A Review of DNA Risk Alleles to Determine Epigenetic Repair of mRNA Expression to Prove Therapeutic Effectiveness in Reward Deficiency Syndrome (RDS): Embracing "Precision Behavioral Management".

This is a review of research on "Precision Behavioral Management" of substance use disorder (SUD). America is experiencing a high prevalence of substance use disorder, primarily involving legal and illegal opioid use. A 3000% increase in treatment for substance abuse has occurred between 2000 and 2016. Unfortunately, present day treatment of opioid abuse involves providing replacement therapy with powerful opioids to, at best, induce harm reduction, not prophylaxis. These interventions do not enhance gene expression and restore the balance of the brain reward system's neurotransmitters. We are proposing a generalized approach called "Precision Behavioral Management". This approach includes 1) using the Genetic Addiction Risk Severity (GARS, a 10 candidate polymorphic gene panel shown to predict ASI-alcohol and drug severity) to assess early pre-disposition to substance use disorder; 2) using a validated reward deficiency syndrome (RDS) questionnaire; 3) utilization of the Comprehensive Analysis of Reported Drugs (CARD™) to assess treatment compliance and abstinence from illicit drugs during treatment, and, importantly; 4) utilization of a "Pro-dopamine regulator (KB220)" (via IV or oral [KB220Z] delivery systems) to optimize gene expression, restore the balance of the Brain Reward Cascade's neurotransmitter systems and prevent relapse by induction of dopamine homeostasis, and; 5) utilization of targeted DNA polymorphic reward genes to direct mRNA genetic expression profiling during the treatment process. Incorporation of these events can be applied to not only the under-considered African-American RDS community, but all victims of RDS, as a demonstration of a paradigm shift that uniquely provides a novel putative "standard of care" based on DNA guided precision nutrition therapy to induce "dopamine homeostasis" and rebalance neurotransmitters in the Brain Reward Cascade. We are also developing a Reward Deficiency Syndrome Diagnostic Criteria (RDSDC) to assist in potential tertiary treatment.

Introduction

Success in survival is accompanied by the pleasure of reward satisfaction. In assessing the nature of the out-of-control epidemic of Substance Use Disorder (SUD) conventional perspectives portray SUD as occurring in people who are in some way impaired or somewhat broken, stigmatizing individuals. After more than six decades of published clinical research such diagnostic conclusions are most likely inaccurate. In our view, individuals who carry genetic predispositions to engage in excessive reward seeking or self-medicating behaviors, are arguably high-performing beings, most fit to survive. In a pristine environment with an abundance of healthy natural nutritional “fuel” resources (ie, high-performance fuel) such individuals would have better global/environmental awareness; be more focused, more competitive, better hunters, have greater athletic prowess, and/or be celebrities or leaders in their communities. But, in the absence of superior nutritional fuel resources, such individuals lack those attributes and are unable to achieve reward satisfaction from normal lifestyle thoughts and behaviors. Their inability to achieve reward satisfaction motivates their engagement in excessive reward-seeking or self-medicating behavior. An understanding of this duality in reward seeking behavior may eliminate the potential for a stigma. Our laboratory is focused on reducing stigma to for example alcoholism, by adaptation of the term “Hypodopaminism.”

It is well known that America is experiencing an epidemic of Substance Use Disorder (SUD), associated with licit and illicit opiates/opioids used in the pursuit of reward satisfaction, to avoid pain, and to feel good. Between 2000 and 2016 drug treatment utilization has increased 3000%. Unfortunately, present day treatment of opioid abuse involves providing replacement therapy with other powerful pharmaceutical opioids to, at best, induce harm reduction; but not as prophylaxis. These interventions do not nourish the ability to enhance gene expression and restore the balance of the brain reward system’s neurotransmitters.

