IC87201, a PSD-95/nNOS Inhibitor, Ameliorates Heart Rate Variability in the Rat Model of Middle Cerebral Artery Occlusion

Mohammadian Maryam, Bahaoddini Aminollah
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Abstract

Objective: Assessment of heart rate variability (HRV) is a non-invasive and reliable method to evaluate autonomic disorders after cerebral ischemia. The present study was conducted to investigate the therapeutic potential of IC87201 in reducing post-stroke cardiac dysfunction. Materials and methods: Cerebral ischemia was induced by the middle cerebral artery occlusion (MCAO) method in 15 anesthetized adult male rats in three MCAO, MCAO+ DXM, and MCAO+ IC87201 groups, for one hour. Electrocardiogram was recorded before, and 48 hours after ischemia and drug administration, and HRV parameters were calculated from R-R intervals. In the treatment groups, IC87201 and Dextromethorphan hydrobromide monohydrate (DXM) were injected after an ischemic period. Results: After brain ischemia, the R-R interval decreased and consequently heart rate increased. The R-R intervals were used to extract the HRV frequency and time domains, including normalized low frequency (LF), high frequency (HF), LF/HF ratio, and standard deviation of R-R interval (SDRR). Normalized LF and LF/HF ratio enhanced 48 hours after ischemia, while normalized HF and SDRR significantly reduced compared to the pre-ischemic state. All HRV parameters had returned to their pre-ischemic level 48 hours after IC87201 and DXM administration, except SDRR, which recovered only in the IC87201 administered group. Conclusion: Based on our findings, it can be concluded that cerebral ischemia significantly worsens HRV parameters as a result of sympathetic overactivity. These changes were reversed by administering DXM and IC87201, but IC87201 has generally been more effective in lowering lesions. As a result, IC87201 can be introduced as an effective substance for the treatment of post-ischemic cardiac side effects.
PSD-95/nNOS抑制剂IC87201改善大脑中动脉闭塞模型大鼠心率变异性
目的:评估心率变异性(HRV)是评估脑缺血后自主神经功能紊乱的一种无创、可靠的方法。本研究旨在探讨IC87201在减少脑卒中后心功能障碍方面的治疗潜力。材料与方法:将15只麻醉后的成年雄性大鼠分为MCAO组、MCAO+ DXM组、MCAO+ IC87201组,采用大脑中动脉闭塞法(MCAO)诱导脑缺血1小时。记录缺血及给药前、给药后48 h的心电图,根据R-R间期计算HRV参数。治疗组缺血后注射IC87201和氢溴酸右美沙芬(DXM)。结果:脑缺血后R-R间期缩短,心率升高。利用R-R区间提取HRV频率域和时间域,包括归一化低频(LF)、高频(HF)、LF/HF比值和R-R区间标准差(SDRR)。缺血48 h后,归一化的LF和LF/HF比值升高,而归一化的HF和SDRR较缺血前明显降低。在IC87201和DXM给药后48小时,所有HRV参数均恢复到缺血前水平,但SDRR仅在IC87201给药组恢复。结论:基于我们的研究结果,我们可以得出结论,脑缺血导致交感神经过度活跃导致HRV参数显著恶化。使用ddxm和IC87201可逆转这些变化,但IC87201在降低病变方面通常更有效。因此,IC87201可以作为治疗缺血后心脏副作用的有效物质引入。
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