Introduction of unsaturation into the N-n-alkyl chain of the nicotinic receptor antagonists, NONI and NDNI: effect on affinity and selectivity

Introduction of unsaturation into the N-n-alkyl chain of the nicotinic receptor antagonists, NONI and NDNI: effect on affinity and selectivity

N-n-octylnicotinium iodide (NONI) and N-n-decylnicotinium iodide (NDNI) are selective nicotinic receptor (nAChR) antagonists mediating nicotine-evoked striatal dopamine (DA) release, and inhibiting [3H]nicotine binding, respectively. This study evaluated effects of introducing unsaturation into the...

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Veröffentlicht in:The AAPS journal 2005-08, Vol.7 (1), p.E201-E217
Hauptverfasser: Sumithran, Sangeetha P, Crooks, Peter A, Xu, Rui, Zhu, Jun, Deaciuc, Agripina G, Wilkins, Lincoln H, Dwoskin, Linda P
Format: Artikel
Sprache:eng
Schlagworte:
Aconitine - analogs & derivatives
Aconitine - metabolism
Animals
Corpus Striatum - drug effects
Corpus Striatum - secretion
Dopamine - secretion
Dopamine Plasma Membrane Transport Proteins - antagonists & inhibitors
Dopamine Plasma Membrane Transport Proteins - metabolism
Drug Design
Drug Evaluation, Preclinical
Electric Stimulation
Humans
Male
Molecular Structure
Nicotine - analogs & derivatives
Nicotine - chemistry
Nicotine - metabolism
Nicotine - pharmacology
Nicotinic Antagonists - chemistry
Nicotinic Antagonists - metabolism
Nicotinic Antagonists - pharmacology
Nomifensine - pharmacology
Protein Binding
Protein Subunits
Rats
Rats, Sprague-Dawley
Receptors, Nicotinic - chemistry
Receptors, Nicotinic - drug effects
Receptors, Nicotinic - metabolism
Reward
Rubidium - analysis
Structure-Activity Relationship
Synaptosomes - drug effects
Synaptosomes - metabolism
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Zusammenfassung:N-n-octylnicotinium iodide (NONI) and N-n-decylnicotinium iodide (NDNI) are selective nicotinic receptor (nAChR) antagonists mediating nicotine-evoked striatal dopamine (DA) release, and inhibiting [3H]nicotine binding, respectively. This study evaluated effects of introducing unsaturation into the N-n-alkyl chains of NONI and NDNI on inhibition of [3H]nicotine and [3H]methyllycaconitine binding (alpha4beta2* and alpha7* nAChRs, respectively), (86)Rb+ efflux and [3H]DA release (agonist or antagonist effects at alpha4beta2* and alpha6beta2*-containing nAChRs, respectively). In the NONI series, introduction of a C3-cis- (NONB3c), C3-trans- (NONB3t), C7-double-bond (NONB7e), or C3-triple-bond (NONB3y) afforded a 4-fold to 250-fold increased affinity for [3H]nicotine binding sites compared with NONI. NONB7e and NONB3y inhibited nicotine-evoked 86Rb+ efflux, indicating alpha4beta2* antagonism. NONI analogs exhibited a 3-fold to 8-fold greater potency inhibiting nicotine-evoked [3H]DA overflow compared with NONI (IC50 = 0.62 microM; Imax = 89%), with no change in Imax, except for NONB3y (Imax = 50%). In the NDNI series, introduction of a C4-cis- (NDNB4c), C4-trans-double-bond (NDNB4t), or C3-triple-bond (NDNB3y) afforded a 4-fold to 80-fold decreased affinity for [3H]nicotine binding sites compared with NDNI, whereas introduction of a C9 double-bond (NDNB9e) did not alter affinity. NDNB3y and NDNB4t inhibited nicotine-evoked 86Rb+ efflux, indicating antagonism at alpha4beta2* nAChRs. Although NDNI had no effect, NDNB4t and NDNB9e potently inhibited nicotine-evoked [3H]DA overflow (IC50 = 0.02-0.14 microM, Imax = 90%), as did NDNB4c (IC50 = 0.08 microM; Imax = 50%), whereas NDNB3y showed no inhibition. None of the analogs had significant affinity for alpha7* nAChRs. Thus, unsaturated NONI analogs had enhanced affinity at alpha4beta2*- and alpha6beta2*-containing nAChRs, however a general reduction of affinity at alpha4beta2* and an uncovering of antagonist effects at alpha6beta2*-containing nAChRs were observed with unsaturated NDNI analogs.
ISSN:1550-7416
DOI:10.1208/aapsj070119