D Smart, J C Jerman, M J Gunthorpe, S J Brough, J Ranson, W Cairns, P D Hayes, A D Randall, J B Davis
Index: Eur. J. Pharmacol. 417(1-2) , 51-8, (2001)
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A full pharmacological characterisation of the recently cloned human vanilloid VR1 receptor was undertaken. In whole-cell patch clamp studies, capsaicin (10 microM) elicited a slowly activating/deactivating inward current in human embryonic kidney (HEK293) cells stably expressing human vanilloid VR1 receptor, which exhibited pronounced outward rectification (reversal potential -2.1+/-0.2 mV) and was abolished by capsazepine (10 microM). In FLIPR-based Ca(2+) imaging studies the rank order of potency was resiniferatoxin>olvanil>capsaicin>anandamide, and all were full agonists. Isovelleral and scutigeral were inactive (1 nM-30 microM). The potencies of capsaicin, olvanil and resiniferatoxin, but not anandamide, were enhanced 2- to 7-fold at pH 6.4. Capsazepine, isovelleral and ruthenium red inhibited the capsaicin (100 nM)-induced Ca(2+) response (pK(B)=6.58+/-0.02, 5.33+/-0.03 and 7.64+/-0.03, respectively). In conclusion, the recombinant human vanilloid VR1 receptor stably expressed in HEK293 cells acted as a ligand-gated, Ca(2+)-permeable channel with similar agonist and antagonist pharmacology to rat vanilloid VR1 receptor, although there were some subtle differences.
| Structure | Name/CAS No. | Molecular Formula | Articles |
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Cycloprop[e]indene-1a,2(1H)-dicarboxaldehyde,3a,4,5,6,6a,6b-hexahydro-5,5,6b-trimethyl-, (1aS,3aS,6aS,6bR)-
CAS:37841-91-1 |
C15H20O2 |
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Sesquiterpenoid unsaturated dialdehydes increase the concent...
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The preparation and bioactivities of (-)-isovelleral.
1997-07-01 [Bioorg. Med. Chem. 5(7) , 1363-7, (1997)] |
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A novel route to the marasmane skeleton via a tandem rearran...
2001-04-06 [J. Org. Chem. 66(7) , 2350-7, (2001)] |
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![Cycloprop[e]indene-1a,2(1H)-dicarboxaldehyde,3a,4,5,6,6a,6b-hexahydro-5,5,6b-trimethyl-, (1aS,3aS,6aS,6bR)- Structure](https://image.chemsrc.com/caspic/048/37841-91-1.png)