Nucleus accumbens D2/3 receptors predict trait impulsivity and cocaine reinforcement.
- Authors
- Dalley, Jeffrey W; Fryer, Tim D; Brichard, Laurent; Robinson, Emma S J; Theobald, David E H; LÀÀne, Kristjan; Peña, Yolanda; Murphy, Emily R; Shah, Yasmene; Probst, Katrin; Abakumova, Irina; Aigbirhio, Franklin I; Richards, Hugh K; Hong, Young; Baron, Jean-Claude; Everitt, Barry J; Robbins, Trevor W
- Year
- 2007
- Journal
- Science (New York, N.Y.)
- PMID
- 17332411
- DOI
- 10.1126/science.1137073
- PMCID
- PMC1892797
Stimulant addiction is often linked to excessive risk taking, sensation seeking, and impulsivity, but in ways that are poorly understood. We report here that a form of impulsivity in rats predicts high rates of intravenous cocaine self-administration and is associated with changes in dopamine (DA) function before drug exposure. Using positron emission tomography, we demonstrated that D2/3 receptor availability is significantly reduced in the nucleus accumbens of impulsive rats that were never exposed to cocaine and that such effects are independent of DA release. These data demonstrate that trait impulsivity predicts cocaine reinforcement and that D2 receptor dysfunction in abstinent cocaine addicts may, in part, be determined by premorbid influences.
Behavioral attributes of trait impulsivity on the 5-CSRT task. (A) Impulsive rats exhibit high levels of premature responding on days when visual targets are presented either 5 s after trial initiation (days 1, 2, 4, and 5) or 7 s after trial initiation (day 3), as compared to non-impulsive rats. Two-way analysis of variance (ANOVA) of premature responses revealed a significant main effect of day [F(4,40) = 144.9, P < 0.01] and a significant main effect of group [F(1,10) = 26.1, P < 0.01]. However, there were no significant effects on other measures of task performance, including (B) attentional accuracy [F(1,10) = 1.17, P = 0.306], (C) latency to collect food reward [F < 1, not significant (ns)], (D) omissions (F < 1, ns), (E) latency to respond correctly [F(1,10) = 3.0, P = 0.113], and (F) the time required to complete both standard and challenge (long-ITI) sessions (F < 1, ns). Black circles, high-impulsive rats; white circles, non-impulsive rats.
Reduced binding potential (BP) of the selective D2/3 receptor antagonist [18F]fallypride in the ventral striatum of drug-naΓ―ve trait-impulsive rats (n = 6 rats) as compared to drug-naΓ―ve non-impulsive rats (n = 6). (Top) ROIs are shown in the schematic coronal sections of the rat forebrain [adapted from (46)]. Dorsal and ventral striatal ROIs are depicted by the shaded and striped circles, respectively. Anterior-posterior coordinates (in millimeters) relative to bregma are shown on each coronal section. The ROIs have diameters of 2 mm in the transverse plane. BP values are averages of left and right striata. (A to D) Horizontal MR coregistered PET images of [18F]fallypride binding in the dorsal (upper panels) and ventral (lower panels) striatum of a non-impulsive rat [(A) and (C)] and a high-impulsive rat [(B) and (D)]. The images are 4.5 mm [(A) and (B)] and 7.0 mm [(C) and (D)] below the dorsal brain surface (BP threshold = 9).
Differential escalation of intravenous cocaine self-administration in high-impulsive rats (n = 8) as compared to non-impulsive rats (n = 8). On the first 5 days, access to cocaine was restricted to 5 hours and a maximum of 50 infusions. After a withdrawal period of 9 days, access to cocaine was increased on each of the following 5 days to 8 hours and a maximum of 150 infusions. This pattern of intermittent cocaine self-administration was repeated on two further occasions. Impulsive rats showed a differential increase in their rate of cocaine self-administration after extended access to cocaine [session: F(19,133) = 2.04, P = 0.01; group: F(1,14) = 32.82, P < 0.001; session Γ group: F(19,133) = 1.92, P = 0.017]. Subsequent pairwise comparisons revealed significant differences (P < 0.05) between the first session and sessions 10, 13, 14, and 15 for the non-impulsive group and between the first session and all sessions but nos. 2, 3, 4, 10, and 16 for the high-impulsive group. Black circles, high-impulsive rats; white circles, non-impulsive rats.
Effects of intermittent intravenous cocaine self-administration in high-impulsive rats (n = 8) and non-impulsive rats (n = 8) on sustained visual attention on the 5-CSRT task. (A) Rats were withdrawn from intravenous cocaine self-administration on four occasions and tested 24 hours later for 7 consecutive days on the 5-CSRT task. ShA, tested after short access to cocaine over 5 days, when rats received 50 cocaine infusions over 5 hours; LgA-1, tested after long access to cocaine, when the daily number of cocaine infusions increased to 150 and the session duration to 8 hours; LgA-2, tested after a second long-access exposure to cocaine; LgA-3, tested after a third long-access exposure to cocaine. ANOVA of premature responses revealed significant group Γ cycle [F(3,42) = 7.86, P = 0.023] and group Γ cycle Γ session [F(18,252) = 4.29, P < 0.001] interactions. Subsequent analyses revealed that premature responding was higher in high-impulsive rats as compared to non-impulsive rats during the ShA cycle [group: F(1,14) = 20.58, P < 0.001] but not during subsequent LgA-1 [F(1,14) = 0.62, P = 0.44], LgA-2 [F(1,14) = 3.82, P = 0.071], and LgA-3 [F(1,14) = 0.51, P = 0.49] cycles. There were no significant differences between non-impulsive and high-impulsive rats with respect to (B) attentional accuracy, (C) omissions, and (D) correct response latency (F < 1.44, P > 0.24 for all comparisons). Black circles, high-impulsive rats; white circles, non-impulsive rats.
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