Literature DB >> 24900874

New Hits as Antagonists of GPR103 Identified by HTS.

Anneli Nordqvist1, Lisbeth Kristensson1, Kjell E Johansson1, Krystle Isaksson da Silva1, Tomas Fex1, Christian Tyrchan1, Anette Svensson Henriksson1, Kristina Nilsson1.   

Abstract

Preclinical data indicate that GPR103 receptor and its endogenous neuropeptides QRFP26 and QRFP43 are involved in appetite regulation. A high throughput screening (HTS) for small molecule GPR103 antagonists was performed with the clinical goal to target weight management by modulation of appetite. A high hit rate from the HTS and initial low confirmation with respect to functional versus affinity data challenged us to revise the established screening cascade. To secure high quality data while increasing throughput, the binding assay was optimized on quality to run at single concentration. This strategy enabled evaluation of a larger fraction of chemical clusters and singletons delivering 17 new compound classes for GPR103 antagonism. Representative compounds from three clusters are presented. One of the identified clusters was further investigated, and an initial structure-activity relationship study is reported. The most potent compound identified had a pIC50 of 7.9 with an improved ligand lipophilic efficiency.

Entities:  

Keywords:  26RFa; 43RFa; G-protein coupled receptor; GPCR; SP9155; appetite regulation; high throughput screening

Year:  2014        PMID: 24900874      PMCID: PMC4027783          DOI: 10.1021/ml400519h

Source DB:  PubMed          Journal:  ACS Med Chem Lett        ISSN: 1948-5875            Impact factor:   4.345


  16 in total

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9.  Identification and characterization of a novel RF-amide peptide ligand for orphan G-protein-coupled receptor SP9155.

Authors:  Ying Jiang; Lin Luo; Eric L Gustafson; Deepmala Yadav; Maureen Laverty; Nicholas Murgolo; Galya Vassileva; Ming Zeng; Thomas M Laz; Jiang Behan; Ping Qiu; Luquan Wang; Suke Wang; Marvin Bayne; Jonathan Greene; Frederick Monsma; Fang L Zhang
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