Lefi Achmad, Asmarani Denisa Nugrahita, Dharmadjati Budi Baktijasa, Suwanto Denny, Saputra Mahendra Eko, Pravitasari Vemaniarti Lian, Anandita Faizal Ablansah
Department of Cardiology and Vascular Medicine, Faculty of Medicine Universitas Airlangga-Dr. Soetomo General Hospital, Surabaya, Indonesia.
J Tehran Heart Cent. 2024 Oct;19(4):256-263. doi: 10.18502/jthc.v19i4.17610.
Rheumatic heart disease (RHD) is exacerbated by chronic inflammation that stimulates the release of proinflammatory cytokines, most notably transforming growth factor-beta 1 (TGF-β1), which promotes myofibroblast differentiation. This study aims to determine the optimal dosage of Lisinopril, an angiotensin-converting enzyme inhibitor, for mitigating the fibrotic changes associated with RHD.
This in vitro, posttest-only control group study involved obtaining valvular interstitial cells from the heart valves of 25 male New Zealand rabbits (Oryctolagus cuniculus). Valvular interstitial cells were divided into 5 groups: a control group exposed to TGF-β1, and 4 experimental groups exposed to various Lisinopril doses (1 μM, 10 μM, and 100 μM) in addition to TGF-β1. The effect of Lisinopril on myofibroblast differentiation was assessed by measuring alpha-smooth muscle actin (αSMA) expression through immunocytochemical methods. Statistical significance was determined using an independent T-test with a P value of less than 0.050.
Independent T-tests conducted on 25 male Oryctolagus cuniculus demonstrated significantly lower αSMA expression in the groups treated with various Lisinopril doses (1 μM, 10 μM, and 100 μM) compared with the TGF-β1-induced control group (P<0.050). The most significant reduction in αSMA expression was observed in the group treated with the highest Lisinopril dose of 100 μM.
Lisinopril demonstrates a significant ability to inhibit TGF-β1-induced myofibroblast differentiation in rabbit valve interstitial cells, with the 100 μM dose proving most effective. These results suggest that Lisinopril may have the potential to curb RHD progression, warranting further investigations in vivo.
风湿性心脏病(RHD)因慢性炎症而加重,这种炎症刺激促炎细胞因子的释放,最显著的是转化生长因子-β1(TGF-β1),它可促进肌成纤维细胞分化。本研究旨在确定血管紧张素转换酶抑制剂赖诺普利减轻与RHD相关纤维化改变的最佳剂量。
这项体外单组后测对照研究涉及从25只雄性新西兰兔(穴兔)的心脏瓣膜获取瓣膜间质细胞。瓣膜间质细胞分为5组:一组为暴露于TGF-β1的对照组,4个实验组除暴露于TGF-β1外,还分别暴露于不同剂量的赖诺普利(1 μM、10 μM和100 μM)。通过免疫细胞化学方法测量α平滑肌肌动蛋白(αSMA)表达,评估赖诺普利对肌成纤维细胞分化的影响。使用独立样本t检验确定统计学意义,P值小于0.050。
对25只雄性穴兔进行的独立样本t检验表明,与TGF-β1诱导的对照组相比,使用不同剂量赖诺普利(1 μM、10 μM和100 μM)处理的组中αSMA表达显著降低(P<0.050)。在使用最高赖诺普利剂量100 μM处理的组中,观察到αSMA表达下降最为显著。
赖诺普利在兔瓣膜间质细胞中显示出显著抑制TGF-β1诱导的肌成纤维细胞分化的能力,100 μM剂量最为有效。这些结果表明,赖诺普利可能有抑制RHD进展的潜力,值得在体内进行进一步研究。