In 2013, the National Survey on Drug Abuse and Health (NSDUH)1 estimated that 24.6 million people, 12 or older (9.4% of the American population), used illegal drugs, in the past month and this number increased further to 35.8 million (13% of the population) in 2019. During this six-year time frame, 11.2 million additional people endorsed using illicit drugs during the prior month and 7 million additional people initiated use of marijuana (cannabis). In addition, illicit, past-year drug use for individuals 12+ years, increased from 41.6 million to 57.2 million people. In 2019, the three most often used illicit drugs, were marijuana, opioids and pain relievers.2

The 2014 and 2019 data from NSDUH indicate slight declines in the percentages of past year users of heroin and users of pain reducing medications, with Opioid Use Disorder also decreasing in that time frame. However, the prevalence of past year opiate use, for people twelve years and older, was still high in 2019 at 10.1 million individuals. Among those individuals, 92% of them misused pain relievers, exclusively.2

The number of new drug users in 2013 was 2.8 million. New users increased to 16.5 million in 2019, with another 4.9 million new users of alcohol, followed by marijuana with 3.5 million new users.2 The cost of alcohol abuse is high. Alcohol was associated with 97,000 reports of date rape and sexual assault, and 696,000 physical assaults, in general, were committed by students affected by alcohol.3

The National Institute of Drug Abuse (NIDA) recently presented their Monitoring the Future (MTF) Survey4 of drug use and attitudes for 42,500 8th, 10th and 12th graders from almost 400 public and private schools in the US. The MTF Survey found that vaping is prevalent and has increased for high school students and Marijuana use has increased from 2018 to 2019. Lifetime use of alcohol has continued to decline from 1994 through 2019 for all high school grades. Misuse of narcotics “other than heroin” has declined for 12 grade students. Vicodin use has decreased for 10th and 12th graders and Oxycontin use has also decreased for 12th grade students. Misuse of prescription opioids is low, and heroin use has declined from 2014 to 2019 for 10th and 12th grade students.

While this general landscape seems promising the opioid crisis is indeed, during this period of a viral pandemic, increasing. Most recently the Director of the National Institute of Drug Abuse (NIDA), Nora Volkow commented that job losses and social isolation associated with the Covid-19 pandemic may increase opioid overdoses by 30% to 40%.5 Although this statistic is anecdotal, it is indeed a grave concern to health-care professionals. The cost of the opioid epidemic is high. The Society of Actuaries6 reported that the United States had experienced 400,000 opioid-related deaths from 1997 to 2017 and estimated the total economic burden of opioid misuse and death, from 2015 to 2018 to be 631 billion dollars. Their 2019 cost projection was 188 billion dollars. These figures include the costs of additional health-care services, premature mortality, child and family support, lost productivity, education and criminal justice activity.

Perspective and Goals of This Review

Understanding these facts, one aim of this review is to delineate the current genomic disparity of various ethnic groups, especially African-Americans, and discuss how variations in dopamine (DRD2) receptor alleles (A1 vs A2) may convey vulnerability for Reward Deficiency Syndrome (RDS). RDS is a cluster of disorders, including drug and alcohol addiction that are related to low dopamine metabolism. We must note that in discussing genomic and racial disparity, we are not implying that race or ethnicity causes RDS conditions, but explicitly indicating that variants in dopamine D2 alleles, moderated by the social and economic conditions of our lives, may increase our risk for RDS illnesses such as alcoholism and Opiate/Opioid Use Disorder (OUD). The investigation of genetic variants related to addiction, for example, in the African-American community is important since African-Americans have been under represented in research on genetic correlates of addiction.7

It is indeed important not to target any particular group whether Caucasian, Latino, Black or Asian, but to encourage more genomic type research to at least include an array of these diverse ethnicities in their respective studies before any unfounded interpretations are enunciated.

In addition, another goal of this review is to provide some novel concepts that could become future treatments and a prophylactic model for the entire field of Reward Deficiency Syndrome (RDS). RDS is the umbrella term for all non-substance and substance-dependent behaviors, coined by one of our authors (KB) in 1995. The treatment and prophylactic model we will discuss includes assessment of genetic vulnerability for RDS, use of an RDS questionnaire, monitoring compliance with drug treatment, use of pro-dopamine regulation to establish dopamine homeostasis and impact DNA polymorphic reward genes to influence mRNA genetic expression during drug treatment. These innovations could have significant value for minority populations and people of color who have been dramatically under-served by the health-care system and have had limited access to innovative health care and substance use treatments.

