(2012). A transmitter that KOR may interact with in producing these effects is noradrenaline. Noradrenaline plays a key role in stress responses (Dunn and Swiergiel 2008). The distribution of KOR and noradrenaline receptors overlap in a number of brain regions involved in reinstatement of drug and alcohol seeking (Mansour et al. 1987; Zilles et al. 1993), and KOR stimulation can affect

the release of noradrenaline Inhibitors,research,lifescience,medical from terminals in forebrain areas (Grilli et al. 2009). U50,488-induced reinstatement of CPP to cocaine in mice was reduced by injections of nor-BNI into the locus coeruleus, the location of noradrenergic cell bodies that project to the hippocampus and cortex (Al-Hasani et al. 2013). KOR in the locus coeruleus has also been implicated in liability to opioid abuse (Van Bockstaele et al. 2010). Future experiments should be directed at GDC-0973 research buy exploring the potential interaction of noradrenaline and KOR in alcohol seeking. Inhibitors,research,lifescience,medical Our findings of blockade of cue-induced reinstatement of alcohol seeking by nor-BNI are in agreement with those of Schank et al. (2012) who showed a significant blockade of cue-induced reinstatement of alcohol seeking by another KOR antagonist JDTic. Taken together, these Inhibitors,research,lifescience,medical data suggest that KOR play a key role in reinstatement induced by alcohol-associated cues. Data

from this study and earlier work shows that KOR are involved in stress as well as cue-induced alcohol seeking. This is consistent with the speculation that drug-associated cues are Inhibitors,research,lifescience,medical a form of stress (Karoly and Hutchison 2012). Drug-associated cues and stress have additive effects on reinstatement of

alcohol and cocaine seeking (Liu and Weiss 2002; Feltenstein and See 2006). The neuronal substrates Inhibitors,research,lifescience,medical underlying cue-and stress-induced relapse overlap at a number of levels (Sinha and Li 2007), although there are also important differences (Liu and Weiss 2002). The brain areas in which DYN release underlies cue-induced drug seeking are not known. A likely candidate is the amygdala (Johansen et al. 2011; Young and Williams 2013). Rutecarpine This area is especially enriched in KOR (Mansour et al. 1987), and has been shown to mediate different aspects of learning and memory (Maren 1996; Dityatev and Bolshakov 2005). Future studies could be aimed at determining the effects of local application of KOR antagonists on cue-induced reinstatement of alcohol seeking. CRF R1 and KOR interaction in alcohol seeking Evidence for a KOR-CRF R interaction in modulating reinstatement of alcohol seeking was also found. The CRF R1 antagonist antalarmin significantly reduced reinstatement of alcohol seeking induced by U50,488. This supports the results of Valdez et al. (2007), who found that the CRF R1 antagonist CP154,526 significantly reduced reinstatement of cocaine seeking induced by the KOR agonist spiradoline, and extends them to alcohol seeking.