Title : Methyllycaconitine: a selective probe for neuronal alpha-bungarotoxin binding sites - Ward_1990_FEBS.Lett_270_45 |
Author(s) : Ward JM , Cockcroft VB , Lunt GG , Smillie FS , Wonnacott S |
Ref : FEBS Letters , 270 :45 , 1990 |
Abstract :
The ability of methyllycaconitine (MLA) to inhibit the binding of [125I]alpha-bungarotoxin to rat brain membranes, frog and human muscle extracts and the human muscle cell line TE671 has been measured. MLA showed a markedly higher affinity for the rat brain site (Ki 1.4 x 10(-9) M) than for the muscle receptors (Ki 10(-5)-10(-6) M). Structure modelling techniques were used to fit the structure of MLA to a nicotinic pharmacophore model. MLA is the first low molecular weight ligand to be shown to discriminate between muscle nicotinic receptors and their alpha-bungarotoxin-binding counterpart in the brain, and as such may be a useful structural probe for pursuing the structural and functional properties of the neuronal protein. |
PubMedSearch : Ward_1990_FEBS.Lett_270_45 |
PubMedID: 2226787 |
Ward JM, Cockcroft VB, Lunt GG, Smillie FS, Wonnacott S (1990)
Methyllycaconitine: a selective probe for neuronal alpha-bungarotoxin binding sites
FEBS Letters
270 :45
Ward JM, Cockcroft VB, Lunt GG, Smillie FS, Wonnacott S (1990)
FEBS Letters
270 :45