Substance Use Disorder and Ethnicity

Wu et al8 employed a case–control design to study the association of the A1 and B1 DRD2 alleles with smoking vs non-smoking status in lung cancer cases and controls for their African-American and Mexican-American participants. They found that 50% of a community-based sample of 111 African-American controls (albeit not properly screened to eliminate all RDS behaviors) carried the DRD2 A1/A2 receptor alleles, compared to 56% for Mexican-American control participants. This difference was not statistically significant. These alleles, in combination with other genetic variants that affect the Brain Reward Cascade, have been postulated by Blum et al9–11 to contribute unhealthy reward seeking behaviors consistent with how the DRD2 A1 allele functions in reward regardless of race or ethnicity. Combined with the important role of social, economic and legal variables, the net potential effect of an individual’s genetic and epigenetic landscape on behavior can have a devastating inequitable outcome on the life of that individual and on their community. In speaking of genetics and behavior, we are not implying genetic determinism, but rather a genetic contribution to a complex interaction of factors that shape the final behavioral and societal outcome also involving epigenetic insults. Indeed, African-American communities are over policed and experience drug possession charges substantially more frequently than Caucasian drug users.12 Furthermore, compared to Caucasian drug users, addiction in the African-American community is often criminalized,13 rather than treated as a medical emergency.

The NSDUH 2020 survey2 revealed that 2019 rates of illicit, past month drug use for adults, 18+ were 14% for Whites, 15.3% for Blacks or African-Americans, 14.8% for Native Americans/Alaskan Natives, 11% for Native Hawaiians or Pacific Islanders, 5.9% for Asians, and 11.3% for Hispanic or Latino individuals. Rates of SUD for adults were 8.1% Whites, 7.6% for Black or African-Americans, 7.0% for Hispanic or Latinos, 4.6% for Asian-Americans, 10.2% for Native American or Alaskan Natives and 8.3% for Native Hawaiian or Pacific Islanders. Although SUD rates were somewhat higher for Native Americans/Alaskan Natives and Native Hawaiian or Pacific Islanders, and lower for Asians, it is important to note that SUD rates for White, Black, and Hispanic or Latino individuals are fundamentally the same.

In summary, the above statistics do not support big differences between ethnic groups for Substance Use Disorder (SUD), which, in our view, may be more related to an interaction between genetic vulnerability for addiction, epigenetic factors and the social and economic conditions that affect peoples’ lives, rather than general ethnic values and attitudes. We believe that the data we have presented suggest that the allegations of racial profiling, associated with the war on drugs, are likely correct; only the causes espoused by conventional perspectives are to be disputed. The take home message here is that racial or ethnic bias in the investigation and prosecution of drug-related crimes cannot be justified and should cease.

While there may not be a difference in a “cultural romance with drugs” in terms of comparative ethnic groups (ie, African-Americans vs American Caucasians), genomic disparity is an important issue that can inform targeted, personalized therapeutic strategies to treat drug addiction. Both treatment and prevention tactics must be adequately addressed, and informed by a psychosocial genetics approach. In an effort to shed some new light on this very important issue, the authors, have gathered information from an array of different backgrounds, pooling experience, academic knowledge, and data, that indicates a paradigm shift called “Precision Behavioral Management” is occurring and has therapeutic potential in the future.14–20

