Abstract
Patients suffering from opioid use disorder often relapse during periods of abstinence, which is posited to be caused by negative affective states that drive motivated behaviors. Here, we explored whether conditioning mice with morphine in a conditioned place preference (CPP) training paradigm evoked anxiety-like behavior during morphine abstinence. To do this, mice were conditioned with morphine (10 mg/kg, i.p.) for 5 days. Twenty-four hours following conditioning, anxiety levels were tested by measuring time in the open arms of the elevated plus-maze. The next day, mice were placed in the three-compartment chamber to measure morphine-induced CPP. Our results show that following morphine conditioning, mice spent significantly less time in the open arm of the elevated plus-maze and expressed robust morphine CPP on CPP test day. Furthermore, we found that an acute treatment with (R,S)-ketamine (10 mg/kg, i.p.), a medication demonstrating promise for preventing anxiety-related phenotypes, 30 min before testing on post-conditioning day 1, increased time spent in the open arm of the elevated plus-maze in saline- and morphine-conditioned mice. Additionally, we found that the second injection of ketamine 30 min before CPP tests on post-conditioning day 2 prevented morphine-induced CPP, which lasted for up to 28 days post-conditioning. Furthermore, we found that conditioning mice with 10% (w/v) sucrose using an oral self-administration procedure did not evoke anxiety-like behavior, but elicited robust CPP, which was attenuated by ketamine treatment 30 min before CPP tests. Overall, our results suggest that the ketamine-induced block of morphine CPP may not be attributed solely to alleviating negative affective states, but potentially through impaired memory of morphine-context associations.
Highlights
The motivation to continually seek and obtain addictive substances during periods of abstinence or recovery is caused, in part, by the necessity to avoid aversive internal states (Solomon and Corbit, 1978)
In an attempt to provide evidence that morphine-induced conditioned place preference (CPP), using our training paradigm, is mediated, in part, by negative affective states, 24 h following the last morphine conditioning session (Figure 1A), we measured anxiety-like behavior using the elevated plus maze (EPM; Pellow et al, 1985)
We found that morphine-treated mice, who showed robust locomotor sensitization by conditioning day 5 (Figure 1B), expressed a significant decrease in the percent time spent in the open arm of the EPM compared to saline-treated controls (t(38) = 3.35, p = 0.002, student’s t-test; Figure 1C)
Summary
The motivation to continually seek and obtain addictive substances during periods of abstinence or recovery is caused, in part, by the necessity to avoid aversive internal states (Solomon and Corbit, 1978). This is followed by a test day whereby the time spent in the drug-paired context is measured This behavioral paradigm is a form of Pavlovian learning whereby injection of a drug (i.e., unconditioned stimulus) elicits a hedonic feeling of pleasure (i.e., unconditioned response), which, when paired with a context (neutral stimulus), invokes incentive value to the context (i.e., a conditioned stimulus), driving a behavioral response to ‘‘seek’’ the context (conditioned response). We have found that 5 days of morphine (10 mg/kg) conditioning elicits robust morphine CPP (Graziane et al, 2016; McDevitt and Graziane, 2019) It is unclear whether this ‘‘drug contextseeking’’ behavior is mediated by negative affective states. It is unclear whether a subanesthetic dose of ketamine, an anxiolytic agent (Engin et al, 2009), blocks morphine-induced CPP by mitigating morphine-induced negative affective states
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