共 49 条
Identification of the GPR55 Antagonist Binding Site Using a Novel Set of High-Potency GPR55 Selective Ligands
被引:42
作者:

Kotsikorou, Evangelia
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机构:
Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Sharir, Haleli
论文数: 0 引用数: 0
h-index: 0
机构:
Temple Univ, Ctr Subst Abuse Res, Philadelphia, PA 19140 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Shore, Derek M.
论文数: 0 引用数: 0
h-index: 0
机构:
Univ N Carolina, Ctr Drug Discovery, Greensboro, NC 27402 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Hurst, Dow P.
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h-index: 0
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Univ N Carolina, Ctr Drug Discovery, Greensboro, NC 27402 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Lynch, Diane L.
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h-index: 0
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Univ N Carolina, Ctr Drug Discovery, Greensboro, NC 27402 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Madrigal, Karla E.
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h-index: 0
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Univ N Carolina, Ctr Drug Discovery, Greensboro, NC 27402 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Heynen-Genel, Susanne
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h-index: 0
机构:
Univ N Carolina, Ctr Drug Discovery, Greensboro, NC 27402 USA
Sanford Burnham Med Res Inst, Conrad Prebys Ctr Chem Genom, La Jolla, CA 92037 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Milan, Loribelle B.
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Sanford Burnham Med Res Inst, Conrad Prebys Ctr Chem Genom, La Jolla, CA 92037 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Chung, Thomas D. Y.
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Sanford Burnham Med Res Inst, Conrad Prebys Ctr Chem Genom, La Jolla, CA 92037 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Seltzman, Herbert H.
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Res Triangle Inst, Ctr Organ & Med Chem, Res Triangle Pk, NC 27709 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Bai, Yushi
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h-index: 0
机构:
Duke Univ, Dept Cell Biol, Durham, NC 27708 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Caron, Marc G.
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h-index: 0
机构:
Duke Univ, Dept Cell Biol, Durham, NC 27708 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Barak, Larry S.
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Duke Univ, Dept Cell Biol, Durham, NC 27708 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Croatt, Mitchell P.
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Univ N Carolina, Ctr Drug Discovery, Greensboro, NC 27402 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Abood, Mary E.
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h-index: 0
机构:
Temple Univ, Ctr Subst Abuse Res, Philadelphia, PA 19140 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA

Reggio, Patricia H.
论文数: 0 引用数: 0
h-index: 0
机构:
Univ N Carolina, Ctr Drug Discovery, Greensboro, NC 27402 USA Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA
机构:
[1] Univ Texas Pan Amer, Dept Chem, Edinburg, TX 78539 USA
[2] Temple Univ, Ctr Subst Abuse Res, Philadelphia, PA 19140 USA
[3] Univ N Carolina, Ctr Drug Discovery, Greensboro, NC 27402 USA
[4] Sanford Burnham Med Res Inst, Conrad Prebys Ctr Chem Genom, La Jolla, CA 92037 USA
[5] Res Triangle Inst, Ctr Organ & Med Chem, Res Triangle Pk, NC 27709 USA
[6] Duke Univ, Dept Cell Biol, Durham, NC 27708 USA
基金:
美国国家卫生研究院;
关键词:
PROTEIN-COUPLED RECEPTOR;
BETA(2) ADRENERGIC-RECEPTOR;
INDUCED CONFORMATIONAL-CHANGES;
CANCER-CELL PROLIFERATION;
CRYSTAL-STRUCTURE;
EXTRACELLULAR LOOP;
ACTIVATION;
RHODOPSIN;
LYSOPHOSPHATIDYLINOSITOL;
ORIENTATION;
D O I:
10.1021/bi4008885
中图分类号:
Q5 [生物化学];
Q7 [分子生物学];
学科分类号:
071010 ;
081704 ;
摘要:
GPR55 is a class A G protein-coupled receptor (GPCR) that has been implicated in inflammatory pain, neuropathic pain, metabolic disorder, bone development, and cancer. Initially deorphanized as a cannabinoid receptor, GPR55 has been shown to be activated by non-cannabinoid ligands such as L-alpha-lysophosphatidylinositol (LPI). While there is a growing body of evidence of physiological and pathophysiological roles for GPR55, the paucity of specific antagonists has limited its study. In collaboration with the Molecular Libraries Probe Production Centers Network initiative, we identified a series of GPR55 antagonists using a beta-arrestin, high-throughput, high-content screen of similar to 300000 compounds. This screen yielded novel, GPR55 antagonist chemotypes with IC50 values in the range of 0.16-2.72 mu M [Heynen-Genel, S., et al. (2010) Screening for Selective Ligands for GPR55: Antagonists (ML191, ML192, ML193) (Bookshelf ID NBK66153; PMID entry 22091481)]. Importantly, many of the GPR55 antagonists were completely selective, with no agonism or antagonism against GPR35, CB1, or CB2 up to 20 mu M. Using a model of the GPR55 inactive state, we studied the binding of an antagonist series that emerged from this screen. These studies suggest that GPR55 antagonists possess a head region that occupies a horizontal binding pocket extending into the extracellular loop region, a central ligand portion that fits vertically in the receptor binding pocket and terminates with a pendant aromatic or heterocyclic ring that juts out. Both the region that extends extracellularly and the pendant ring are features associated with antagonism. Taken together, our results provide a set of design rules for the development of second-generation GPR55 selective antagonists.
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页码:9456 / 9469
页数:14
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