Selective Allosteric Antagonists for the G Protein-Coupled Receptor GPRC6A Based on the 2-Phenylindole Privileged Structure Scaffold

被引:19
作者
Johansson, Henrik [1 ]
Boesgaard, Michael Worch [1 ]
Norskov-Lauritsen, Lenea [1 ]
Larsen, Inna [1 ]
Kuhne, Sebastiaan [1 ]
Gloriam, David E. [1 ]
Brauner-Osborne, Hans [1 ]
Pedersen, Daniel Sejer [1 ]
机构
[1] Univ Copenhagen, Fac Hlth & Med Sci, Dept Drug Design & Pharmacol, DK-2100 Copenhagen, Denmark
来源
JOURNAL OF MEDICINAL CHEMISTRY | 2015年 / 58卷 / 22期
关键词
AMINO ACID RECEPTOR; CLASS-C; DRUG DISCOVERY; L-ARGININE; GLUTAMATE; CLONING; INDOLE; GPCR; EXPRESSION; CHEMISTRY;
D O I
10.1021/acs.jmedchem.5b01254
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
G protein-coupled receptors (GPCRs) represent a biological target class of fundamental importance in drug therapy. The GPRC6A receptor is a newly deorphanized class C GPCR that we recently reported for the first allosteric antagonists based on the 2-arylindole privileged structure scaffold (e.g., 1-3). Herein, we present the first structure-activity relationship study for the 2-arylindole antagonist 3, comprising the design, synthesis, and pharmacological evaluation of a focused library of 3-substituted 2-arylindoles. In a FRET-based inositol monophosphate (IP1) assay we identified compounds 7, 13e, and 34b as antagonists at the GPRC6A receptor in the low micromolar range and show that 7 and 34b display >9-fold selectivity for the GPRC6A receptor over related GPCRs, making 7 and 34b the most potent and selective antagonists for the GPRC6A receptor reported to date.
引用
收藏
页码:8938 / 8951
页数:14
相关论文
共 33 条
  • [21] Toward G protein-coupled receptor structure-based drug design using X-ray lasers
    Ishchenko, Andrii
    Stauch, Benjamin
    Han, Gye Won
    Batyuk, Alexander
    Shiriaeva, Anna
    Li, Chufeng
    Zatsepin, Nadia
    Weierstall, Uwe
    Liu, Wei
    Nango, Eriko
    Nakane, Takanori
    Tanaka, Rie
    Tono, Kensuke
    Joti, Yasumasa
    Iwata, So
    Moraes, Isabel
    Gati, Cornelius
    Cherezov, Vadim
    IUCRJ, 2019, 6 : 1106 - 1119
  • [22] Chemerin-activated functions of CMKLR1 are regulated by G protein-coupled receptor kinase 6 (GRK6) and β-arrestin 2 in inflammatory macrophages
    Serafin, D. Stephen
    Allyn, Brittney
    Sassano, Maria F.
    Timoshchenko, Roman G.
    Mattox, Daniel
    Brozowski, Jaime M.
    Siderovski, David P.
    Truong, Young K.
    Esserman, Denise
    Tarrant, Teresa K.
    Billard, Matthew J.
    MOLECULAR IMMUNOLOGY, 2019, 106 : 12 - 21
  • [23] Design of substrates and inhibitors of G protein-coupled receptor kinase 2 (GRK2) based on its phosphorylation reaction
    Kang, Jeong-Hun
    Toita, Riki
    Kawano, Takahito
    Murata, Masaharu
    Asai, Daisuke
    AMINO ACIDS, 2020, 52 (6-7) : 863 - 870
  • [24] High-throughput screening of G protein-coupled receptor antagonists using a bioluminescence resonance energy transfer 1-based β-arrestin2 recruitment assay
    Hamdan, FF
    Audet, M
    Garneau, P
    Pelletier, J
    Bouvier, M
    JOURNAL OF BIOMOLECULAR SCREENING, 2005, 10 (05) : 463 - 475
  • [25] G protein-coupled estrogen receptor (GPER) mediates NSCLC progression induced by 17β-estradiol (E2) and selective agonist G1
    Liu, Changyu
    Liao, Yongde
    Fan, Sheng
    Tang, Hexiao
    Jiang, Zhixiao
    Zhou, Bo
    Xiong, Jing
    Zhou, Sheng
    Zou, Man
    Wang, Jianmiao
    MEDICAL ONCOLOGY, 2015, 32 (04)
  • [26] An oral dsRNA delivery system based on chitosan induces G protein-coupled receptor kinase 2 gene silencing for Apolygus lucorum control
    Qiao, Heng
    Zhao, Jing
    Wang, Xiaofeng
    Xiao, Liubin
    Zhu-Salzman, Keyan
    Lei, Jiaxin
    Xu, Dejin
    Xu, Guangchun
    Tan, Yongan
    Hao, Dejun
    PESTICIDE BIOCHEMISTRY AND PHYSIOLOGY, 2023, 194
  • [27] Discovery of 6,7-Dihydro-5H-pyrrolo[2,3-a]pyrimidines as Orally Available G Protein-Coupled Receptor 119 Agonists
    Katamreddy, Subba R.
    Carpenter, Andrew J.
    Ammala, Carina E.
    Boros, Eric E.
    Brashear, Ron L.
    Briscoe, Celia P.
    Bullard, Sarah R.
    Caldwell, Richard D.
    Conlee, Christopher R.
    Croom, Dallas K.
    Hart, Shane M.
    Heyer, Dennis O.
    Johnson, Paul R.
    Kashatus, Jennifer A.
    Minick, Doug J.
    Peckham, Gregory E.
    Ross, Sean A.
    Roller, Shane G.
    Samano, Vicente A.
    Sauls, Howard R.
    Tadepalli, Sarva M.
    Thompson, James B.
    Xu, Yun
    Way, James M.
    JOURNAL OF MEDICINAL CHEMISTRY, 2012, 55 (24) : 10972 - 10994
  • [28] Modeling G protein-coupled receptors for structure-based drug discovery using low-frequency normal modes for refinement of homology models: Application to H3 antagonists
    Rai, Brajesh K.
    Tawa, Gregory J.
    Katz, Alan H.
    Humblet, Christine
    PROTEINS-STRUCTURE FUNCTION AND BIOINFORMATICS, 2010, 78 (02) : 457 - 473
  • [29] Sequential ligand- and structure-based virtual screening approach for the identification of potential G protein-coupled estrogen receptor-1 (GPER-1) modulators
    Khan, Shafi Ullah
    Ahemad, Nafees
    Chuah, Lay-Hong
    Naidu, Rakesh
    Htar, Thet Thet
    RSC ADVANCES, 2019, 9 (05) : 2525 - 2538
  • [30] The Kaposi's Sarcoma-Associated Herpesvirus G Protein-Coupled Receptor Contains an Immunoreceptor Tyrosine-Based Inhibitory Motif That Activates Shp2
    Philpott, Nicola
    Bakken, Thomas
    Pennell, Christopher
    Chen, Liwei
    Wu, Jie
    Cannon, Mark
    JOURNAL OF VIROLOGY, 2011, 85 (02) : 1140 - 1144
1234