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心脏和血管组织中的β3-肾上腺素能受体:新出现的概念和治疗前景

Beta3-adrenergic receptors in cardiac and vascular tissues emerging concepts and therapeutic perspectives.

作者信息

Dessy Chantal, Balligand Jean-Luc

机构信息

Pole of Pharmacology and Therapeutics, Institute of Experimental and Clinical Research, Université catholique de Louvain, Brussels, Belgium.

出版信息

Adv Pharmacol. 2010;59:135-63. doi: 10.1016/S1054-3589(10)59005-7.

DOI:10.1016/S1054-3589(10)59005-7
PMID:20933201
Abstract

Catecholamines released by the orthosympathetic system play a major role in the short- and long-term regulation of cardiovascular function. Beta1- and beta2-adrenoreceptors (ARs) have classically been considered as mediating most of their effects on cardiac contraction. After their initial cloning and pharmacologic characterization in the late 1980s, beta3-ARs have been mostly thought of as receptors mediating metabolic effects (e.g., lipolysis) in adipocytes. However, definitive evidence for their expression and functional coupling in cardiovascular tissues (including in humans) has recently initiated a re-examination of their implication in the pathophysiology of cardiovascular diseases. Distinctive pharmacodynamic properties of beta3-AR, e.g., their upregulation in disease and resistance to desensitization, suggest that they may be attractive targets for therapeutic intervention. They may substitute efficient vasodilating pathways when beta1/2-ARs are inoperative. In the heart, their contractile effects, which are functionally antipathetic to those of beta1/2-AR, may protect the myocardium against adverse effects of excessive catecholamine stimulation and perhaps mediate additional ancillary effects on key aspects of electrophysiology or remodeling. Longitudinal studies in animals and patients with different stages of heart failure are now needed to identify the optimal therapeutic scheme using specific combinations of agonists or antagonists at all three beta-ARs.

摘要

交感神经系统释放的儿茶酚胺在心血管功能的短期和长期调节中起主要作用。β1和β2肾上腺素能受体(ARs)传统上被认为介导了它们对心脏收缩的大部分作用。20世纪80年代末首次克隆并进行药理学特性鉴定后,β3-ARs大多被认为是介导脂肪细胞代谢效应(如脂肪分解)的受体。然而,最近在心血管组织(包括人类)中其表达和功能偶联的确切证据引发了对其在心血管疾病病理生理学中作用的重新审视。β3-AR独特的药效学特性,如在疾病中的上调和对脱敏的抗性,表明它们可能是有吸引力的治疗干预靶点。当β1/2-ARs不起作用时,它们可能替代有效的血管舒张途径。在心脏中,其收缩作用在功能上与β1/2-AR的作用相反,可能保护心肌免受过多儿茶酚胺刺激的不利影响,或许还介导对电生理学或重塑关键方面的额外辅助作用。现在需要对动物和不同心力衰竭阶段的患者进行纵向研究,以确定使用针对所有三种β-AR的激动剂或拮抗剂的特定组合的最佳治疗方案。

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