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首页> 外文期刊>Cardiovascular drugs and therapy >Advanced Interfere Treatment of Diabetic Cardiomyopathy Rats by aFGF-Loaded Heparin-Modified Microbubbles and UTMD Technique
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Advanced Interfere Treatment of Diabetic Cardiomyopathy Rats by aFGF-Loaded Heparin-Modified Microbubbles and UTMD Technique

机译:载有aFGF的肝素修饰的微泡和UTMD技术对糖尿病性心肌病大鼠的晚期干扰治疗。

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摘要

This study aims to investigate the preclinical performance and mechanism of a novel strategy of aFGF-loaded heparin-modified microbubbles (aFGF-HMB) combined with ultrasound-targeted microbubble destruction (UTMD) technique for diabetic cardiomyopathy (DCM) prevention. Type 1 diabetic rats were induced by streptozotocin. Twelve weeks after intervention, indexes from transthoracic echocardiography and cardiac catheterization showed that the left ventricular function in the aFGF-HMB/UTMD group was significantly improved compared with diabetes control (DM). From Picrosirius Red staining and TUNEL staining, the aFGF-HMB/UTMD group showed significant difference from the other groups. The cardiac collagen volume fraction (CVF) and myocardial cell apoptosis index (AI) in aFGF-HMB/UTMD group decreased to 7.2 % and 7.11 % respectively, compared with the DM group (CVF = 24.5 % and AI =20.3 % respectively). The results of myocardial microvascular density (MCD) also proved the strongest inhibition of aFGF-HMB/UTMD group on DCM progress. CD31 staining of aFGF-HMB/UTMD group reached 22 n/hrp, much higher than that of DM group (9 n/hrp). These results confirmed that the abnormalities including left ventricular dysfunction, myocardial fibrosis, cardiomyocytes apoptosis and microvascular rarefaction could be suppressed by twice weekly aFGF treatments for 12 consecutive weeks (free aFGF or aFGF-HMB+/-UTMD), with the strongest improvements observed in the aFGF-HMB/UTMD group (P < 0.05 vs free aFGF or aFGF-HMB). Western blot analyses of heart tissue further revealed the highest aFGF, anti-apoptosis protein (Bcl-2), VEGF-C, pAkt, pFoxo-3a levels and strongest reduction in pro-apoptosis proteins (Bax) level in aFGF-HMB/UTMD group. Overall, aFGF-HMB combined with UTMD technique might be developed as an effective strategy to prevent DCM in future clinical therapy.
机译:这项研究旨在探讨aFGF负载肝素修饰的微泡(aFGF-HMB)结合超声靶向微泡破坏(UTMD)技术预防糖尿病性心肌病(DCM)的新策略的临床前性能和机理。链脲佐菌素诱导1型糖尿病大鼠。干预后十二周,经胸超声心动图和心脏导管检查的指标显示,与糖尿病对照组(DM)相比,aFGF-HMB / UTMD组的左心室功能明显改善。从Picrosirius Red染色和TUNEL染色来看,aFGF-HMB / UTMD组与其他组相比有显着差异。与DM组相比,aFGF-HMB / UTMD组的心肌胶原蛋白体积分数(CVF)和心肌细胞凋亡指数(AI)分别降低至7.2%和7.11%.CDM分别为CVF = 24.5%和AI = 20.3%。心肌微血管密度(MCD)的结果还证明了aFGF-HMB / UTMD组对DCM进展的最强抑制作用。 aFGF-HMB / UTMD组的CD31染色达到22 n / hrp,远高于DM组(9 n / hrp)。这些结果证实,连续12周每周两次aFGF治疗(游离aFGF或aFGF-HMB +/- UTMD)可以抑制包括左心室功能障碍,心肌纤维化,心肌细胞凋亡和微血管稀疏在内的异常,其中最明显的改善是aFGF-HMB / UTMD组(相对于游离aFGF或aFGF-HMB,P <0.05)。心脏组织的蛋白质印迹分析进一步揭示了aFGF-HMB / UTMD中最高的aFGF,抗凋亡蛋白(Bcl-2),VEGF-C,pAkt,pFoxo-3a水平和促凋亡蛋白(Bax)水平降低最强组。总体而言,aFGF-HMB结合UTMD技术可能被开发为预防DCM在未来临床治疗中的有效策略。

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