Ventral Pallidum Output Pathways in Context-Induced Reinstatement of Alcohol Seeking

• Published in: The Journal of neuroscience Vol. 36; no. 46; pp. 11716 - 11726
• Main Authors: Prasad, Asheeta A, McNally, Gavan P
• Format: Journal Article
• Language: English
• Published: United States Society for Neuroscience 16.11.2016
• Subjects: Animals; Basal Forebrain - cytology; Basal Forebrain - drug effects; Basal Forebrain - physiology; Conditioning, Operant - drug effects; Conditioning, Operant - physiology; Drug-Seeking Behavior - drug effects; Drug-Seeking Behavior - physiology; Efferent Pathways - cytology; Efferent Pathways - drug effects; Efferent Pathways - physiology; Ethanol - administration & dosage; Extinction, Psychological - drug effects; Extinction, Psychological - physiology; Male; Nerve Net - cytology; Nerve Net - drug effects; Nerve Net - physiology; Neuronal Plasticity - drug effects; Neuronal Plasticity - physiology; Rats; Rats, Sprague-Dawley; Recurrence; ventral pallidum; reinstatement; relapse; DREADD
• ISSN: 0270-6474; 1529-2401; 1529-2401
• DOI: 10.1523/jneurosci.2580-16.2016

Ventral pallidum (VP) is a well-established locus for the reinforcing effects of drugs of abuse and reinstatement of drug seeking. However, VP neurons are at the origin of multiple output pathways, with strong projections to ventral tegmental area (VTA), subthalamic nucleus (STN), lateral hypothalamus, among others, and the roles of these VP output pathways in reinstatement of drug seeking remain poorly understood. Here we addressed these issues using a combination of neuroanatomical tracing and chemogenetic approaches. First, using dual-retrograde tracing, we show that VP neurons projecting to either VTA or STN are recruited during context-induced reinstatement of extinguished alcohol seeking in rats. Then, using chemogenetics, we show modulation of context-induced reinstatement and reacquisition of alcohol seeking via designer receptors exclusively activated by designer drugs excitation or inhibition of the VP. To determine the causal roles of VP → VTA and VP → STN pathways in context-induced reinstatement and reacquisition we used a chemogenetic disconnection approach and show that silencing either the VP → VTA or VP → STN pathways is sufficient to reduce both reinstatement and reacquisition of alcohol seeking. Moreover, these disconnections also each reduced responding and motivation during a progressive ratio test but had no effect on locomotor activity. Together, these results show that multiple ventral pallidal output pathways contribute to relapse to alcohol seeking. Ventral pallidum (VP) serves important roles in reward and motivation and is a critical node in the neural circuitry for reinstatement of drug seeking. Despite being a common locus for different forms of reinstatement, fundamental aspects of neural circuitry for these VP contributions to reinstatement of drug seeking remain unknown. Here we used a combination of neuroanatomical tracing and chemogenetic approaches to map the VP output pathways for context-induced reinstatement and reacquisition of alcohol seeking. We show that VP output pathways to the subthalamic nucleus and also to the ventral tegmental area are necessary for these forms of reinstatement.