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远程心脏保护通过直接外周神经刺激和局部辣椒素实现,其机制是循环体液因子介导的。

Remote cardioprotection by direct peripheral nerve stimulation and topical capsaicin is mediated by circulating humoral factors.

机构信息

Division of Cardiology, Labatt Family Heart Center, Hospital for Sick Children, Toronto, ON, Canada.

出版信息

Basic Res Cardiol. 2012 Mar;107(2):241. doi: 10.1007/s00395-011-0241-5. Epub 2012 Jan 10.

Abstract

We have previously shown that remote ischemic preconditioning by limb ischemia (rIPC) or intra-arterial adenosine releases a dialyzable cardioprotective circulating factor(s), the release of which requires an intact neural connection to the limb and is blocked by pretreatment with S-nitroso-N-acetylpenicillamine (SNAP). Remote cardioprotection can be induced by other forms of peripheral stimulation including topical capsaicin, but the mechanisms of their signal transduction are incompletely understood. Rabbits were anesthetized by intravenous pentobarbital, intubated and ventilated, then randomized (4-7 animals in each group) to receive sham procedure, rIPC (4 cycles of 5 min lower limb ischemia, 5 min reperfusion), direct femoral nerve stimulation, topical capsaicin, pretreatment with intra-arterial SNAP + capsaicin, pretreatment with topical DMSO (a sensory nerve blocker) + topical capsaicin, or pretreatment with intra-arterial SNAP + femoral nerve stimulation, topical DMSO alone, or intra-arterial SNAP alone. Blood was then rapidly drawn from the carotid artery to produce the plasma dialysate which was used to perfuse a naïve heart from an untreated donor rabbit. The infarct size and recovery of LV-developed pressure and end-diastolic pressure were measured after 30 min of global ischemia and 120 min of reperfusion. Compared to sham, dialysate from rIPC, femoral nerve stimulation, and topical capsaicin groups all produced significant cardioprotection with significantly reduced infarct size, and improved the post-ischemic cardiac performance. Cardioprotection was not seen in the topical DMSO-capsaicin, SNAP + capsaicin, and SNAP + FNS groups. These results confirm the central role of peripheral nerves in the local signal transduction of remote cardioprotection. Direct electrical or peripheral neural stimulation evokes the release of cardioprotective substances into the bloodstream, with comparable effects to that of rIPC induced by limb ischemia.

摘要

我们之前已经表明,肢体缺血的远程缺血预处理(rIPC)或动脉内腺苷释放可透析的心脏保护循环因子(s),其释放需要与肢体的完整神经连接,并且可以通过预先用 S-亚硝基-N-乙酰青霉胺(SNAP)处理来阻断。远程心脏保护可以通过其他形式的外周刺激诱导,包括局部辣椒素,但它们的信号转导机制尚不完全清楚。兔子通过静脉注射戊巴比妥麻醉,插管并通气,然后随机(每组 4-7 只动物)接受假手术、rIPC(4 个循环 5 分钟下肢缺血,5 分钟再灌注)、直接股神经刺激、局部辣椒素、动脉内 SNAP+辣椒素预处理、局部 DMSO(感觉神经阻滞剂)+局部辣椒素预处理、或动脉内 SNAP+股神经刺激、局部 DMSO 单独、或动脉内 SNAP 单独预处理。然后迅速从颈总动脉采血产生血浆透析液,用于灌注未经处理的供体兔子的心脏。在 30 分钟的整体缺血和 120 分钟的再灌注后,测量梗死面积和左心室发展压和舒张末期压的恢复。与假手术相比,rIPC、股神经刺激和局部辣椒素组的透析液均产生明显的心脏保护作用,梗死面积显著减小,缺血后心脏功能得到改善。在局部 DMSO-辣椒素、SNAP+辣椒素和 SNAP+FNS 组中未观察到心脏保护作用。这些结果证实了外周神经在远程心脏保护的局部信号转导中的核心作用。直接电刺激或外周神经刺激会将心脏保护物质释放到血液中,其效果与肢体缺血引起的 rIPC 相当。

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