1Starting from the structure of an old 4-oxystilbene derivate with ganglioplegic activity (MG624), we synthesized two further derivates (F2 and F3) and two stereoisomers of F3 (F3A and F3B), and studied their selective effect on neuronal nicotinic acetylcholine receptor (AChR) subtypes.2MG 624, F3, F3A and F3B inhibited of 125I-αBungarotoxin (αBgtx) binding to neuronal chick optic lobe (COL) membranes, with nM affinity, but inhibited 125I-αBgtx binding to TE671 cell-expressed muscle-type AChR only at much higher concentrations.3We immobilized the α7, β2 and β4 containing chick neuronal nicotinic AChR subtypes using anti-subunit specific antibodies. MG 624, F3, F3A and F3B inhibited 125I-αBgtx binding to the α7-containing receptors with nm affinity, but inhibited 3H-Epi binding to β2-containing receptors only at very high concentrations (more than 35 μm); their affinity for the β4-containing receptors was ten times more than for the β2-containing subtype.4Both MG624 and F3 compounds inhibited the ACh evoked currents in homomeric oocyte-expressed chick α7 receptors with an IC50 of respectively 94 and 119 nm.5High doses of both MG 624 and F3 depressed the contractile response to vagus nerve stimulation in guinea pig nerve-stomach preparations although at different IC50s (49.4 vs 166.2 μm) The effect of MG624 on rat nerve-hemidiaphragm preparations was 33 times less potent than that of F3 (IC50 486 vs 14.5 μm).6In conclusion, MG624 and F3 have a high degree of antagonist selectivity for neuronal nicotinic αBgtx receptors containing the α7 subunit.
4-Oxystilbene compounds are selective for neuronal nicotinic α7 Bungarotoxin receptors / C., Gotti; B., Balestra; M., Moretti; G. E., Rovati; Maggi, Laura; G., Rossoni; F., Berti; L., Villa; M. PALLAVICINI AND F., Clementi. - In: BRITISH JOURNAL OF PHARMACOLOGY. - ISSN 0007-1188. - STAMPA. - 124:(1998), pp. 1197-1206. [10.1038/sj.bjp.0701957]
4-Oxystilbene compounds are selective for neuronal nicotinic α7 Bungarotoxin receptors
MAGGI, Laura;
1998
Abstract
1Starting from the structure of an old 4-oxystilbene derivate with ganglioplegic activity (MG624), we synthesized two further derivates (F2 and F3) and two stereoisomers of F3 (F3A and F3B), and studied their selective effect on neuronal nicotinic acetylcholine receptor (AChR) subtypes.2MG 624, F3, F3A and F3B inhibited of 125I-αBungarotoxin (αBgtx) binding to neuronal chick optic lobe (COL) membranes, with nM affinity, but inhibited 125I-αBgtx binding to TE671 cell-expressed muscle-type AChR only at much higher concentrations.3We immobilized the α7, β2 and β4 containing chick neuronal nicotinic AChR subtypes using anti-subunit specific antibodies. MG 624, F3, F3A and F3B inhibited 125I-αBgtx binding to the α7-containing receptors with nm affinity, but inhibited 3H-Epi binding to β2-containing receptors only at very high concentrations (more than 35 μm); their affinity for the β4-containing receptors was ten times more than for the β2-containing subtype.4Both MG624 and F3 compounds inhibited the ACh evoked currents in homomeric oocyte-expressed chick α7 receptors with an IC50 of respectively 94 and 119 nm.5High doses of both MG 624 and F3 depressed the contractile response to vagus nerve stimulation in guinea pig nerve-stomach preparations although at different IC50s (49.4 vs 166.2 μm) The effect of MG624 on rat nerve-hemidiaphragm preparations was 33 times less potent than that of F3 (IC50 486 vs 14.5 μm).6In conclusion, MG624 and F3 have a high degree of antagonist selectivity for neuronal nicotinic αBgtx receptors containing the α7 subunit.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
