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跳出“RGS 框框”思维:靶向 G 蛋白信号转导调节剂的治疗新方法。

Thinking outside of the "RGS box": new approaches to therapeutic targeting of regulators of G protein signaling.

机构信息

Department of Pharmacology, University of Michigan, 1150 W Medical Center Dr, MSRB III, Ann Arbor, MI 48109, USA.

出版信息

Mol Pharmacol. 2010 Oct;78(4):550-7. doi: 10.1124/mol.110.065219. Epub 2010 Jul 27.

Abstract

Regulators of G protein signaling (RGS) proteins are emerging as potentially important drug targets. The mammalian RGS protein family has more than 20 members and they share a common ∼120-residue RGS homology domain or "RGS box." RGS proteins regulate signaling via G protein-coupled receptors by accelerating GTPase activity at active α subunits of G proteins of the G(q) and G(i/o) families. Most studies searching for modulators of RGS protein function have been focused on inhibiting the GTPase accelerating protein activity. However, many RGS proteins contain additional domains that serve other functions, such as interactions with proteins or subcellular targeting. Here, we discuss a rationale for therapeutic targeting of RGS proteins by regulation of expression or allosteric modulation to permit either increases or decreases in RGS function. Several RGS proteins have reduced expression or function in pathophysiological states, so strategies to increase RGS function would be useful. Because several RGS proteins are rapidly degraded by the N-end rule pathway, finding ways to stabilize them may prove to be an effective way to enhance RGS protein function.

摘要

G 蛋白信号转导调节因子(RGS)蛋白正在成为潜在的重要药物靶点。哺乳动物 RGS 蛋白家族有 20 多个成员,它们共享一个共同的约 120 个残基的 RGS 同源结构域或“RGS 盒”。RGS 蛋白通过加速 G(q)和 G(i/o)家族中活性 G 蛋白 α 亚基的 GTP 酶活性来调节通过 G 蛋白偶联受体的信号。大多数研究寻找 RGS 蛋白功能调节剂的研究都集中在抑制 GTP 酶加速蛋白活性上。然而,许多 RGS 蛋白包含其他结构域,用于发挥其他功能,例如与蛋白质相互作用或亚细胞靶向。在这里,我们讨论了通过调节表达或变构调节来治疗性靶向 RGS 蛋白的基本原理,以允许 RGS 功能的增加或减少。在病理生理状态下,几种 RGS 蛋白的表达或功能降低,因此增加 RGS 功能的策略将是有用的。由于几种 RGS 蛋白被 N 端规则途径快速降解,因此找到稳定它们的方法可能被证明是增强 RGS 蛋白功能的有效方法。

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