通过β2-肾上腺素能受体的β-抑制蛋白偏向性信号传导促进心肌细胞收缩。
β-arrestin-biased signaling through the β2-adrenergic receptor promotes cardiomyocyte contraction.
作者信息
Carr Richard, Schilling Justin, Song Jianliang, Carter Rhonda L, Du Yang, Yoo Sungsoo M, Traynham Christopher J, Koch Walter J, Cheung Joseph Y, Tilley Douglas G, Benovic Jeffrey L
机构信息
Department of Biochemistry and Molecular Biology, Thomas Jefferson University, Philadelphia, PA 19107;
Department of Pharmacology, Center for Translational Medicine, Temple University School of Medicine, Philadelphia, PA 19140;
出版信息
Proc Natl Acad Sci U S A. 2016 Jul 12;113(28):E4107-16. doi: 10.1073/pnas.1606267113. Epub 2016 Jun 27.
β-adrenergic receptors (βARs) are critical regulators of acute cardiovascular physiology. In response to elevated catecholamine stimulation during development of congestive heart failure (CHF), chronic activation of Gs-dependent β1AR and Gi-dependent β2AR pathways leads to enhanced cardiomyocyte death, reduced β1AR expression, and decreased inotropic reserve. β-blockers act to block excessive catecholamine stimulation of βARs to decrease cellular apoptotic signaling and normalize β1AR expression and inotropy. Whereas these actions reduce cardiac remodeling and mortality outcomes, the effects are not sustained. Converse to G-protein-dependent signaling, β-arrestin-dependent signaling promotes cardiomyocyte survival. Given that β2AR expression is unaltered in CHF, a β-arrestin-biased agonist that operates through the β2AR represents a potentially useful therapeutic approach. Carvedilol, a currently prescribed nonselective β-blocker, has been classified as a β-arrestin-biased agonist that can inhibit basal signaling from βARs and also stimulate cell survival signaling pathways. To understand the relative contribution of β-arrestin bias to the efficacy of select β-blockers, a specific β-arrestin-biased pepducin for the β2AR, intracellular loop (ICL)1-9, was used to decouple β-arrestin-biased signaling from occupation of the orthosteric ligand-binding pocket. With similar efficacy to carvedilol, ICL1-9 was able to promote β2AR phosphorylation, β-arrestin recruitment, β2AR internalization, and β-arrestin-biased signaling. Interestingly, ICL1-9 was also able to induce β2AR- and β-arrestin-dependent and Ca(2+)-independent contractility in primary adult murine cardiomyocytes, whereas carvedilol had no efficacy. Thus, ICL1-9 is an effective tool to access a pharmacological profile stimulating cardioprotective signaling and inotropic effects through the β2AR and serves as a model for the next generation of cardiovascular drug development.
β-肾上腺素能受体(βARs)是急性心血管生理的关键调节因子。在充血性心力衰竭(CHF)发展过程中,对升高的儿茶酚胺刺激作出反应时,Gs依赖性β1AR和Gi依赖性β2AR途径的慢性激活会导致心肌细胞死亡增加、β1AR表达降低和心肌收缩储备减少。β受体阻滞剂的作用是阻断儿茶酚胺对βARs的过度刺激,以减少细胞凋亡信号,并使β1AR表达和心肌收缩力正常化。虽然这些作用可减少心脏重塑和死亡率,但效果并不持久。与G蛋白依赖性信号传导相反,β-arrestin依赖性信号传导可促进心肌细胞存活。鉴于CHF中β2AR表达未改变,通过β2AR起作用的β-arrestin偏向性激动剂代表了一种潜在有用的治疗方法。卡维地洛是目前处方的非选择性β受体阻滞剂,已被归类为β-arrestin偏向性激动剂,可抑制βARs的基础信号传导,并刺激细胞存活信号通路。为了了解β-arrestin偏向性对选定β受体阻滞剂疗效的相对贡献,使用了一种针对β2AR细胞内环(ICL)1-9的特异性β-arrestin偏向性肽模拟物,以将β-arrestin偏向性信号传导与正构配体结合口袋的占据解耦。ICL1-9具有与卡维地洛相似的功效,能够促进β2AR磷酸化、β-arrestin募集、β2AR内化和β-arrestin偏向性信号传导。有趣的是,ICL1-9还能够在原代成年小鼠心肌细胞中诱导β2AR和β-arrestin依赖性且不依赖Ca(2+)的收缩力,而卡维地洛则无效。因此,ICL1-9是一种有效的工具,可通过β2AR获得刺激心脏保护信号和心肌收缩力的药理学特征,并作为下一代心血管药物开发的模型。
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