ERYTHROPOIETIN HAS AN ADDITIVE CYTOPROTECTIVE AND BENEFICIAL EFFECT TO SILDENAFIL IN A MODEL OF DIASTOLIC HEART FAILURE IN RATS

Essam F. Alalkamy
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Abstract

Development of new forms of interventions for diastolic heart failure (HFpEF) remains a challenging task.  The aim: Assessing the effect of combining erythropoietin and sildenafil on the left ventricle “LV” functions and morphometry in NG-nitro-L-arginine methyl ester (L-NAME)-induced HFpEF model in rats. Method: Forty-eight female albino rats were randomly assigned to one of six treatment groups: “C” (Control), “L” (L-NAME-treated), “L+M” (L-NAME+milrinone-treated), “L+S” (L-NAME+sildenafil-treated), “L+E” (L-NAME+erythropoietin-treated), and “L+S+E”  (L-NAME+sildenafil+erythropoietin-treated). Assessment was done by morphometric examination, LV ejection fraction (LVEF) and fraction of shortening (LVFS)], ECG changes, and mean time to peak tension (TPT) and to complete relaxation (TCR) of isometric contraction of LV muscle strip stimulated by single (TPT-S & TCR-S) and by repeated pulses (TPT-R & TCR-R), respectively. Results: L-NAME resulted in cardiac dysfunction with significant reduction in the mean “LVEF” and “LVFS”, and prolonged both the mean “TPT-R” and “TCR-R”. Milrinone and sildenafil treatment significantly corrected these parameters. In addition, erythropoietin significantly ameliorated “LVEF” and “LVFS” and shortened “TPT-S”. Similarly, “sildenafil+erythropoietin” treatment significantly corrected the measured parameters; however, they were insignificantly different from that of sildenafil only treatment. Morphometrically, sildenafil treatment resulted in significant but partial improvement in L-NAME-induced myocardial injury. Meanwhile, erythropoietin treatment showed more improvement. Moreover, combination treatment showed the best histologic picture in all of the treated groups. Conclusion: Sildenafil was able to improve cardiac functions mainly by accelerating diastolic relaxation. Addition of erythropoietin to sildenafil improved its cytoprotective effect.
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在大鼠舒张性心力衰竭模型中,促红细胞生成素对西地那非具有细胞保护和有益作用
开发新的干预手段治疗舒张性心力衰竭(HFpEF)仍然是一项具有挑战性的任务。目的:探讨促红细胞生成素联合西地那非对ng -硝基- l -精氨酸甲酯(L-NAME)诱导大鼠HFpEF模型左心室“LV”功能及形态学的影响。方法:48只雌性白化大鼠随机分为“C”组(对照组)、“L”组(L- name组)、“L+M”组(L- name组+米力农组)、“L+S”组(L- name组+西地那非组)、“L+E”组(L- name组+西地那非组)、“L+S+E”组(L- name组+西地那非组+促红细胞生成素组)。通过形态学检查、左室射血分数(LVEF)和缩短分数(LVFS)、心电图变化、单脉冲(TPT- s和TCR- s)和重复脉冲(TPT- r和TCR- r)分别刺激左室肌条等距收缩的平均张力峰值时间(TPT)和完全松弛时间(TCR)进行评估。结果:L-NAME导致心功能障碍,显著降低LVEF和LVFS平均值,延长TPT-R和TCR-R平均值。米力农和西地那非治疗显著纠正了这些参数。此外,促红细胞生成素可显著改善“LVEF”和“LVFS”,缩短“TPT-S”。同样,“西地那非+促红细胞生成素”治疗显著纠正了测量参数;但与单用西地那非治疗差异不显著。形态学上,西地那非治疗可显著但部分改善l - name诱导的心肌损伤。同时,促红细胞生成素治疗更有改善。而且,联合治疗组在所有治疗组中表现出最好的组织学图像。结论:西地那非主要通过加速舒张作用改善心功能。在西地那非中加入促红细胞生成素可提高其细胞保护作用。
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