Precision Behavioral Management

While we are particularly interested in the reasons for addiction to drugs within the African-American and other ethnic groups in various communities across America, we are proposing a generalized approach called “Precision Behavioral Management” to address this problem. This approach consists of; 1) Using the Genetic Addiction Risk Severity assessment (GARS, a 10 candidate polymorphic gene panel shown to predict the Addiction Severity Index, ASI-alcohol and drug severity)21 to assess early pre-disposition to Substance Use Disorder;9,22 2) A validated RDS questionnaire;23 3) Utilization of the Comprehensive Analysis of Reported Drugs (CARD™)9,22 to assess treatment compliance and abstinence from illicit drugs during treatment24,25 and, importantly; 4) Initiation of oral and IV therapy utilization of a DNA guided “Pro-dopamine regulator (KB220Z and KB220 respectively)” to optimize gene expression, restore the balance of the Brain Reward Cascade’s neurotransmitter systems and prevent relapse by induction of dopamine homeostasis26,27 and; 5) Utilization of targeted DNA polymorphic reward genes to direct mRNA genetic expression profiling during the treatment process.28 These concepts will provide a framework for this review. Incorporation of these events can be applied in benefit of, for example, the African–American community, as a demonstration of a paradigm shift that has been the subject of an NIH grant. This unique program is called the “Reward Deficiency Syndrome Solution System”TM (RDSSS).

The following sections of this review will provide the rationale for our proposition of “Precision Behavioral Management”. Blum’s group is currently engaged in the novel development of utilizable Reward Deficiency Syndrome diagnostic criteria which will be published elsewhere.

Genetic Addiction Risk Severity (GARS)

The Brain Reward Cascade (BRC) describes the genetic and neurotransmitter interactions that regulate the release of dopamine. Alterations in the BRC, whether due to genetic or epigenetic factors, may predispose individuals to altered pain tolerance and addictive behaviors. The GARS accurately predicts RDS component behaviors, including vulnerability to pain, addiction and other compulsive behaviors. In this review, the authors propose innovative strategies for fighting opioid and prescription drug abuse and death, based on the role of dopaminergic tone in pain pathways. The mesolimbic projection system may influence pain sensitivity, and genetic polymorphisms associate with a predisposition to pain vulnerability or tolerance. Genetic polymorphisms offer targets for therapy that could help in pain treatment and, most important, identify risk for subsequent addiction.

The evaluation of genes like CB1, mu receptors and PENK, with pharmacogenomic tests offers the possibility to provide pharmacogenomic, individualized solutions, improve gene expression, rebalance neurotransmitters in the BRC to optimize mental and physical performance and improve treatment results. The genetic identification of RDS behavior risks, especially in groups with an increased percentage of genetic vulnerabilities, may be an important early technique to assist government agencies in improving the distribution of available financial resources.29,30

Blum et al was the first group to report a genetic association with severe alcoholism10 and later, cocaine.11 Although there was disagreement within the scientific community in the 1990s, the Dopamine D2 receptor (DRD2) gene, located on chromosome 11 q22q23,31 was the first gene identified to be associated with not only severe alcoholism, but more importantly, non-specific dopaminergic reward system impairment/inadequacies (anhedonia), which are central to all addictive behaviors.32 Following an historic controversy, Goldman’s group reported a meta-analysis of 62 studies of DRD2 and more than 16,000 participants with Alcohol Use Disorder (AUD). Alcohol Use Disorder showed a significant association with the rs1800497 Single Nucleotide Polymorphism (SNP). According to Goldman’s group30 the association resulted from low allele frequency in controls in positive studies which also explained some of the differences between these experiments. This is exactly what one should expect. The lower allelic presence of the DRD2 A1 allele in controls will improve robustness of association, especially when the rs1800497 SNP is found in approximately one-third of the American population. This was discussed by Blum’s and Goldman’s laboratories over 30 years ago33 and indicates the need for more robust controls that have been seriously screened to eliminate all RDS behaviors. We suggested that future gene research producing positive associations with dopaminergic polymorphisms and RDS behaviors, using controls that eliminated addictive, compulsive and impulsive behaviors in participants and their families could have important implications in any diverse population.34 Recruitment of these ‘super controls’ can prove challenging given the number of behaviors and psychiatric conditions under the umbrella of RDS or that are co-morbid with an RDS condition.

