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(+)-Anatoxin-a Is a Potent Agonist at Neuronal Nicotinic Acetylcholine Receptors
Authors:P Thomas  M Stephens  G Wilkie  M Amar  G G Lunt  P Whiting  T Gallagher‡  E Pereira‡  M Alkondon‡  E X Albuquerque‡  S Wonnacott
Institution:Department of Biochemistry, University of Bath, Bath;Merck Sharp &Dohme Neuroscience Research Centre, Harlow, Essex;School of Chemistry, University of Bristol, Bristol, England;Department of Pharmacology &Experimental Therapeutics, University of Maryland School of Medicine, Baltimore, Maryland, U.S.A.
Abstract:Abstract: The effects of the nicotinic agonist (+)-anatoxin-a have been examined in four different preparations, representing at least two classes of neuronal nicotinic receptors. (+)-Anatoxin-a was most potent (EC50= 48 n M ) in stimulating 86Rb+ influx into M10 cells, which express the nicotinic receptor subtype comprising α4 and β2 subunits. A presynaptic nicotinic receptor mediating acetylcholine release from hippocampal synaptosomes was similarly sensitive to (+)-anatoxin-a (EC50= 140 n M ). α-Bungarotoxin-sensitive neuronal nicotinic receptors, studied using patch-clamp recording techniques, required slightly higher concentrations of this alkaloid for activation: Nicotinic currents in hippocampal neurons were activated by (+)-anatoxin-a with an EC50 of 3.9 γ M , whereas α7 homooligomers reconstituted in Xenopus oocytes yielded an EC50 value of 0.58 γ M for (+)-anatoxin-a. In these diverse preparations, (+)-anatoxin-a was between three and 50 times more potent than (–)-nicotine and ˜20 times more potent than acetylcholine, making it the most efficacious nicotinic agonist thus far described.
Keywords:Neuronal nicotinic receptors  Presynaptic nicotinic auto-receptor  Hippocampal neurons  Synaptosomes              Xenopus oocytes  Anatoxin-a  Nicotine  
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