Role of Corticotropin Releasing Factor 1 Signaling in Cocaine Seeking during Early Extinction in Female and Male Rats.

Angie M Cason,Gary Aston-Jones,Amy Kohtz,Judith Homberg

doi:10.1371/journal.pone.0158577

Angie M Cason, Gary Aston-Jones + Show 2 more

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https://doi.org/10.1371/journal.pone.0158577

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Abstract

Locus coeruleus norepinephrine (LC-NE) and corticotropin releasing factor (CRF) neurons are involved in stress responses, including stress’s ability to drive drug relapse. Previous animal studies indicate that female rats exhibit greater drug seeking than male rats during initial drug abstinence. Moreover, females are more sensitive to the effect of stress to drive drug seeking than males. Finally, LC-NE neurons are more sensitive to CRF in females compared to males. We hypothesized that increased drug seeking in females on extinction day one (ED1) is due to increased response to the stress of early withdrawal and is dependent upon the increased response of LC in females to CRF. We predicted that LC-NE neurons would exhibit Fos activation on ED1, and that blocking CRF1 signaling would decrease drug seeking on ED1 measured by responding on an active lever previously associated with cocaine self- administration. After chronic cocaine self-administration, female and male rats underwent a test for initial extinction responding by measuring lever pressing in the absence of cocaine. Prior to this Extinction Day 1 (ED1) session, rats were injected with vehicle or the selective CRF1 antagonist (CP) to measure effects of CRF antagonism on drug seeking during early abstinence. ED1 increased corticosterone in female rats, in proportion to lever responding in male and female, indicating that ED1 was stressful. Pretreatment with CP decreased cocaine seeking on ED1 more effectively in female compared to male rats. This increase in responding was associated with an increase in activation of LC NE neurons. Together, these findings indicate that stress, and signaling at CRF receptors in LC, may be involved in the increased drug seeking during initial abstinence.

Highlights

Accumulating evidence indicates that there is a strong relationship between stress, substance abuse and sex [1,2]
Our results indicate that the increased cocaine seeking observed during initial abstinence, extinction day 1 (ED1), is accompanied by increased activation of Locus coeruleus norepinephrine (LC-NE) neurons, but not other NE neurons in A1 or A2/NTS
Pretreatment with CP decreased cocaine seeking on Extinction Day 1 (ED1) in female and male rats, but was more effective in females supporting the hypothesis that signaling at the CRF1 receptor is involved in drug seeking during initial abstinence

Summary

Introduction

Accumulating evidence indicates that there is a strong relationship between stress, substance abuse and sex [1,2]. Clinical findings indicate that there is increased neural activation in response to stressful stimuli in cocaine-dependent women compared to cocaine-dependent men, which may influence the propensity to relapse [3]. CRF Signaling in Cocaine Seeking response to stress, and recent findings indicate a link between the sex/gender differences in drug abuse and these brain systems. Stress drives reinstatement of drug seeking in a CRF-dependent manner [5,6,7,8], and females show greater stress-induced reinstatement compared to males [9,10]. Several studies link stress and the central NE system in relapse to drug seeking [11,12,13,14,15]

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