METABOLISM AND DISPOSITION OF VARENICLINE, a SELECTIVE Α4β2 ACETYLCHOLINE RECEPTOR PARTIAL AGONIST, IN VIVO AND IN VITRO

Obach, R. Scott; Reed-Hagen, Anne E.; Krueger, Suzanne S.; Obach, Beth; O’Connell, Thomas N.; Zandi, Kathleen S.; Miller, Sandra A.; Coe, Jotham W.

doi:10.1124/dmd.105.006767

Cited by 199 publications

(174 citation statements)

References 10 publications

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“…Therefore, the nAChR antagonist mecamylamine (3 mg/kg) was injected 15 min before the administration of 0.3 mg/kg of varenicline. In all the experiments, the minimum time interval between the drug injections was at least 72 h. All the tested drugs have short half-lives in rats (nicotine t 1/2 ¼ 1.3 h; varenicline t 1/2 ¼ 4 h; cytisine t 1/2 ¼ 1.5 h; mecamylamine t 1/2 ¼ 1.2 h) (Kyerematen et al, 1988;Rollema et al, 2010;Obach et al, 2006;Debruyne et al, 2003). The half-life of 3-pyr-Cyt has not been reported.…”

Section: Experimental Designmentioning

confidence: 99%

Varenicline and Cytisine Diminish the Dysphoric-Like State Associated with Spontaneous Nicotine Withdrawal in Rats

Igari

Alexander

et al. 2013

Neuropsychopharmacol

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Tobacco addiction is characterized by a negative mood state upon smoking cessation and relapse after periods of abstinence. Clinical studies indicate that negative mood states lead to craving and relapse. The partial a4/a6/b2* nicotinic acetylcholine receptor (nAChR) agonists varenicline and cytisine are widely used as smoking cessation treatments. Varenicline has been approved in the United States for smoking cessation and cytisine is used in Eastern European countries. Despite the widespread use of these compounds, very little is known about their effects on mood states. These studies investigated the effects of varenicline, cytisine, and the cytisine-derivative 3-(pyridin-3 0 -yl)-cytisine (3-pyr-Cyt) on brain reward function in nicotine-naive and nicotine-withdrawing rats. The cytisine-derivative 3-pyr-Cyt is a very weak a4b2* nAChR partial agonist and like cytisine and varenicline has antidepressant-like effects in animal models. The intracranial self-stimulation (ICSS) procedure was used to investigate the effects of these compounds on brain reward function. Elevations in ICSS thresholds reflect a dysphoric state and a lowering of thresholds is indicative of a potentiation of brain reward function. It was shown that acute administration of nicotine and varenicline lowered ICSS thresholds. Acute administration of cytisine or 3-pyr-Cyt did not affect ICSS thresholds. Discontinuation of chronic, 14 days, nicotine administration led to elevations in ICSS thresholds that lasted for about 2 days. Varenicline and cytisine, but not 3-pyr-Cyt, diminished the nicotine withdrawal-induced elevations in ICSS thresholds. In conclusion, these studies indicate that varenicline and cytisine diminish the dysphoric-like state associated with nicotine withdrawal and may thereby prevent relapse to smoking in humans.

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Section: Experimental Designmentioning

confidence: 99%

Varenicline and Cytisine Diminish the Dysphoric-Like State Associated with Spontaneous Nicotine Withdrawal in Rats

Igari

Alexander

et al. 2013

Neuropsychopharmacol

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“…This schedule allows 2-FA to reach steady-state levels in the presence of varenicline near its peak level. Given the long plasma halflife (17 h) of varenicline, we predicted high plasma levels of the medication throughout the 2-FA bolus plus infusion injection, thereby remaining reasonably constant during the initial period of 2-FA uptake (1200 to 1600 hours) and first block of the PET scanning session (1600-1700 hours) and slowly decreasing through the end of the imaging session (Obach et al, 2006).…”

Section: Placebo and Varenicline Administrationmentioning

confidence: 99%

“…The timing of varenicline administration was chosen to have peak plasma levels at roughly the start of the 2-FA infusion at 1200 hours (Obach et al, 2006). The aim was to have peak occupancy of a4b2* nAChRs by varenicline at approximately the time of bolus 2-FA administration.…”

Section: Placebo and Varenicline Administrationmentioning

confidence: 99%

A Single Administration of Low-Dose Varenicline Saturates α4β2* Nicotinic Acetylcholine Receptors in the Human Brain

Lotfipour

Mandelkern

Alvarez-Estrada

et al. 2012

Neuropsychopharmacol

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The primary objective of this project was to determine the a4b2* nicotinic acetylcholine receptor (nAChR) occupancy in human brain of a single low dose of varenicline (0.5 mg), and to explore the relationship between receptor occupancy by varenicline and tobacco withdrawal symptoms (*denoting other putative nAChR subunits). Otherwise healthy smokers (n ¼ 9) underwent two positron emission tomography (PET) sessions with the selective a4b2* radioligand 2-FA. For the PET sessions, participants received either a low dose of varenicline (0.5 mg) or matching placebo pill (double-blind, random order) before imaging. For both sessions, participants received bolus plus continuous infusions of 2-FA, were scanned for 1 h after allowing the radiotracer to reach a steady state, smoked to satiety, and were scanned for 2 more hours. We estimated the fractional receptor occupancy by a single dose of varenicline (0.5 mg) and the corresponding varenicline dissociation constant (K V ), along with the effect of low-dose varenicline, pill placebo, and smoking-to-satiety on withdrawal rating scales. The data are compatible with 100% occupancy of a4b2* nAChRs by a single dose of varenicline, with a 90% lower confidence limit of 89% occupancy for the thalamus and brainstem. The corresponding 90% upper limit on effective K V with respect to plasma varenicline was 0.49 nM. Smoking to satiety, but not low-dose varenicline, significantly reduced withdrawal symptoms. Our findings demonstrate that low-dose varenicline results in saturation of a4b2* nAChRs in the thalamus and brainstem without reducing withdrawal symptoms.

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“…Nicotine inhibits tetraethylammonium (an OCTn model substrate) accumulation within a human embryonic kidney cell line (HEK-293) mediated by OCT1 with an IC 50 of 63 µM in vitro, and by OCT2 with an IC 50 of 50 μM. 33 Lips et al 32 35 , serves as an OCT2 substrate in vitro, and, at a much higher concentration, as an OCT2 inhibitor. A clinical study (N = 12) of joint administration of varenicline and cimetidine, a known OCT2 inhibitor, demonstrated reduced clearance and increased plasma concentration of varenicline of ~25% and 29%, changes that the authors did not consider clinically meaningful.…”

mentioning

confidence: 99%

Organic Cation Transporter Variation and Response to Smoking Cessation Therapies

Bergen

Javitz

Krasnow

et al. 2014

Nicotine & Tobacco Research

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METABOLISM AND DISPOSITION OF VARENICLINE, a SELECTIVE Α4β2 ACETYLCHOLINE RECEPTOR PARTIAL AGONIST, IN VIVO AND IN VITRO

Cited by 199 publications

References 10 publications

Varenicline and Cytisine Diminish the Dysphoric-Like State Associated with Spontaneous Nicotine Withdrawal in Rats

Varenicline and Cytisine Diminish the Dysphoric-Like State Associated with Spontaneous Nicotine Withdrawal in Rats

A Single Administration of Low-Dose Varenicline Saturates α4β2* Nicotinic Acetylcholine Receptors in the Human Brain

Organic Cation Transporter Variation and Response to Smoking Cessation Therapies

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