One source of differences in this research is variation in the frequency of A1 alleles in the control groups. Barr and Kidd35 studied the frequencies of the DRD2 A1 allele in various populations. They examined 381 unrelated people from 16 different populations. The frequency of the A1 allele varied from 0.09 in Ashkenazi Jews to 0.75 in Native American Indians. Due to these important variations in A1 allele frequency, as association study of this polymorphism must control for the ethnicity of the participants. The results of such studies must be interpreted with caution, which suggests a requirement to highly screen all RDS behaviors in controls (super controls). In fact, utilization of an approach to reduce hidden RDS behaviors in controls of families by Hill et al36 showed a rather low frequency of the DRD2 A1 allele, and this finding helped identify the linkage to severe alcoholism. Specifically, indicators of more severe alcoholism, eg, symptoms of physical dependence, earlier age of onset, or comorbid antisocial personality disorder, supported evidence for linkage. In addition, the Feighner criteria for alcoholism combined with one or more symptoms of physical dependence gave some evidence of linkage between two dopamine receptor alleles (Taq1 A and D4). Early age of onset and physical dependence (morning drinking, inability to stop drinking, withdrawal symptoms, binging) also gave some evidence for linkage. Finally, alcoholics with personality disorder showed significant differences in allele composition compared to non-alcoholics, for both D2 polymorphisms.37

It is indeed important to consider protective genetic mechanisms as a way of potential interventional therapeutic targets. Blum et al38 proposed that the Taq1 A2 allele of the dopamine D2 receptor gene is associated with a subtype of schizophrenia, not vulnerable to SUD, and the Taq1 A2 allele may provide some protection against alcohol addiction or dependence on other drugs of abuse.39 Previous research suggests that a deficiency of gamma type endorphins, that has been associated with schizophrenic type psychosis, may be a mechanism that explains alcohol seeking in schizophrenics with SUD.40 The present authors also suggest that schizophrenics who seek alcohol may be self-medicating by decreasing abnormal dopaminergic activity in the nucleus accumbens (NAc) via increased gamma endorphin activity. Further support of shared genetics is also derived from the Psychological Genetics of Addiction (PGA)23 studies in Hungary which suggest a substantial co-occurrence of addictions and compulsive behaviors. The authors emphasize the importance of studying the common neural, genetic and psychological mechanisms that may underlie this association. The PGA studies also support the component model of addictions and the RDS concept that suggests different addictive and compulsive behaviors share a common etiological and phenomenological background.41

Genes and the pathways underlying addiction have been revealed by new research technologies. Li et al42 in a comprehensive analysis of peer reviewed studies between 1976 and 2006, integrated 2343 pieces of evidence that linked chromosome regions and genes to addiction by single gene strategies, microarray, proteomics or genetic studies. Fifteen hundred human addiction related genes were identified. Their findings produced the Knowledgebase for Addiction Related Genes (KARG) network map (), a user friendly molecular database of genes related to addiction.

Their meta-analysis extracted 396 genes and each gene was supported by at least two lines of evidence. Li et al42 identified 18 statistically significant molecular pathways. Five of the pathways “enriched for all four different types of addictive drugs” including the Gonadotropin-releasing hormone (GnRH) signaling pathway and the gap junction, were suggested as underlying the rewarding and addictive effects of drugs. These pathways were integrated into a hypothetical molecular network for addiction. The network included both fast and slow positive feedback loops that were interconnected with calcium/calmodulin-dependent protein kinase II (CAMKII), a protein kinase that is involved in memory, which may explain the relative permanence of addiction. Finally, the common elements in this research include dopaminergic and glutaminergic genes.

