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胆碱能神经支配与RGS2在房性心律失常中的作用。

Role of Cholinergic Innervation and RGS2 in Atrial Arrhythmia.

作者信息

Jones Douglas L, Tuomi Jari M, Chidiac Peter

机构信息

Department of Physiology and Pharmacology, The University of  Western Ontario London, ON, Canada.

出版信息

Front Physiol. 2012 Jun 29;3:239. doi: 10.3389/fphys.2012.00239. eCollection 2012.

Abstract

The heart receives sympathetic and parasympathetic efferent innervation as well as the ability to process information internally via an intrinsic cardiac autonomic nervous system (ICANS). For over a century, the role of the parasympathetics via vagal acetylcholine release was related to controlling primarily heart rate. Although in the late 1800s shown to play a role in atrial arrhythmia, the myocardium took precedence from the mid-1950s until in the last decade a resurgence of interest in the autonomics along with signaling cascades, regulators, and ion channels. Originally ignored as being benign and thus untreated, recent emphasis has focused on atrial arrhythmia as atrial fibrillation (AF) is the most common arrhythmia seen by the general practitioner. It is now recognized to have significant mortality and morbidity due to resultant stroke and heart failure. With the aging population, there will be an unprecedented increased burden on health care resources. Although it has been known for more than half a century that cholinergic stimulation can initiate AF, the classical concept focused on the M2 receptor and its signaling cascade including RGS4, as these had been shown to have predominant effects on nodal function (heart rate and conduction block) as well as contractility. However, recent evidence suggests that the M3 receptor may also playa role in initiation and perpetuation of AF and thus RGS2, a putative regulator of the M3 receptor, may be a target for therapeutic intervention. Mice lacking RGS2 (RGS2(-/-)), were found to have significantly altered electrophysiological atrial responses and were more susceptible to electrically induced AF. Vagally induced or programmed stimulation-induced AF could be blocked by the selective M3R antagonist, darifenacin. These results suggest a potential surgical target (ICANS) and pharmacological targets (M3R, RGS2) for the management of AF.

摘要

心脏接受交感神经和副交感神经传出神经支配,并且能够通过心脏固有自主神经系统(ICANS)在内部处理信息。一个多世纪以来,副交感神经通过迷走神经释放乙酰胆碱的作用主要与控制心率有关。尽管在19世纪后期已证明其在房性心律失常中起作用,但从20世纪50年代中期到过去十年,随着对自主神经系统以及信号级联、调节因子和离子通道兴趣的复苏,心肌成为研究重点。最初,由于被认为是良性的而被忽视且未得到治疗,最近的重点已集中在房性心律失常上,因为心房颤动(AF)是全科医生所见最常见的心律失常。现在人们认识到,由于由此导致的中风和心力衰竭,它具有显著的死亡率和发病率。随着人口老龄化,医疗保健资源将面临前所未有的负担增加。尽管半个多世纪以来人们就知道胆碱能刺激可引发房颤,但经典概念集中在M2受体及其信号级联,包括RGS4,因为这些已被证明对节点功能(心率和传导阻滞)以及收缩性有主要影响。然而,最近的证据表明,M3受体也可能在房颤的起始和持续中起作用,因此RGS2,一种假定的M3受体调节因子,可能是治疗干预的靶点。发现缺乏RGS2(RGS2(-/-))的小鼠具有明显改变的心房电生理反应,并且更容易发生电诱导的房颤。选择性M3R拮抗剂达非那新可阻断迷走神经诱导或程控刺激诱导的房颤。这些结果提示了用于房颤治疗的潜在手术靶点(ICANS)和药理学靶点(M3R、RGS2)。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7da6/3386567/4a84b5db38a9/fphys-03-00239-g001.jpg

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