Adhesion G Protein-Coupled Receptors as Drug Targets for Neurological Diseases

Christopher J. Folts; Stefanie Giera; Tao Li; Xianhua Piao

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Adhesion G Protein-Coupled Receptors as Drug Targets for Neurological Diseases

机译：粘附G蛋白偶联受体作为神经疾病的药物靶标

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The family of adhesion G protein-coupled receptors (aGPCRs) consists of 33 members in humans. Although the majority are orphan receptors with unknown functions, many reports have demonstrated critical functions for some members of this family in organogenesis, neurodevelopment, myelination, angiogenesis, and cancer progression. Importantly, mutations in several aGPCRs have been linked to human diseases. The crystal structure of a shared protein domain, the GPCR Autoproteolysis INducing (GAIN) domain, has enabled the discovery of a common signaling mechanism – a tethered agonist – for this class of receptors. A series of recent reports has shed new light on their biological functions and disease relevance. This review focuses on these recent advances in our understanding of aGPCR biology in the nervous system and the untapped potential of aGPCRs as novel therapeutic targets for neurological disease.

机译：粘附性G蛋白偶联受体（AGPCR）的家族由33个人组成。虽然大多数是具有未知功能的孤儿受体，但许多报告已经表现出该家庭中某些成员的关键职能，在有机组织中，神经发育，髓鞘，血管生成和癌症进展。重要的是，几种AGPCR中的突变与人类疾病有关。共用蛋白质结构域的晶体结构，GPCR自蛋白酶诱导（增益）域，使得能够发现常见的信号调制机制 - 拴系激动剂 - 对于这类受体。一系列最近的报告对其生物功能和疾病相关性阐述了新的光线。本综述重点介绍了我们对神经系统中AGPCR生物学的理解以及AGPCR作为神经疾病的新治疗目标的未开发潜力。

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《Trends in pharmacological sciences》 |2019年第4期|共16页
作者
Christopher J. Folts; Stefanie Giera; Tao Li; Xianhua Piao;
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作者单位

Division of Newborn Medicine Department of Medicine Children’s Hospital and Harvard Medical School;

Division of Newborn Medicine Department of Medicine Children’s Hospital and Harvard Medical School;

Division of Newborn Medicine Department of Medicine Children’s Hospital and Harvard Medical School;

Division of Newborn Medicine Department of Medicine Children’s Hospital and Harvard Medical School;

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原文格式 PDF
正文语种 eng
中图分类药理学;
关键词
adhesion G protein-coupled receptors; GPCR Autoproteolysis INducing domain; GAIN domain; neurological disease; neurodevelopment;

机译：粘附G蛋白偶联受体;GPCR自海外溶解域;增益域;神经病;神经发育;

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1. Adhesion G Protein-Coupled Receptors as Drug Targets for Neurological Diseases [J] . Christopher J. Folts, Stefanie Giera, Tao Li, Trends in pharmacological sciences . 2019,第4期

机译：粘附G蛋白偶联受体作为神经疾病的药物靶标
2. G protein-coupled receptors as potential drug targets for lymphangiogenesis and lymphatic vascular diseases. [J] . Dunworth WP, Caron KM Arteriosclerosis, thrombosis, and vascular biology . 2009,第5期

机译：G蛋白偶联受体作为淋巴管生成和淋巴管疾病的潜在药物靶标。
3. Regulated expression of pH sensing G protein-coupled receptor-68 identified through chemical biology defines a new drug target for ischemic heart disease [J] . Russell J.L., Goetsch S.C., Aguilar H.R., ACS Chemical Biology . 2012,第6期

机译：通过化学生物学鉴定的pH感应G蛋白偶联受体68的调节表达确定了缺血性心脏病的新药物靶标
4. Mutations in G proteins and G protein-coupled receptors in human endocrine diseases [C] . Allen Spiege Colloque me?decine et recherche . 2006

机译：在人内分泌疾病中G蛋白和G蛋白偶联受体中的突变
5. Vascular drug targeting: Engineered poly(ethylene glycol) microparticle surfaces modulate receptor-specific adhesion. [D] . Ham, Anthony Sang Won. 2006

机译：靶向血管药物：工程化的聚乙二醇微粒表面可调节受体特异性粘附。
6. Regulated expression of pH sensing G protein-coupled receptor-68 identified through chemical biology defines a new drug target for ischemic heart disease [O] . Jamie L. Russell, Sean C. Goetsch, Hector R. Aguilar, -1

机译：的调节表达的pH感测G蛋白偶联受体68通过化学生物学标识定义一个新的药物靶标缺血性心脏疾病
7. Adhesion G Protein-Coupled Receptors as Drug Targets for Neurological Diseases [O] . Christopher J. Folts, Stefanie Giera, Tao Li, 2019

机译：粘附G蛋白偶联受体作为神经疾病的药物靶标

Adhesion G Protein-Coupled Receptors as Drug Targets for Neurological Diseases

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