后肢远程预处理对心肌缺血再灌注与心交感神经损伤的影响

目的:后肢远程缺血预处理对急性心肌缺血再灌注与心交感神经损伤影响的实验研究。方法:20只雄性新西兰大白兔随机被均分成两组:对照组及远程缺血预处理(RIPC)组。两组均制作心肌缺血模型。RIPC组在心肌缺血前行双后肢短暂缺血预处理2次(充气式压力止血带环扎双后肢腘窝上1/3,压力26.6 kPa,每次10 min,间隔10 min),最后一次后肢缺血预处理后再灌注60 min制作急性心肌缺血模型。其方法为:冠状动脉左前降支完全闭塞45 min,于松开结扎圈再灌注2、4 h时,分别以131碘-间位碘代苄胍(131I-MIBG)、99m锝-甲氧基异丁基异腈(99mTc-MIBI)双核素作放射自显影,其后以美蓝、氯化四唑(TTC)作组织染色,分别确定心肌危险梗塞灶与实际梗塞灶。结果:再灌注4h后,预处理组危险梗塞灶与实际梗塞灶均小于对照组(P<0.01)。131I-MIBG及99mTc-MIBI自显影在同一区域摄取存在差异性,两组131I-MIBG显影缺损面积(40.8±3.2)%,均显著比99mTc-MIBI显影缺损及实际梗塞灶大(P<0.05)。结论:远程预处理能有效阻断心肌缺血再灌注对交感神经损伤的作用;利用交感神经显影剂MIBG显影能客观监测心肌梗塞病变范围和程度,评价远程预处理的心肌保护效应。

Cardiac Remote Conditioning and Clinical Relevance:All Together Now!

Acute myocardial infarction （AMI） is the leading cause of death and disability worldwide. Timely reperfusion is the standard of care and results in decreased infarct size, improving patient survival and prognosis. However, 25% of patients proceed to develop heart failure （HF） after myocardial infarction （MI） and 50% of these will die within five years. Since the size of the infarct is the major predictor of the outcome, including the development of HF, therapies to improve myocardial salvage have great potential. Over the past three decades, a number of stimuli have been discovered that activate endogenous cardioprotective pathways. In ischemic preconditioning （IPC） and ischemic postconditioning, ischemia within the heart initiates the protection. Brief reversible episodes of ischemia in vascular beds remote from the heart can also trigger cardioprotection when applied before, during, or immediately after myocardial ischemia-- known as remote ischemic pre-, per-, and post-conditioning, respectively. Although the mechanism of remote ischemic preconditioning （RIPC） has not yet been fully elucidated, many mechanistic components are shared with IPC. The discovery of RIPC led to research into the use of remote non-ischemic stimuli including nerve stimulation （spinal and vagal）, and electroacupuncture （EA）. We discovered and, with others, have elucidated mechanistic aspects of a non- ischemic phenomenon we termed remote preconditioning of trauma （RPCT）. RPCT operates via neural stimulation of skin sensory nerves and has similarities and differences to nerve stimulation and EA conducted at acupoints. We show herein that RPCT can be mimicked using electrical stimulation of the abdominal midline （EA-like treatment） and that this modality of activating cardioprotection is powerful as both a preconditioning and a postconditioning stimulus （when applied at reperfusion）. Investigations of these cardioprotective phenomena have led to a more integrative understanding of mechanisms related to cardioprotection, and in the last five to ten years, it has become clear that the mechanisms are similar, whether induced by ischemic or non-ischemic stimuli. Taking together much of the data in the literature, we propose that all of these cardioprotective ＂conditioning＂ phenomena represent activation from different entry points of a cardiac conditioning network that converges upon specific mediators and effectors of myocardial cell survival, including NF-KB, Stat3/5, protein kinase C, bradykinin, and the mitoKA^P channel. Nervous system pathways may represent a novel mechanism for initiating conditioning of the heart and other organs. IPC and RIPC have proven difficult to translate clinically, as they have associated risks and cannot be used in some patients. Because of this, the use of neural and nociceptive stimuli is emerging as a potential non-ischemic and non-traumatic means to initiate cardiac conditioning. Clinical relevance is underscored by the demonstration of postconditioning with one of these modalities, supporting the conclusion that the development of pharmaceuticals and electroceuticals for this purpose is an area ripe for clinical development.