The role of 17-beta estradiol in ischemic preconditioning protection of the heart.

Experimental & Clinical Cardiology Pub Date : 2012-09-01

Fawzi A Babiker, Lamia J Hoteit, Shaji Joseph, Abu Salim Mustafa, Jasbir S Juggi

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Abstract

Background: The protective effects of 17-beta estradiol (E2) on cardiac tissue during ischemia/reperfusion (I/R) injury have not yet been fully elucidated.

Objective: To assess the protective effects of short- and long-term E2 treatments on cardiac tissue exposed to I/R, and to assess the effects of these treatments in combination with ischemic preconditioning (IPC) on cardiac protection from I/R injury.

Methods: SPRAGUE DAWLEY RATS WERE ASSIGNED TO THE FOLLOWING TREATMENT PROTOCOLS: control (no preconditioning); IPC (isolated hearts were subjected to two cycles of 5 min global ischemia followed by 10 min of reperfusion); E2 preconditioning (E2PC; isolated hearts were subjected to E2 pharmacological perfusion for 15 min); short-term in vivo E2 pretreatment for 3 h; long-term in vivo E2 pretreatment or withdrawal (ovariectomy followed by a six-week treatment with E2 or a placebo); combined IPC and E2PC; combined IPC and short- or long-term E2 pretreatments or withdrawal. All hearts were isolated and stabilized for at least 30 min before being subjected to 40 min of global ischemia followed by 30 min of reperfusion; left ventricular function and vascular hemodynamics were then assessed.

Results: IPC, E2PC and short-term E2 pretreatment led to the recovery of left ventricle function and vascular hemodynamics. Long-term E2 and placebo treatments did not result in any protection compared with untreated controls. The combination of E2PC or short-term E2 treatments with IPC did not block the IPC protection or result in any additional protection to the heart. Long-term E2 treatment blocked IPC protection; however, placebo treatment did not.

Conclusions: Short-term treatment with E2 protected the heart against I/R injury through a pathway involving the regulation of tumour necrosis factor-alpha. The combination of short-term E2 treatment with IPC did not provide additional protection to the heart. Short-term E2 treatment may be a suitable alternative for classical estrogen replacement therapy.

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17- β雌二醇在心脏缺血预处理保护中的作用。

背景:17- β雌二醇(E2)对缺血/再灌注(I/R)损伤心肌组织的保护作用尚未完全阐明。目的:评价短期和长期E2处理对I/R损伤心脏组织的保护作用，并评价这些处理联合缺血预处理(IPC)对I/R损伤心脏的保护作用。方法:将SPRAGUE DAWLEY大鼠分为以下治疗方案:对照组(无预处理);IPC(离体心脏进行5分钟全脑缺血和10分钟再灌注两个周期);E2预处理(E2PC;离体心脏E2药理灌注15 min;短期体内E2预处理3小时;长期体内E2预处理或停药(卵巢切除术后用E2或安慰剂治疗6周);IPC和E2PC的结合;联合IPC和短期或长期E2预处理或停药。所有心脏均被分离并稳定至少30分钟，然后进行40分钟的全身缺血和30分钟的再灌注;然后评估左心室功能和血管血流动力学。结果:IPC、E2PC和短期E2预处理均能恢复左心室功能和血管血流动力学。与未治疗的对照组相比，长期E2和安慰剂治疗没有产生任何保护作用。E2PC或短期E2与IPC联合治疗不会阻断IPC保护或导致对心脏的任何额外保护。长期E2处理阻断IPC保护;然而，安慰剂治疗没有。结论:短期E2治疗可通过调节肿瘤坏死因子- α通路保护心脏免受I/R损伤。短期E2治疗与IPC联合治疗对心脏没有额外的保护作用。短期E2治疗可能是经典雌激素替代疗法的合适选择。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Experimental & Clinical Cardiology CARDIAC & CARDIOVASCULAR SYSTEMS-

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6-12 weeks