α1-Adrenergic Receptors Control the Activity of Sinoatrial Node by Modulating Transmembrane Transport of Chloride Anions

IF 1.1 Q4 CELL BIOLOGY

Biochemistry (Moscow), Supplement Series A: Membrane and Cell Biology Pub Date : 2024-01-17 DOI:10.1134/S1990747823070061

Y. A. Voronina, A. V. Fedorov, M. A. Chelombitko, U. E. Piunova, V. S. Kuzmin

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Abstract

Norepinephrine (NE), which is released by sympathetic nerve endings, causes an increase in the frequency of spontaneous action potentials in the pacemaker cardiomyocytes of the sinoatrial node (SAN) of the heart. This results in an increase in heart rate (HR). Two types of postsynaptic adrenoreceptors (ARs), α1-AR and β-AR, mediate the effects of NE. The role of α1-AR in the sympathetic control of heart rate and SAN automaticity, as well as the membrane mechanisms involved in α1-AR-mediated pacemaker control, have not yet been elucidated. In this study, we utilized immunofluorescence confocal microscopy to examine the distribution of α1A-AR in the SAN of rats. Additionally, we assessed the expression of α1A-AR mRNA in the SAN tissue using RT-PCR. Furthermore, we investigated the impact of α1-AR stimulation on key functional parameters of the pacemaker, including the corrected sinus node recovery time (SNRT/cSNRT) and the SAN accommodation, using the Langendorff perfused heart technique. We also used optical mapping of the electrical activity of perfused, isolated tissue preparations to study the effect of α1-AR stimulation on the spatiotemporal characteristics of SAN excitation. We tested the effects of chloride transmembrane conductance blockade on alteration of functional parameters and pattern of SAN excitation caused by α1-AR. Fluorescent signals corresponding to α1A-AR have been identified in SAN cardiomyocytes, indicating the presence of α1A-AR at protein level. The expression of α1A-AR in SAN has been also confirmed at the mRNA level. The stimulation of α1-AR affects SAN functioning. Phenylephrine (PHE) utilized as α1A-AR agonist caused a decrease in SNRT/cSNRT, as well as an acceleration of SAN accommodation. These effects were rate dependent and were observed in a high frequency range of pacemaker tissue stimulation. PHE induces changes in the excitation pattern of the SAN. The effects of PHE on functional parameters and SAN excitation pattern are attenuated by Ca²⁺-dependent chloride channel blocker NPPB but remains unaffected by the protein kinase C inhibitor BIM. Our results suggest that cardiac α1-ARs are important for maintaining function of SAN pacemaker at high heart rates and that α1-AR signalling cascades in the SAN by targeting Ca²⁺-dependent chloride channels are involved in the α1-adrenergic modulation of the electrophysiological properties of the heart pacemaker.

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α1-肾上腺素能受体通过调节氯离子的跨膜转运控制心房结的活动

摘要由交感神经末梢释放的去甲肾上腺素（NE）会导致心脏中心房结（SAN）的起搏心肌细胞自发动作电位频率增加。这导致心率（HR）增加。两种突触后肾上腺素受体（AR）--α1-AR 和 β-AR--介导 NE 的作用。α1-AR在交感神经控制心率和SAN自动性中的作用以及α1-AR介导的起搏器控制所涉及的膜机制尚未阐明。在本研究中，我们利用免疫荧光共聚焦显微镜检查了大鼠 SAN 中 α1A-AR 的分布。此外，我们还利用 RT-PCR 评估了 α1A-AR mRNA 在 SAN 组织中的表达。此外，我们还使用 Langendorff 灌注心脏技术研究了 α1-AR 刺激对起搏器关键功能参数的影响，包括校正窦房结恢复时间（SNRT/cSNRT）和 SAN 容积。我们还利用灌注分离组织制备的电活动光学图谱来研究α1-AR刺激对SAN兴奋时空特征的影响。我们测试了氯跨膜传导阻滞对α1-AR引起的SAN兴奋的功能参数和模式改变的影响。在SAN心肌细胞中发现了与α1A-AR相对应的荧光信号，表明α1A-AR在蛋白水平上的存在。α1A-AR在SAN中的表达也在mRNA水平上得到了证实。α1-AR 的刺激会影响 SAN 的功能。苯肾上腺素（PHE）作为α1A-AR 激动剂可导致 SNRT/cSNRT 下降，并加速 SAN 的容纳。这些效应与速率有关，并在起搏器组织刺激的高频率范围内观察到。PHE 可诱导 SAN 兴奋模式的改变。Ca2+依赖性氯离子通道阻滞剂NPPB可减弱PHE对功能参数和SAN兴奋模式的影响，而蛋白激酶C抑制剂BIM则不受影响。我们的研究结果表明，心脏α1-AR 对维持高心率下 SAN 起搏器的功能非常重要，α1-AR 信号级联通过靶向 Ca2+ 依赖性氯离子通道参与了α1-肾上腺素能对心脏起搏器电生理特性的调节。

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来源期刊

Biochemistry (Moscow), Supplement Series A: Membrane and Cell Biology CELL BIOLOGY-

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1.40

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0.00%

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期刊介绍： Biochemistry (Moscow), Supplement Series A: Membrane and Cell Biology is an international peer reviewed journal that publishes original articles on physical, chemical, and molecular mechanisms that underlie basic properties of biological membranes and mediate membrane-related cellular functions. The primary topics of the journal are membrane structure, mechanisms of membrane transport, bioenergetics and photobiology, intracellular signaling as well as membrane aspects of cell biology, immunology, and medicine. The journal is multidisciplinary and gives preference to those articles that employ a variety of experimental approaches, basically in biophysics but also in biochemistry, cytology, and molecular biology. The journal publishes articles that strive for unveiling membrane and cellular functions through innovative theoretical models and computer simulations.