The treatment of patients would be enhanced by classifying them for genetic risk for alcohol and drug seeking behavior, prior to the initiation of residential or non-residential chemical dependency or pain treatment programs. The authors have developed an addiction risk severity index based on 11 polymorphisms in 10 genes that contribute to the operation of the brain’s reward system. The Genetic Addiction Risk Severity test (GARS) includes six Single Nucleotide Polymorphisms (SNPs) in the DRD1, DRD2, DRD4, COMT, and OPRM1 genes. The GARS test also includes four simple sequence repeats (SSRs) in the DAT1, DRD4, MAOA and 5HTT transporter genes, as well as a dinucleotide polymorphism in the GABRA3 gene. Blum’s group22 approached the genetic risk for alcohol and substance abuse by examining the potential contribution of reward genes to a hypodopaminergia, and its linkage to RDS related substance abuse risk. The Blum et al21 report of findings included 393 poly drug using patients selected from eight independent treatment centers around the United States. The severity of substance misuse was evaluated with the Addiction Severity Index (ASI-MV). Saliva samples were provided by 273 patients, who also had ASI phenotyping, and these samples were subjected to DNA genotyping. The average age of individuals in the study was 35.3 years (S.D. 13.1 years, range was 18–70 years). The sample was 57.8% male (n = 160) and 88.1% (n = 244) white (self-report of race). The average number of GARS alleles was 7.97 (S.D. = 2.34), and the number of alleles ranged from 3 to 15. The genotypes were all in Hardy-Weinberg equilibrium (HWE). Initial evaluation of the association between the GARS results and the ASI scores, using Fisher’s Exact Test, showed a significant predictive value (x2= 8.84, df = 1, p.004, 2 tailed). This finding was still statistically significant after controlling for age (p < 0.01). Chi-square (p < 0.05) and linear regression (b = −0.122, t=−1.91, p = 0.057, 2 tailed) analyses of the relationship between the GARS panel and the ASI drug severity risk score were also significant, though less robust than the Fisher Exact Test result. The association between the GARS panel and the ASI score was statistically significant at p = 0.028, following correction for our a priori hypothesis. The Blum et al method data is the first report of the development of the GARS measure of alcohol and drug severity risk.21

Although it is important to conduct research with RDS free controls, studies to date have not accomplished this. Case–control studies, however, have used participants free of SUDs. We contend that the use of RDS free controls, if adopted properly, would decrease the frequency of false results and confusion regarding the contribution of genetics to addiction.21 Given the previous literature we have cited, we believe that there is a strong association between alcohol and drug risk. In our report,21 we note a total of 110,241 cases and 122,525 controls that came from the current literature. Although we can differ over the criteria for selecting these controls (eg, blood donors), there are many case–control studies reporting selective association of these risk alleles (measured with GARS), generally indicating the presence of hypodopaminergia in both cases and controls, thus providing genetic confusion, attenuated robustness and potentially spurious results.

In fact, the Blum et al study21 found that ≥7 risk alleles load onto prediction of alcohol severity, whereas ≥4 risk alleles load onto prediction of drug severity. The risk for alcohol and drug use severity increase, with increasing numbers of sequence variations in the genes that regulate dopamine signaling. Age is a meaningful covariate for the alcohol severity scores. Global research provides evidence that DRD2 receptor numbers decline with advancing age.43–46 Additional research may be needed to verify the contribution of these and other genetic variations to SUD. Even though there is some disagreement regarding the candidate approach compared to micro-array or cluster analysis techniques,47–54 the GARS assessment offers valuable information for substance use treatment, screening of patients for pain treatment and relapse prevention.21

Reward Deficiency Syndrome (RDS) Questionnaire

In conjunction with Zsolt Demetrovics in the Eötvös Loránd University, Institute of Psychology, Budapest, Hungary, an unpublished 29-item RDS questionnaire, was reduced from an initial 51 items that was generated based on the RDS construct. The questionnaire has been validated in over 1726 individuals attending college. Demetrovics and associates utilized Exploratory and Confirmatory Factor Analyses on four independent subsamples of the 1726 subjects. Specifically, a 5-factor solution had an optimal goodness of fit with a final factor analysis result: a reward deficiency trait was the main factor (Z. Demetrovics, personal communication, 2016).

This work will be published elsewhere with further in-depth details.

