Cocaine addiction is characterized by excessive demand for drug and high propensity to relapse to drug seeking after quitting. Although many people experiment with drugs, individuals differ substantially in the degree to which addiction-related behaviors occur after drug exposure. Extensive research over the last 10 years has shown that the hypothalamic orexin neuropeptide system contributes importantly to reward processing, including cocaine demand and seeking. However, the role of orexins in either individual differences in cocaine demand and seeking ('trait' factors associated with increased risk of cocaine abuse), or in the excessive demand and seeking that occurs after extensive drug exposure ('state' factors associated with cocaine addiction), is unknown. Here, we will use a novel behavioral economics approach, combined with antisense knockdown, optogenetics, pharmacology and Fos staining, to measure the role of orexin signaling as a 'trait' factor that contributes to individual differences in cocaine demand and seeking. We will use similar methods in a model of cocaine addiction (long-access cocaine self-administration) to determine the role of orexin in 'state' factors that lead to addiction. In addition, we will examine trait-stte interactions, and determine what role orexin plays in the propensity for some individuals to readily transition to excessive drug seeking after extensive cocaine self-administration. Our preliminary studies indicate that high cocaine demand is a reliable predictor of high propensity to relapse to cocaine seeking; we will determine the role of orexin in this relationship. We will also determine which subpopulations of orexin neurons mediate cocaine demand and relapse in non-addicted subjects, as well as in the long access model of cocaine addiction. These studies will delineate the role of orexins in motivational differences that occur naturally within a population, and that may put certain individuals at risk for drug abuse. They will also provide the first test of orexin's role in the excessive demand and drug seeking in addiction, produced by prolonged experience with cocaine. We predict that spontaneous individual variability in cocaine demand and seeking involves the level of engagement of specific orexin neuronal subpopulations, and that the excessive demand and inflexible seeking characteristic of addiction corresponds to excessive orexin signaling. We also will examine the possibility that this excessive signaling in addiction may involve interactions between subpopulations of reward-related and stress-related orexin neurons. This research also has translational potential for individualized treatment: Addicts that exhibit high demand for cocaine may particularly benefit from treatments to attenuate signaling in an overly active orexin system.

Public Health Relevance

Cocaine addiction is a chronic condition that remains clinically difficult to treat. The proposed studies will reveal the role of a key brain neuropeptid system in individual differences in propensity for cocaine abuse, and in the excessive demand and relapse propensity that characterizes cocaine addiction. These findings will increase our knowledge of brain mechanisms involved in addiction, and include a test to identify addicts that may particularly benefit from orexin-based therapy.

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA006214-28
Application #
9232098
Study Section
Neurobiology of Motivated Behavior Study Section (NMB)
Program Officer
Volman, Susan
Project Start
1992-08-01
Project End
2019-02-28
Budget Start
2017-03-01
Budget End
2018-02-28
Support Year
28
Fiscal Year
2017
Total Cost
$393,727
Indirect Cost
$146,100
Name
Rbhs-Robert Wood Johnson Medical School
Department
Psychiatry
Type
Schools of Medicine
DUNS #
078795875
City
Piscataway
State
NJ
Country
United States
Zip Code
08854
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Bowrey, Hannah E; James, Morgan H; Aston-Jones, Gary (2017) New directions for the treatment of depression: Targeting the photic regulation of arousal and mood (PRAM) pathway. Depress Anxiety 34:588-595

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