殖评估。>结果: miR-21海绵可以显着降低培养的VSMC中miR-21的表达和增殖。与对照组相比,经miR-21海绵处理的移植物在搭桥手术后28天的细胞增殖率显着降低(14.6±9.4 vs 34.9±10.8%,P = 0.0032)。与对照组相比,miR-21海绵基因转移治疗降低了静脉移植物中的内膜/中膜面积比(1.38±0.08 vs. 0.6±0.10,P <0.0001)。 miR-21海绵处理还改善了静脉移植物的血流动力学。我们进一步鉴定到,磷酸酶和张力蛋白同源物(PTEN)是潜在的靶基因,参与了miR-21介导的静脉移植物对内膜增生的作用。>结论:腺病毒介导的miR-21海绵基因治疗有效地减少了静脉移植物中新内膜的形成。这些结果表明,miR-21海绵有可能用于预防静脉移植失败。

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