Regulation of the deleterious effects of binge-like exposure to alcohol during adolescence by α7 nicotinic acetylcholine receptor agents: prevention by pretreatment with a α7 negative allosteric modulator and emulation by a α7 agonist in alcohol-preferring (P) male and female rats

Abstract

Rationale and objectives: Binge-like alcohol consumption during adolescence associates with several deleterious consequences during adulthood including an increased risk for developing alcohol use disorder (AUD) and other addictions. Replicated preclinical data has indicated that adolescent exposure to binge-like levels of alcohol results in a reduction of choline acetyltransferase (ChAT) and an upregulation in the α7 nicotinic receptor (α7). From this information, we hypothesized that the α7 plays a critical role in mediating the effects of adolescent alcohol exposure.

Methods: Male and female P rats were injected with the α7 agonist AR-R17779 (AR) once during 6 time points between post-natal days (PND) 29-37. Separate groups were injected with the α7 negative allosteric modulator (NAM) dehydronorketamine (DHNK) 2 h before administration of 4 g/kg EtOH (14 total exposures) during PND 28-48. On PND 75, all rats were given access to water and ethanol (15 and 30%) for 6 consecutive weeks (acquisition). All rats were then deprived of EtOH for 2 weeks and then, alcohol was returned (relapse).

Results: Administration of AR during adolescence significantly increased acquisition of alcohol consumption during adulthood and prolonged relapse drinking in P rats. In contrast, administration of DHNK prior to binge-like EtOH exposure during adolescence prevented the increase in alcohol consumption observed during acquisition of alcohol consumption and the enhancement of relapse drinking observed during adulthood.

Discussion: The data indicate that α7 mediates the effects of alcohol during adolescence. The data also indicate that α7 NAMs are potential prophylactic agents to reduce the deleterious effects of adolescent alcohol abuse.

Keywords: Acquisition; Addiction; Adolescence; Alcohol; Alcohol-preferring (P) rats; Ethanol; Relapse.

Figure 1.

Depicts the experiment timeline for the a7 agonist (AR, top panel) and DHNK (bottom panel) used in the current experiments.

Figure 2.

Depicts the average alcohol intake in female (top) and male (bottom) rats administered AR-R17779 during adolescence on adult alcohol consumption. * indicates 10 mg/kg AR-R17779 > 3 mg/kg and saline. # indicates 3 mg/kg > saline.

Figure 3.

Depicts the mean (+ SEM) for female (top) and male (bottom) alcohol-preferring (P) rats during relapse EtOH drinking. * indicates EtOH consumption exceeds baseline intake.+ indicates that rats administered 10 mg/kg AR-R177779 during adolescence consumed more alcohol than saline controls.

Figure 4.

Depicts the average alcohol intake in male (top) and female (bottom) rats administered DHNK 2 hours prior to AIE or CON treatment during adolescence.* indicates AIE-Saline rats consumed more alcohol than all other groups.

Figure 5.

Depicts the mean (+ SEM) for female (top) and male (bottom) alcohol-preferring (P) rats during relapse EtOH drinking. * indicates EtOH consumption exceeds baseline intake.+ indicates that rat pretreated with saline prior to AIE exposure (AIE - Saline) consumed more alcohol than any other group.