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Isoflurane post-conditioning stimulates the proliferative phase of myocardial recovery in an ischemia-reperfusion model of heart injury in rats

机译:异氟烷后处理可在大鼠心脏缺血/再灌注模型中刺激心肌恢复的增殖期

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The application of isoflurane in a post-conditioning manner, during early reperfusion following a period of coronary occlusion, has numerous beneficial effects on the ischemic myocardium, including reduction of infarct size. It does so by stimulating a sequence of well studied anti-apoptotic pro-survival mechanisms in a similar manner to various 'ischemic' pre-/post-conditioning approaches which achieve their cardio protective effects in both laboratory and clinical situations. Proliferation of newly formed blood vessels, resulting in formation of highly vascularized granulation tissue, is an essential stage of infarct healing. It can be evaluated by detecting various angiogenic factors, including vascular endothelial growth factor (VEGF) and platelet endothelial cell adhesion molecule-1 (PECAM-1/CD31) or by quantification of expression of vascular smooth muscle progenitors, such as Nestin. Expression of these three markers was used to evaluate the effect of early isoflurane post-conditioning in ischemia-reperfusion type cardiac injury. A large reduction in infarct size (59.3% of control), and marked increase of expression of VEGF (43.4%), PECAM-1/CD31 (136%) and Nestin (77.9%) was found in experimental animals when compared to control animals that did not receive isoflurane treatment. Hence, based on our results, we can emphasize two morphologically detectable benefits of isoflurane post-conditioning: a marked reduction in infarct size and much better organization/vascularization of necrotic tissue.
机译:在冠状动脉闭塞一段时间后的早期再灌注过程中,以异氟烷后处理的方式对缺血性心肌具有许多有益的作用,包括减少梗塞面积。它是通过刺激一系列经过充分研究的抗凋亡促生存机制来实现的,类似于各种“缺血性”预处理/后处理方法,这些方法可在实验室和临床情况下实现其心脏保护作用。新形成的血管的增殖,导致高度血管化的肉芽组织的形成,是梗塞愈合的重要阶段。可以通过检测各种血管生成因子(包括血管内皮生长因子(VEGF)和血小板内皮细胞粘附分子1(PECAM-1 / CD31))或量化血管平滑肌祖细胞(如Nestin)的表达来进行评估。这三种标记物的表达被用于评估早期异氟烷后处理在缺血再灌注型心脏损伤中的作用。与对照动物相比,在实验动物中发现梗死面积大大减少(占对照的59.3%),并显着增加了VEGF(43.4%),PECAM-1 / CD31(136%)和Nestin(77.9%)的表达。没有接受异氟烷治疗。因此,基于我们的结果,我们可以强调异氟烷后处理的两种形态学可检测的好处:梗死面积的明显减少和坏死组织的更好的组织/血管形成。

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