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Regulation of the NRG1/ErbB4 Pathway in the Intrinsic Cardiac Nervous System Is a Potential Treatment for Atrial Fibrillation

机译:内在神经神经系统中的NRG1 / ErbB4通路的调节是房颤的潜在治疗方法。

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摘要

>Background: The NRG1/ErbB4 signaling mechanism has been widely studied in the central nervous system for many years. However, the role of this pathway in modulating the intrinsic cardiac nervous system is largely unknown.>Objective: The present study investigated whether the NRG1/ErbB4 signaling system affects the activity of major atrial ganglionated plexi (GP) in a paroxysmal atrial fibrillation (AF) model by 6-h rapid atrial pacing (RAP).>Methods: Twenty-four dogs were randomly divided into (1) a control group (saline microinjections into GP), (2) RAP group (saline microinjections into GP plus 6 h-RAP), (3) NRG1 group (microinjections of neuregulin-1 into GP plus 6 h-RAP) and (4) NRG1 + ERA group (microinjections of neuregulin-1 and ErbB4 receptor antagonist-ERA into GP plus 6 h-RAP). The effective refractory period (ERP), window of vulnerability (WOV), anterior right GP (ARGP) function and neural activity were measured. ARGP tissues were excised for histological study and western blotting.>Results: When compared to the control group, 6 h-RAP produced a significant (1) decrease in ERP, an increase in ΣWOV, (2) an increase in ARGP neural activity and neural function, and (3) an increase in c-fos and nerve growth factor protein expression in the ARGP. However, microinjection of NRG1 into the ARGP prior to RAP prevented ERP shortening and AGRP activity enhancement and inhibited the expression of c-Fos and NGF proteins. Furthermore, these changes were significantly attenuated by pretreatment with an ErbB4 receptor antagonist.>Conclusion: The NRG1/ErbB4 signaling pathway may exist in the GP, and activation of this pathway suppressed RAP-induced GP activation, atrial electrical remodeling and AF.
机译:>背景:NRG1 / ErbB4信号传导机制已在中枢神经系统中广泛研究了很多年。然而,该途径在调节内源性心脏神经系统中的作用尚不清楚。>目的:本研究调查了NRG1 / ErbB4信号传导系统是否影响了主要心房神经节丛(GP)的活动。通过6小时快速心房起搏(RAP)建立阵发性心房颤动(AF)模型。>方法:将24只狗随机分为(1)对照组(盐水微注射入GP),( 2)RAP组(盐水微注射入GP加6 h-RAP),(3​​)NRG1组(神经调节素-1注射到GP加6 h-RAP)和(4)NRG1 + ERA组(显微注射neuregulin-1和ErbB4受体拮抗剂-ERA加GP加6 h-RAP)。测量有效不应期(ERP),脆弱性窗口(WOV),右前GP(ARGP)功能和神经活动。切除了ARGP组织用于组织学研究和Western blotting。>结果:与对照组相比,6 h-RAP导致(1)的ERP显着下降,(ΣWOV的增加)(2) ARGP神经活动和神经功能增加;(3)ARGP中c-fos和神经生长因子蛋白表达增加。但是,在RAP之前向ARGP中微量注射NRG1可以防止ERP缩短和AGRP活性增强,并抑制c-Fos和NGF蛋白的表达。此外,通过用ErbB4受体拮抗剂进行预处理,这些改变被显着减弱。重塑和自动对焦。

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