首页> 外文期刊>Journal of Medicinal Chemistry >Discovery of Polypharmacological Melanocortin-3 and-4 Receptor Probes and Identification of a 100-Fold Selective nM MC3R Agonist versus a mu M MC4R Partial Agonist
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Discovery of Polypharmacological Melanocortin-3 and-4 Receptor Probes and Identification of a 100-Fold Selective nM MC3R Agonist versus a mu M MC4R Partial Agonist

机译:多酚摩洛哥毒素-3和-4受体探针的发现和鉴定100倍选择性NM MC3R激动剂与MU M MC4R局部激动剂的鉴定

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摘要

The centrally expressed melanocortin-3 and melanocortin-4 receptors (MC3R and MC4R, respectively) are established targets to treat diseases of positive- and negative-energy homeostasis. We previously reported [Doering, S. R.; et al. J. Med. Chem. 2017, 60, 4342-4357] mixture-based positional scanning approaches to identify dual MC3R agonist and MC4R antagonist tetrapeptides. Herein, 46 tetrapeptides were chosen for MC3R agonist screening selectivity profiles, synthesized, and pharmacologically characterized at the mouse melanocortin-1, -3, -4, and -5 receptors. Substitutions to the tetrapeptide template were selected solely based on MC3R agonist potency from the mixture-based screen. This study resulted in the discovery of compound 42 (Ac-Val-Gln-(pI)DPhe-DTic-NH2), a full MC3R agonist that is 100-fold selective for the MC3R over the mu M MC4R partial agonist pharmacology. This compound represents a first-in-class MC3R selective agonist. This ligand will serve as a useful in vivo molecular probe for the investigation of the roles of the MC3R and MC4R in diseases of dysregulated energy homeostasis.
机译:中央表达的黑素素-3和Melanocortin-4受体(分别是MC3R和MC4R)是建立治疗阳性和阴性稳态疾病的靶标。我们之前报道了[Doing,S. R .;等等。 J.Med。化学。 2017年,60,为基础的混合物4342-4357]位置扫描方法,以确定双重MC3R激动剂和拮抗剂MC4R的四肽。本文中,选择46四肽用于MC3R激动剂筛选选择性谱,合成,并在小鼠黑色素蛋白-1,-3,-4和-5受体中进行药理学表征。仅基于来自基于混合物的筛选的MC3R激动剂效力,选择四肽模板的取代。该研究导致发现化合物42(AC-VAL-GLN-(PI)Dphe-DTIC-NH2),全MC3R激动剂是在MU M MC4R部分激动剂药理学上为MC3R选择的100倍。该化合物代表了一类阶级MC3R选择性激动剂。该配体将作为体内分子探针的可用于调查MC3R和MC4R在疾病疾病疾病中的作用。

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