S6821 [Ligand Id: 12429] activity data from GtoPdb and ChEMBL
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| ChEMBL ligand: CHEMBL3924866 |
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| DB | Assay description | Assay Type | Standard value | Standard parameter | Original value | Original units | Original parameter | Reference |
|---|---|---|---|---|---|---|---|---|
| TAS2R14/Taste receptor type 2 member 14 in Human (target type: SINGLE PROTEIN) [ChEMBL: CHEMBL3309105] [GtoPdb: 668] [UniProtKB: Q9NYV8] | ||||||||
| ChEMBL | Agonist activity at TAS2R14 (unknown origin) by stably expressed cell-based assay | B | 4.4 | pEC50 | 40000 | nM | EC50 | J Med Chem (2020) 63: 4957-4977 [PMID:32330040] |
| TAS2R8/Taste receptor type 2 member 8 in Human (target type: SINGLE PROTEIN) [ChEMBL: CHEMBL3988599] [GtoPdb: 664] [UniProtKB: Q9NYW2] | ||||||||
| ChEMBL | Fluorescence Polarization Assays: In another embodiment, Fluorescence Polarization ("FP") based assays may be used to detect and monitor ligand binding. Fluorescence polarization is a versatile laboratory technique for measuring equilibrium binding, nucleic acid hybridization, and enzymatic activity. Fluorescence polarization assays are homogeneous in that they do not require a separation step such as centrifugation, filtration, chromatography, precipitation, or electrophoresis. These assays are done in real time, directly in solution and do not require an immobilized phase. Polarization values can be measured repeatedly and after the addition of reagents since measuring the polarization is rapid and does not destroy the sample. Generally, this technique can be used to measure polarization values of fluorophores from low picomolar to micromolar levels. | B | 7.46 | pIC50 | 35 | nM | IC50 | US-9247759-B2. Identification of human T2R receptors that respond to bitter compounds that elicit the bitter taste in compositions, and the use thereof in assays to identify compounds that inhibit (block) bitter taste in compositions and use thereof (2016) |
| ChEMBL | HTS assay: To determine the effectiveness of an individual antagonist, taste tests were performed with a T2R8 specific agonist, the compound of interest and a reference bitter blocker. We have previously described a good hT2R8 antagonist that was proven to have taste effect. It was shown to reduce bitterness of coffee by itself and in combination with a Broad spectrum bitter blocker. | B | 7.52 | pIC50 | 30 | nM | IC50 | US-9247759-B2. Identification of human T2R receptors that respond to bitter compounds that elicit the bitter taste in compositions, and the use thereof in assays to identify compounds that inhibit (block) bitter taste in compositions and use thereof (2016) |
| ChEMBL | Antagonist activity at recombinant human TAS2R8 stably expressed in cells co-expressing Galpha16gust44 assessed as inhibition of andrographolide-induced intracellular calcium level measured for 100 secs by fluo-4 dye based FLIPR assay | F | 7.7 | pIC50 | 20 | nM | IC50 | J Med Chem (2020) 63: 4957-4977 [PMID:32330040] |
| GtoPdb | - | - | 7.7 | pIC50 | 20 | nM | IC50 | J Med Chem (2020) 63: 4957-4977 [PMID:32330040] |
ChEMBL data shown on this page come from version 33:
Mendez D, Gaulton A, Bento AP, Chambers J, De Veij M, Félix E, Magariños MP, Mosquera JF, Mutowo P, Nowotka M, Gordillo-Marañón M, Hunter F, Junco L, Mugumbate G, Rodriguez-Lopez M, Atkinson F, Bosc N, Radoux CJ, Segura-Cabrera A, Hersey A, Leach AR. (2019) 'ChEMBL: towards direct deposition of bioassay data' Nucleic Acids Res., 47(D1). DOI: 10.1093/nar/gky1075. [EPMCID:30398643]
Davies M, Nowotka M, Papadatos G, Dedman N, Gaulton A, Atkinson F, Bellis L, Overington JP. (2015) 'ChEMBL web services: streamlining access to drug discovery data and utilities.' Nucleic Acids Res., 43(W1). DOI: 10.1093/nar/gkv352. [EPMCID:25883136]
