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首页> 外文期刊>Oxidative Medicine and Cellular Longevity >Melatonin against Myocardial Ischemia-Reperfusion Injury: A Meta-analysis and Mechanism Insight from Animal Studies
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Melatonin against Myocardial Ischemia-Reperfusion Injury: A Meta-analysis and Mechanism Insight from Animal Studies

机译:褪黑激素免受心肌缺血再灌注损伤:动物研究中的荟萃分析和机制洞察力

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Aims. Myocardial reperfusion damage after severe ischemia was an important issue during a clinical practice. However, the exacted pathogenesis involved remained unclear and also lacks effective interventions. Melatonin was identified to exert protective effects for alleviating the myocardial I/R injury. This meta-analysis was determined to evaluate the efficacy of melatonin treatment against reperfusion insult and further summarize potential molecular and cellular mechanisms. Methods and Results. 15 eligible studies with 211 animals (108 received melatonin and 103 received vehicle) were included after searching the databases of PubMed, MEDLINE, Embase, and Cochrane. Pretreatment with melatonin was associated with a significant lower infarct size in comparison with vehicle in myocardial I/R damage (WMD: -20.45, 95% CI: -25.43 to -15.47, p0.001; I2=91.4%, p0.001). Evidence from subgroup analyses and sensitivity analysis indicated the robust and consistent cardioprotective effect of melatonin, while the metaregression also did not unmask any significant interactions between the pooled estimates and covariates (i.e., sample size, state, species, study type, route of administration, and duration of reperfusion, along with timing regimen of pretreatment). Accordingly, melatonin evidently increased EF (WMD: 17.19, 95% CI: 11.08 to 23.29, p0.001; I2=77.0%, p0.001) and FS (WMD: 14.18, 95% CI: 11.22 to 17.15, p0.001; I2=3.5%, p=0.387) in the setting of reperfusion damage. Conclusions. Melatonin preadministration conferred a profound cardioprotection against myocardial I/R injury in preclinical studies.
机译:目标。在临床实践期间,严重缺血后心肌再灌注损伤是一个重要问题。然而,涉及的患病性仍然不清楚,并且还缺乏有效的干预措施。鉴定褪黑激素以施加缓解心肌I / R损伤的保护作用。确定该荟萃分析评估褪黑素处理对再灌注损伤的疗效,并进一步总结潜在的分子和细胞机制。方法和结果。在搜索PubMed,Medline,Embase和Cochrane数据库之后,包括使用211只动物(108种褪黑激素和103辆接收的车辆)的合格研究。与媒体的预处理与近似的梗死尺寸有关,与载体在心肌I / R损伤中(WMD:-20.45,95%CI:-25.43至-15.47,P <0.001; I2 = 91.4%,P <0.001) 。来自亚组分析和敏感性分析的证据表明了褪黑激素的稳健和一致的心脏保护作用,而甲状腺素也没有揭示汇集估计和协变量之间的任何显着相互作用(即样本大小,状态,物种,学习类型,给药途径,和再灌注的持续时间,以及预处理的时序方案)。因此,褪黑素明显增加了EF(WMD:17.19,95%CI:11.08至23.29,P <0.001; I2 = 77.0%,P <0.001)和FS(WMD:14.18,95%CI:11.22至17.15,P <0.001 ; I2 = 3.5%,p = 0.387)在再灌注损伤时。结论。褪黑激素撇草商在临床前研究中赋予了对心肌I / R损伤的深刻心脏保护。

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