Varenicline Is a Partial Agonist at α4β2 and a Full Agonist at α7 Neuronal Nicotinic Receptors

Hoestgaard-Jensen

Journal of Biological Chemistry

2013

Background: Inefficient functional receptor expression in heterologous expression systems has hampered investigations of ␣6* nAChRs. Results: Determinants in the ␣6 subunit for ␣6␤4* functionality have been delineated. Conclusion: Phe 223 and the intracellular loop in ␣6 are molecular impediments to functional ␣6␤4* nAChR expression in vitro. Significance: The molecular basis for the inefficient functional expression of ␣6␤4* nAChRs in vitro has been elucidated.

Section: Journal Of Biological Chemistry 33711supporting

confidence: 75%

Elucidation of Molecular Impediments in the α6 Subunit for in Vitro Expression of Functional α6β4* Nicotinic Acetylcholine Receptors

Hoestgaard-Jensen

Journal of Biological Chemistry

2013

Behavioural Brain Research

“…number of withdrawal symptoms, withdrawal severity) and the efficacy of pharmacotherapeutic treatments for smoking cessation. In support, it has been shown that variations in CHRNA4 are associated with smoking cessation outcomes [75], and it is possible that polymorphisms in nAChR subunit genes may modulate the effects of nicotine replacement therapy and varenicline (a α4β2* partial agonist and α7 nAChR full agonist) [21,118] on smoking cessation. Furthermore, given that the protein products of these genes are known to interact with each other to form receptors, it is possible that interactions between nAChR subunit genes may have a greater influence on smoking phenotypes than an individual nAChR subunit gene; thus, additional research should investigate possible gene-gene interactions between nAChR subunit genes.…”

Section: The Chrnb3-chrna6 and Chrna5-chrna3-chrnb4 Gene Clustersmentioning

confidence: 99%

Genetic variability in nicotinic acetylcholine receptors and nicotine addiction: Converging evidence from human and animal research

Portugal

Gould

2008

Tobacco smoking is a leading preventable cause of death in the United States and produces a major health and economic burden. Although the majority of smokers want to quit, few are successful. These data highlight the need for additional research into the neurobiology of tobacco dependence. Addiction to nicotine, the main psychoactive component of tobacco, is influenced by multiple factors that include individual differences in genetic makeup. Twin studies have demonstrated that genetic factors can influence vulnerability to nicotine addiction, and subsequent research has identified genes that may alter sensitivity to nicotine. In humans, genome-wide and candidate gene association studies have demonstrated that genes encoding nicotinic acetylcholine receptor (nAChR) proteins are associated with multiple smoking phenotypes. Similarly, research in mice has provided evidence that naturally occurring variability in nAChR genes is associated with changes in nicotine sensitivity. Furthermore, the use of genetic knockout mice has allowed researchers to determine the nAChR genes that mediate the effects of nicotine, whereas research with knockin mice has demonstrated that changes to nAChR genes can dramatically alter nicotine sensitivity. This review will examine the genetic factors that alter susceptibility to nicotine addiction, with an emphasis on the genes that encode nAChR proteins.

Behavioural Brain Research

“…In fact, medications that effectively increase acetylcholine by inhibiting acetylcholinesterase reduce the positive subjective effects of meth (De La Garza et al, 2008a; De La Garza 2008b; De La Garza et al, 2012). Additionally, varenicline (Chantix ® ), a partial α4β2 and full α7 nicotinic acetylcholine receptor agonist, (Coe et al, 2005a; Mihalak et al, 2006) can reduce the positive subjective effects of meth in humans, an effect that may reflect nAChR agonism reversing dopaminergic hypofunction (Verrico et al, 2014; Zorick et al, 2009). …”

Section: Introductionmentioning

confidence: 99%

The effects of varenicline on methamphetamine self-administration and drug-primed reinstatement in male rats

Pittenger

Barrett

Chou

et al. 2017

Methamphetamine (meth) addiction is a costly burden to both the individual user and society as a whole. Establishing effective pharmacotherapies to treat meth dependence is needed to help solve this health problem. The study reported herein examined the effects of varenicline, a partial α4β2 and full α7 nicotinic acetylcholine receptor agonist, on meth self-administration and reinstatement in male Sprague-Dawley rats. Following indwelling jugular catheter surgery, rats were either trained to self-administer meth or saline on a variable ratio (VR) 3 schedule of reinforcement. Self-administration sessions (2 hour duration; 19 total sessions) were conducted daily. The effect of varenicline pretreatment on meth and saline self-administration was then determined using a within-study design. All rats received varenicline (0.0, 0.3, 1.0, and 3.0 mg/kg) prior to 4 different test sessions. Dose order was randomly assigned and each test was separated by 2 standard self-administration sessions to assess stability of responding. Fifteen extinction sessions (no meth available) followed the last test. Extinction was followed by meth-primed (0.3 mg/kg IP) reinstatement tests to examine the effect of varenicline on meth-seeking behavior. All rats again received all doses of varenicline over 4 separate reinstatement tests performed on 4 consecutive days. Varenicline did not alter self-administration of meth or saline. Additionally, the 0.3 and 1.0 doses of varenicline non-specifically increased active lever responding during the reinstatement test sessions. This latter finding suggests that varenicline may increase relapse liability and should not be utilized as pharmacotherapy to treat meth dependence.