Neuropharmacological and Neurogenetic Correlates of Opioid Use Disorder (OUD) As a Function of Ethnicity: Relevance to Precision Addiction Medicine

Tomilowo Abijo; Kenneth Blum; Marjorie C Gondré-Lewis

doi:10.2174/1570159X17666191118125702

Neuropharmacological and Neurogenetic Correlates of Opioid Use Disorder (OUD) As a Function of Ethnicity: Relevance to Precision Addiction Medicine

Curr Neuropharmacol. 2020;18(7):578-595. doi: 10.2174/1570159X17666191118125702.

Authors

Tomilowo Abijo^{1

2}, Kenneth Blum³, Marjorie C Gondré-Lewis^{1

2}

Affiliations

¹ Neuropsychopharmacology Laboratory, Howard University College of Medicine, Washington D.C., United States.
² Developmental Neuropsychopharmacology Laboratory, Department of Anatomy, Howard University College of Medicine, Washington D.C., USA
³ Graduate School of Biomedical Science, Western University Health Sciences, Pomona, CA., USA

Abstract

Background: Over 100 people die daily from opioid overdose and $78.5B per year is spent on treatment efforts, however, the real societal cost is multifold greater. Alternative strategies to eradicate/manage drug misuse and addiction need consideration. The perception of opioid addiction as a social/criminal problem has evolved to evidence-based considerations of them as clinical disorders with a genetic basis. We present evaluations of the genetics of addiction with ancestryspecific risk profiles for consideration.

Objective: Studies of gene variants associated with predisposition to substance use disorders (SUDs) are monolithic, and exclude many ethnic groups, especially Hispanics and African Americans. We evaluate gene polymorphisms that impact brain reward and predispose individuals to opioid addictions, with a focus on the disparity of research which includes individuals of African and Hispanic descent.

Methodology: PubMed and Google Scholar were searched for: Opioid Use Disorder (OUD), Genome- wide association studies (GWAS); genetic variants; polymorphisms, restriction fragment length polymorphisms (RFLP); genomics, epigenetics, race, ethnic group, ethnicity, ancestry, Caucasian/ White, African American/Black, Hispanic, Asian, addictive behaviors, reward deficiency syndrome (RDS), mutation, insertion/deletion, and promotor region.

Results: Many studies exclude non-White individuals. Studies that include diverse populations report ethnicity-specific frequencies of risk genes, with certain polymorphisms specifically associated with Caucasian and not African-American or Hispanic susceptibility to OUD or SUDs, and vice versa.

Conclusion: To adapt precision medicine-based addiction management in a blended society, we propose that ethnicity/ancestry-informed genetic variations must be analyzed to provide real precision- guided therapeutics with the intent to attenuate this uncontrollable fatal epidemic.

Keywords: Dopamine homeostasis; Precision Addiction Management (PAM); Reward Deficiency Syndrome (RDS); ethnic groups; gene guided therapy; genetics.

Publication types

Review

MeSH terms

Addiction Medicine
Animals
Behavior, Addictive / genetics
Black or African American / genetics
Ethnicity / genetics*
Genotype
Hispanic or Latino / genetics
Humans
Opioid-Related Disorders / genetics*
Polymorphism, Genetic
Precision Medicine

Grants and funding

R01 AA021262/AA/NIAAA NIH HHS/United States