3-Phenyltropane analogues of cocaine are useful neurobiologic tools for exa
mining mechanisms of neurotransmitter transporters and psychostimulant drug
s. They are also potential substitute medications for psychostimulant abuse
. In this study, 18 3-phenyltropane analogues were characterized in uptake
and binding studies at dopamine (DAT), norepinephrine (NET) and serotonin (
SERT) transporters from the rat, and in binding at DAT in rat, rhesus monke
y, and human brain tissue. In rat brain tissue, potency in inhibiting uptak
e generally correlated with the potency in inhibiting binding at all three
transporters suggesting that none of these compounds have antagonist proper
ties. At the DAT, there was a significant correlation of inhibitory potenci
es between the rat and monkey, the monkey and human, and the rat and human
transporters although some compounds showed some species difference. These
findings suggest that with regard to the 3-phenyltropane series, there is g
enerally little pharmacologic difference between DATs from the three specie
s examined, although binding data from rat may not be a perfect predictor o
f uptake inhibition in human. (C) 1999 Elsevier Science Ireland Ltd. All ri
ghts reserved.