The Reward Deficiency Factor showed correlations with gender, sensation seeking and impulsivity. The reward deficiency trait showed greater expression in females. In addition, the reward deficiency trait was predicted by higher levels of sensation seeking and impulsivity. Impulsivity positively predicted the need for being in action. Male subjects showed a higher level of need for action. Need for overstimulation was not associated with any predictors. Finally, risk seeking behavior was positively associated with sensation seeking and impulsivity while reward deficiency was under control.55 We are aware that when evaluating RDS in AfricanAmericans or other cultures and geographies that differ from the Hungarian group, a culturally appropriate RDS questionnaire needs to be developed and validated for the RDS component to be informative.

Comprehensive Analysis of Reported Drugs (CARD)

In response to the rampant substance use problem in America, the Comprehensive Analysis of Reported Drugs (CARD) is providing treatment centers an objective means of evaluating their clients’ compliance with prescribed treatment and abstinence from illicit drugs. For many decades, Dominion Diagnostics has supplied modern, advanced drug testing education and support to drug treatment clinics. Dominion was unique in helping clinics to monitor drug elimination over time, using Creatinine-Adjusted levels. In 2004, the company was repeatedly asked to add medication compliance to their summary reports. In collaboration with the clinics, the following sources of data were developed: 1) a summary of testing results, including the number of patients who tested positive for illicit drugs in the prior quarter; 2) the number of patients receiving prescriptions for treatment related drugs in the quarter; 3) the number of patients taking the medication drugs; 4) identification of illicit drugs used by the patients; and 5) honesty of the patients in their self-reports of drug use. Following many iterations, the CARD assessment project was rolled out as a beta test in 2009. Notably, in 2011 Dominion began reviewing the data summaries followed by Blum et al25 data analysis in 2012. A multi-state sample of 2919 individuals, drawn from in-patient and outpatient settings, was retrospectively studied for treatment compliance (presence of prescribed medications) and abstinence (absence of prohibited drugs) verified by urine testing. The data from initial and final urine tests revealed a 67.2% compliance rate and a 39.2% abstinence rate. During a one year follow-up period, a randomly selected subset of 511 individuals was studied longitudinally with repeated urine tests to assess compliance and abstinence. Statistically significant increases in abstinence (p < 0.001) and compliance (p < 0.001) over time were observed. Increased compliance and abstinence, over time, may be attributed to the frequent use of urine testing and the beneficial effect of CARD on patient management and communication.25 In addition, Buprenorphine/Naloxone patients, involved in Opioid Substitution Programs, demonstrated statistically significant, increased compliance and abstinence during a one year, follow-up period.24,56 These encouraging initial findings suggest that CARD is useful for clinicians in establishing the presence or absence of illicit drugs in their clients. Additional research is necessary to establish long-term treatment benefits. CARD continues to be upgraded and there is now an inclusion of an expanded mental health panel of medications (ie, anti-depressants, etc.).

Pro-Dopamine Regulator (KB220 and Variants)

The dopaminergic-glutaminergic optimization complex, KB220, KB220Z and its variants were designed to balance the brain’s reward system through induction of “dopamine homeostasis”. These preparations offer potential clinical benefits to individuals suffering from RDS and they may support their recovery from dependence on opiates/opioids and other addictive behaviors.57–59 What follows is a review of biochemical actions of commonly used pharmaceutical Medication Assisted Treatment (MAT) and their potential anti-reward activity, a justification for the use of KB220Z, and an explanation of how the KB220Z is purported to target the dopamine pathway to enhance reward. Dopamine, serotonin, endorphins, cannabinoids and glutamine are important elements in the operation of the brain’s reward system. The United States is in the grip of an extraordinary level of opiate/opioid use, with 127 deaths per day, according to the Centers for Disease Control (CDC).

Unfortunately, cases of heroin overdose are increasing. Although MAT has been approved by the FDA, for nicotine, opiate and alcohol dependence, MAT is not yet available for abuse of stimulants or cannabis (Table 1). Acute use of MAT is beneficial in supporting “psychological extinction”, however, its chronic use blocks dopaminergic function, and dopamine is essential for the experience of pleasure and satisfaction through normal life experiences. Both the National Institutes on Alcohol Abuse & Alcoholism (NIAAA) and the National Institute on Drug Abuse (NIDA), institutions that deal with drug dependence and alcoholism, recognize the problem with MATs and support research into improved treatments.

