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前列腺素 EP4 受体及其信号通路。

The prostanoid EP4 receptor and its signaling pathway.

机构信息

Cardiovascular Research Institute, Yokohama City University, Yokohama, Kanagawa, Japan.

出版信息

Pharmacol Rev. 2013 Jun 17;65(3):1010-52. doi: 10.1124/pr.112.007195. Print 2013 Jul.

Abstract

The EP4 prostanoid receptor is one of four receptor subtypes for prostaglandin E2. It belongs to the family of G protein-coupled receptors. It was originally identified, similar to the EP2 receptor as a G(s)α-coupled, adenylyl cyclase-stimulating receptor. EP4 signaling plays a variety of roles through cAMP effectors, i.e., protein kinase A and exchange protein activated by cAMP. However, emerging evidence from studies using pharmacological approaches and genetically modified mice suggests that EP4, unlike EP2, can also be coupled to G(i)α, phosphatidylinositol 3-kinase, β-arrestin, or β-catenin. These signaling pathways constitute unique roles for the EP4 receptor. EP4 is widely distributed in the body and thus plays various physiologic and pathophysiologic roles. In particular, EP4 signaling is closely related to carcinogenesis, cardiac hypertrophy, vasodilation, vascular remodeling, bone remodeling, gastrointestinal homeostasis, renal function, and female reproductive function. In addition to the classic anti-inflammatory action of EP4 on mononuclear cells and T cells, recent evidence has shown that EP4 signaling contributes to proinflammatory action as well. The aim of this review is to present current findings on the biologic functions of the EP4 receptor. In particular, we will discuss its diversity from the standpoint of EP4-mediated signaling.

摘要

EP4 前列腺素受体是前列腺素 E2 的四个受体亚型之一。它属于 G 蛋白偶联受体家族。最初与 EP2 受体一样,它被鉴定为 G(s)α 偶联、腺苷酸环化酶刺激受体。EP4 信号通过 cAMP 效应物(即蛋白激酶 A 和 cAMP 激活的交换蛋白)发挥多种作用。然而,使用药理学方法和基因修饰小鼠进行的研究提供的新证据表明,与 EP2 不同,EP4 也可以与 G(i)α、磷脂酰肌醇 3-激酶、β-抑制蛋白或 β-连环蛋白偶联。这些信号通路构成了 EP4 受体的独特作用。EP4 在体内广泛分布,因此发挥着各种生理和病理生理作用。特别是,EP4 信号与致癌作用、心肌肥大、血管舒张、血管重塑、骨重塑、胃肠道稳态、肾功能和女性生殖功能密切相关。除了 EP4 对单核细胞和 T 细胞的经典抗炎作用外,最近的证据表明 EP4 信号也有助于促炎作用。本综述的目的是介绍 EP4 受体的生物学功能的最新发现。特别是,我们将从 EP4 介导的信号的角度讨论其多样性。

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