Neurological correlates of brain reward circuitry linked to opioid use disorder (OUD): Do homo sapiens acquire or have a reward deficiency syndrome?

Mark S Gold; David Baron; Abdalla Bowirrat; Kenneth Blum

doi:10.1016/j.jns.2020.117137

Neurological correlates of brain reward circuitry linked to opioid use disorder (OUD): Do homo sapiens acquire or have a reward deficiency syndrome?

J Neurol Sci. 2020 Nov 15:418:117137. doi: 10.1016/j.jns.2020.117137. Epub 2020 Sep 15.

Authors

Mark S Gold¹, David Baron², Abdalla Bowirrat³, Kenneth Blum²

Affiliations

¹ Department of Psychiatry, Washington University School of Medicine, St. Louis, MO, United States. Electronic address: drmarkgold@gmail.com.
² Graduate School of Biomedical Sciences, Western University Health Sciences, Pomona, CA, United States.
³ Department of Neuroscience and Genetics, Interdisciplinary Center Herzliya, Israel.

Abstract

The extant literature confirms that an array of polymorphic genes related to- neurotransmitters and second messengers govern the net release of dopamine in the Nucleus Accumbens (NAc) in the mesolimbic region of the brain. They are linked predominantly to motivation, anti-stress, incentive salience (wanting), and wellbeing. Notably, in 2000 the Nobel Prize was awarded to Carlsson, Greengard, and Kandel for their work on the molecular and cellular function of dopaminergic activity at neurons. This historical psychopharmacological work involved neurotransmission of serotonin, endorphins, glutamate, and dopamine, and the seminal work of Blum, Gold, Volkow, Nestler, and others related to neurotransmitter function and related behaviors. Currently, Americans are facing their second and worst opioid epidemic, prescribed opioids, and easy access drive this epidemic of overdoses, and opioid use disorders (OUDs). Presently the clinical consensus is to treat OUD, as if it were an opioid deficiency syndrome, with long-term to life-long opioid substitution therapy. Opioid agonist administration is seen as necessary to replace missing opioids, treat OUD, and prevent overdoses, like insulin is used to treat diabetes. Treatment of OUD and addiction, in general, is similar to the endocrinopathy conceptualization in that it views opioid agonist MATs as an essential core to therapy. Is this approach logical? Other than as harm reduction, is using opioids to treat OUD therapeutic or harmful in the long term? This historical Trieste provides a molecular framework to understand the current underpinnings of endorphinergic/dopaminergic mechanisms related to opioid deficiency syndrome and generalized reward processing depletion. WC 249.

Keywords: Brain reward Cascade (BRC); Dopamine deficiency syndrome; Dopamine release and homeostasis; Endorphinergic deficiency syndrome; Endorphinergic mechanisms; Genetic testing of addiction liability; Neurotransmission; Opioid use disorder (OUD); Precision addiction management’; Reward deficiency syndrome (RDS).

Publication types

Review

MeSH terms

Behavior, Addictive*
Brain
Humans
Opioid-Related Disorders* / drug therapy
Reward
Syndrome