Eldefrawi_1980_Proc.Natl.Acad.Sci.U.S.A_77_7458

Reference

Title : [3H]Phencyclidine: a probe for the ionic channel of the nicotinic receptor - Eldefrawi_1980_Proc.Natl.Acad.Sci.U.S.A_77_7458
Author(s) : Eldefrawi ME , Eldefrawi AT , Aronstam RS , Maleque MA , Warnick JE , Albuquerque EX
Ref : Proc Natl Acad Sci U S A , 77 :7458 , 1980
Abstract :

To evaluate [3H]phencyclidine ([3H]PCP)as a probe for the ionic channel of the nicotinic receptor, the characteristics of its binding to electric organ membranes od Torpedo ocellata and its effects on frog sartorius muscle were studied. Similar to PCP, [3H]PCP depressed the peak amplitude of endplate current, caused nonlinearity in the voltage-current relationship at negative potentials, accelerated the decay time of the end-plate current, and shortened the channel lifetime. Thus, [3H]PCP interacted with the ionic channel of the nicotinic receptor, although there were a few differences between its effect and that of PCP. Binding of [3H]PCP to Torpedo membranes was to sites on the ionic channel of acetylcholine (AcCho) receptor because it was saturable, dependent upon protein concentration, and inhibited by drugs that interact with the ionic channel, and the initial rate of binding was potentiated by receptor agonists. Equilibrium binding of [3H]PCP to Torpedo membranes was with two affinities, but in the presence of AcCho, [3H]PCP binding was with a single affinity. The affinities of channel drugs obtained by inhibition of binding of [3H]PCP and [3H[perhydrohistrionicotoxin to Torpedo membranes were different, with correlation coefficients of 0.52 and 0.82 in the absence and presence of a receptor agonist, respectively; this suggests differences in their binding sites on the ionic channel of the AcCho receptor.

PubMedSearch : Eldefrawi_1980_Proc.Natl.Acad.Sci.U.S.A_77_7458
PubMedID: 6261260

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Citations formats

Eldefrawi ME, Eldefrawi AT, Aronstam RS, Maleque MA, Warnick JE, Albuquerque EX (1980)
[3H]Phencyclidine: a probe for the ionic channel of the nicotinic receptor
Proc Natl Acad Sci U S A 77 :7458

Eldefrawi ME, Eldefrawi AT, Aronstam RS, Maleque MA, Warnick JE, Albuquerque EX (1980)
Proc Natl Acad Sci U S A 77 :7458