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将黑皮质素受体作为潜在的新型治疗靶点。

Targeting melanocortin receptors as potential novel therapeutics.

作者信息

Getting Stephen J

机构信息

The William Harvey Research Institute, Charterhouse Square, London, EC1M 6BQ, United Kingdom.

出版信息

Pharmacol Ther. 2006 Jul;111(1):1-15. doi: 10.1016/j.pharmthera.2005.06.022. Epub 2006 Feb 20.

DOI:10.1016/j.pharmthera.2005.06.022
PMID:16488018
Abstract

Adrenocorticotrophic hormone (ACTH(1-39)) and the melanocortins (alpha, beta and gamma-melanocyte-stimulating hormone [MSH]) are derived from a larger precursor molecule known as the pro-opiomelanocortin (POMC) protein. They exert their numerous biological effects by activating 7 transmembrane G-protein coupled receptors (GPCR), leading to adenylyl cyclase activation and subsequent cAMP accumulation within the target cell. To date, 5 melanocortin receptors (MCR) have been identified and termed MC1R to MC5R, they have been shown to have a wide and varied distribution throughout the body, being found in the central nervous system (CNS), periphery and immune cells. Melanocortins have a multitude of actions including: (i) modulating disease pathologies including arthritis, asthma, obesity; (ii) affecting functions, for example erectile dysfunction, skin tanning; and (iii) organ systems, for example cardiovascular system. Recently a mechanistic approach has been identified with alpha-MSH preventing NF-kappaB activation via the preservation and expression of IkappaBalphaprotein. This leads to a reduction of pro-inflammatory mediators including cytokines and inhibition of adhesion molecule expression, with subsequent reduction in leukocyte emigration. Development of selective ligands with an appropriate pharmacokinetic profile will enable a pharmacological evaluation of the potential beneficial effects of the melanocortins. In this review I have discussed the potential mechanistic action for the melanocortins and some of the disease pathologies shown to be modulated. This review proposes targeting the MCR with the ultimate aim of controlling many of the diseases that we face today.

摘要

促肾上腺皮质激素(ACTH(1 - 39))和促黑素细胞激素(α、β和γ - 促黑素细胞激素[MSH])均来源于一种名为阿黑皮素原(POMC)蛋白的更大前体分子。它们通过激活7次跨膜G蛋白偶联受体(GPCR)发挥多种生物学效应,进而激活腺苷酸环化酶并导致靶细胞内cAMP积累。迄今为止,已鉴定出5种促黑素细胞激素受体(MCR),分别命名为MC1R至MC5R,它们在全身分布广泛且多样,存在于中枢神经系统(CNS)、外周组织和免疫细胞中。促黑素细胞激素具有多种作用,包括:(i)调节疾病病理过程,如关节炎、哮喘、肥胖;(ii)影响功能,例如勃起功能障碍、皮肤晒黑;以及(iii)作用于器官系统,例如心血管系统。最近发现了一种机制,即α - MSH通过保留和表达IkappaBα蛋白来阻止NF - κB激活。这导致包括细胞因子在内的促炎介质减少以及黏附分子表达受到抑制,随后白细胞迁移减少。开发具有合适药代动力学特征的选择性配体将能够对促黑素细胞激素的潜在有益作用进行药理学评估。在这篇综述中,我讨论了促黑素细胞激素的潜在作用机制以及一些已显示可被调节的疾病病理过程。本综述建议以MCR为靶点,并最终目标是控制我们当今面临的许多疾病。

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