18,26,27 These effects have been shown recently to drive increase

18,26,27 These effects have been shown recently to drive increased drug self-administration and relapse, presumably through a process of negative reinforcement.28 These now actions of CREB seem to involve both major subtypes of NAc medium spiny neurons, those that express predominantly D1 versus D2 dopamine receptors.24 Interestingly, a large body of literature has shown that CREB, acting in hippocampus and amygdala, is a key molecule in behavioral memory.29-31 This broad role in addiction and behavioral memory likely reflects the fact

that neurons are imbued with a finite number of molecular mechanisms with which to adapt to Inhibitors,research,lifescience,medical a constantly changing Inhibitors,research,lifescience,medical environment. Target genes for CREB that mediate this behavioral phenotype have been identified through genome-wide assays as well as more selected efforts.10,18,32 One example is the opioid peptide dynorphin: stimulant induction of dynorphin expression in NAc neurons, mediated via CREB, increases dynorphin activation of k opioid receptors on VTA dopamine neurons and thereby suppresses dopaminergic transmission to the NAc and impairs reward.18 Several other CREB targets have been shown to be important for drug-induced synaptic plasticity, as

discussed below. While CREB is Inhibitors,research,lifescience,medical also Inhibitors,research,lifescience,medical activated in several other brain thorough regions by stimulants and opiates,23,24 less is known about the behavioral consequences of this effect and the target genes through which they occur. Likewise, less is known about CREB’s role in mediating the actions of other drugs of abuse.19 ΔFosB Acute exposure to virtually any drug of abuse induces all Fos family transcription factors

in NAc and several other Inhibitors,research,lifescience,medical brain regions. This induction is rapid but also highly transient, with Fos protein levels reverting to normal within 8 to 12 hours. Uniquely among these Fos family proteins is ΔFosB, a truncated product of the FosB gene, which by virtue of its unusual stability, gradually accumulates through a course of repeated drug exposure Cilengitide and becomes the predominant Fos protein expressed under these conditions.22,33 Moreover, because of this stability, levels of ΔFosB persist for weeks after drug withdrawal. Such chronic induction of ΔFosB has been demonstrated for virtually all drugs of abuse34 and, for most drugs, is selective for Dl-type NAc neurons.34,35 It has also been demonstrated in human addicts.35 A large body of literature has demonstrated that such ΔFosB induction in D1-type NAc neurons increases an animal’s sensitivity to drug as well as natural rewards and promotes drug self-administration, presumably through a process of positive reinforcement (see refs 34 to 38).

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