Interaction of cis-(6-Benzhydrylpiperidin-3-yl)benzylamine Analogues with
Monoamine Transporters: Structure−Activity Relationship Study of
Structurally Constrained 3,6-Disubstituted Piperidine Analogues of
(2,2-Diphenylethyl)-[1-(4-fluorobenzyl)piperidin-4-ylmethyl]amine
posted on 2003-04-19, 00:00authored byRohit B. Kolhatkar, Sujit K. Ghorai, Clifford George, Maarten E. A. Reith, Aloke K. Dutta
To explore structure−activity relationships (SAR) of a novel conformationally constrained lead
cis-3,6-disubstituted piperidine derivative derived from (2,2-diphenylethyl)-[1-(4-fluorobenzyl)piperidine-4-ylmethyl]amine (I), a series of compounds was synthesized by derivatizing the
exocyclic N-atom at the 3-position of the lead. This study led to the formation of substituted
phenyl and heterocyclic derivatives. All novel compounds were tested for their affinity at the
dopamine transporter (DAT), serotonin transporter (SERT), and norepinephrine transporter
(NET) in the brain by measuring their potency in competing for the binding of [3H]WIN 35
428, [3H]citalopram, and [3H]nisoxetine, respectively. Selected compounds were also evaluated
for their activity in inhibiting the uptake of [3H]DA. The SAR results demonstrated that the
nature of substitutions on the phenyl ring is important in activity at the DAT with the presence
of an electron-withdrawing group having the maximum effect on potency. Replacement of the
phenyl ring in the benzyl group by heterocyclic moieties resulted in the development of
compounds with moderate activity for the DAT. Two most potent racemic compounds were
separated by a diastereoisomeric separation procedure, and differential affinities were observed
for the enantiomers. Absolute configuration of the enantiomers was obtained unambiguously
by X-ray crystal structural study. One of the enantiomers, compound S,S-(−)-19a, exhibited
the highest potency for the DAT (IC50 = 11.3 nM) among all the compounds tested and was as
potent as GBR 12909 (1-[2-[bis(4-fluorophenyl)methoxy]ethyl]-4-(3-phenylpropyl)piperazine).
However, the compound (−)-19a was more selective than GBR 12909 in binding to the DAT
compared with binding to the SERT and NET. The present results establish the newly developed
3,6-disubstituted piperidine derivatives as a novel template for high-affinity inhibitors of DAT.
Structurally these molecules are more constrained compared to our earlier flexible piperidine
molecules and, thus, should provide more insights about their bioactive conformations.