缺乏促红细胞生成活性的新型选择性促红细胞生成素受体配体可减小大鼠急性心肌梗死的梗死面积。
Novel, selective EPO receptor ligands lacking erythropoietic activity reduce infarct size in acute myocardial infarction in rats.
作者信息
Kiss Krisztina, Csonka Csaba, Pálóczi János, Pipis Judit, Görbe Anikó, Kocsis Gabriella F, Murlasits Zsolt, Sárközy Márta, Szűcs Gergő, Holmes Christopher P, Pan Yijun, Bhandari Ashok, Csont Tamás, Shamloo Mehrdad, Woodburn Kathryn W, Ferdinandy Péter, Bencsik Péter
机构信息
Cardiovascular Research Group, Department of Biochemistry, University of Szeged, Dom ter 9, Szeged H-6720, Hungary.
Department of Biochemistry, University of Szeged, Dom ter 9, Szeged H-6720, Hungary.
出版信息
Pharmacol Res. 2016 Nov;113(Pt A):62-70. doi: 10.1016/j.phrs.2016.08.013. Epub 2016 Aug 10.
Erythropoietin (EPO) has been shown to protect the heart against acute myocardial infarction in pre-clinical studies, however, EPO failed to reduce infarct size in clinical trials and showed significant safety problems. Here, we investigated cardioprotective effects of two selective non-erythropoietic EPO receptor ligand dimeric peptides (AF41676 and AF43136) lacking erythropoietic activity, EPO, and the prolonged half-life EPO analogue, darbepoetin in acute myocardial infarction (AMI) in rats. In a pilot study, EPO at 100U/mL significantly decreased cell death compared to vehicle (33.8±2.3% vs. 40.3±1.5%, p<0.05) in rat neonatal cardiomyocytes subjected to simulated ischemia/reperfusion. In further studies (studies 1-4), in vivo AMI was induced by 30min coronary occlusion and 120min reperfusion in male Wistar rats. Test compounds and positive controls for model validation (B-type natriuretic peptide, BNP or cyclosporine A, CsA) were administered iv. before the onset of reperfusion. Infarct size (IS) was measured by standard TTC staining. In study 1, 5000U/kg EPO reduced infarct size significantly compared to vehicle (45.3±4.8% vs. 59.8±4.5%, p<0.05). In study 2, darbepoetin showed a U-shaped dose-response curve with maximal infarct size-reducing effect at 5μg/kg compared to the vehicle (44.4±5.7% vs. 65.9±2.7%, p<0.01). In study 3, AF41676 showed a U-shaped dose-response curve, where 3mg/kg was the most effective dose compared to the vehicle (24.1±3.9% vs. 44.3±2.5%, p<0.001). The positive control BNP significantly decreased infarct size in studies 1-3 by approximately 35%. In study 4, AF43136 at 10mg/kg decreased infarct size, similarly to the positive control CsA compared to the appropriate vehicle (39.4±5.9% vs. 58.1±5.4% and 45.9±2.4% vs. 63.8±4.1%, p<0.05, respectively). This is the first demonstration that selective, non-erythropoietic EPO receptor ligand dimeric peptides AF41676 and AF43136 administered before reperfusion are able to reduce infarct size in a rat model of AMI. Therefore, non-erythropoietic EPO receptor peptide ligands may be promising cardioprotective agents.
在临床前研究中,促红细胞生成素(EPO)已被证明可保护心脏免受急性心肌梗死的影响,然而,EPO在临床试验中未能减小梗死面积,并显示出显著的安全性问题。在此,我们研究了两种缺乏促红细胞生成活性的选择性非促红细胞生成素EPO受体配体二聚体肽(AF41676和AF43136)、EPO以及半衰期延长的EPO类似物达贝泊汀对大鼠急性心肌梗死(AMI)的心脏保护作用。在一项初步研究中,与载体相比,100U/mL的EPO显著降低了经历模拟缺血/再灌注的大鼠新生心肌细胞的细胞死亡(33.8±2.3%对40.3±1.5%,p<0.05)。在进一步的研究(研究1 - 4)中,通过在雄性Wistar大鼠中进行30分钟冠状动脉闭塞和120分钟再灌注诱导体内AMI。在再灌注开始前静脉注射测试化合物和用于模型验证的阳性对照(B型利钠肽,BNP或环孢素A,CsA)。通过标准的TTC染色测量梗死面积(IS)。在研究1中,与载体相比,5000U/kg的EPO显著减小了梗死面积(45.3±4.8%对59.8±4.5%,p<0.05)。在研究2中,达贝泊汀呈现出U形剂量反应曲线,与载体相比,在5μg/kg时具有最大的梗死面积减小效果(44.±5.7%对65.9±2.7%,p<0.01)。在研究3中,AF41676呈现出U形剂量反应曲线,与载体相比,3mg/kg是最有效的剂量(24.1±3.9%对44.3±2.5%,p<0.001)。阳性对照BNP在研究1 - 3中显著减小梗死面积约35%。在研究4中,10mg/kg的AF43136减小了梗死面积,与阳性对照CsA类似,与相应载体相比(分别为39.4±5.9%对58.1±5.4%和45.9±2.4%对63.8±4.1%,p<0.05)。这是首次证明在再灌注前给予选择性、非促红细胞生成的EPO受体配体二聚体肽AF41676和AF43136能够在大鼠AMI模型中减小梗死面积。因此,非促红细胞生成的EPO受体肽配体可能是有前景的心脏保护剂。
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