Table 1

United States Federal Drug Authority (FDA) Approved Pharmaceutical Agents

Drug	Company	Purpose	Approval Date
Zubsolv®. Zubsolv® (buprenorphine and naloxone)	Orexo AB	Treatment of opioid dependence	July 2013
Vivitrol® extended release naltrexone	Alkermes	Prevention of relapse to opioid dependence	October 2010
Vivitrol® Naltrexone	Alkermes	Treatment of alcohol dependence	April 2006
CHANTIX® (varenicline)	Pfizer	Treatment of nicotine addiction	May 2006
Acamprosate calcium	Campral	Treatment of alcoholism	2004
Suboxone® (buprenorphine/naloxone) Subutex® (buprenorphine)	Reckitt Benckiser	Treatment of opiate dependence	October 2002
Nicoderm CQ ® Nicorette®	GlaxoSmithKline	For smoking cessation	May 1997
Naltrexone Hydrochloride oral tablets	Dupont	Tablet form (50mg taken daily) for the treatment of alcoholism	1994
Antabuse® (disulfiram)	Odyssey Pharmaceuticals	Treatment of alcohol dependence	1951

Notes: Febo M, Blum K, Badgaiyan RD, Perez PD, Colon-Perez LM, Thanos PK, et al. Enhanced functional connectivity and volume between cognitive and reward centers of naïve rodent brain produced by pro-dopaminergic agent KB220Z. PLoS ONE. 2017; 12(4): e0174774. © 2017 Febo et al. This is an open access article distributed under the terms of the Creative Commons Attribution License.109

The development of SUD treatments that affect dopamine and the brain reward system is an ongoing challenge. Table 1 presents, MAT approved by the FDA, to combat substance abuse. Although these approaches have been helpful to some patients, they do not prevent cravings and relapse. Recent results from the CARD study25 of abstinence from drug use and compliance with MAT in inpatient and outpatient settings revealed that only 39% of patients maintained abstinence but in fact 67% were compliant during the period of the research. However, the data indicated a trend towards increasing abstinence and compliance over a one year follow-up period.24,25 The authors acknowledged that these preliminary results require further research. The agents approved by the FDA for MAT may either reduce craving or block the pleasurable effect of drugs. Unfortunately, the latter effect may prevent patients from experiencing normal satisfaction from everyday life experiences. An overall analysis of CARD data for patients on MAT with combined buprenorphine and naloxone treatment (bup/nal) revealed that more than 92% of patients had evidence of bup/nal over the one year follow-up period, indicating good compliance. However, 47% of these patients also gave evidence of concomitant illicit drugs in their urine samples. Compliant patients, however, were more likely to be abstinent during treatment than non-compliant patients.24

A review of the existing FDA-approved drugs to treat various types of SUD behaviors reveals that the opposite or anti-reward mechanisms seem to predominate the listing (Table 1). Briefly, it is well known that narcotic antagonists (in any form) attenuate euphoria via opioid receptor blockade.60,61 Buprenorphine/naloxone may not consistently affect the cingulate gyrus or prevent relapse, and when used chronically, may have significant anti-reward characteristics that include a flat emotional affect due to lack of dopamine homeostasis.62 Bupropion may block DA re-uptake but does not increase extracellular DA in man.63 Acamprosate calcium regulates chemically induced release of dopamine in the Nucleus Accumbens (NAc).64 Decreased activation of the DA system and the failure to release adequate mesolimbic DA in the Nucleus Accumbens (NAc) over time can produce depression and potential suicidal ideation. While this is a bold statement, N-methyl-D-aspartate (NMDA) antagonists are known to inhibit glutamatergic drive in the Ventral Tegmental Area (VTA) ultimately resulting in decreased dopamine release at the NAc.65 There are studies showing poor outcomes with Acamprosate calcium in daily drinkers.66

Individuals with RDS have a hypodopaminergic state or trait. Properties of a hypodopaminergic trait might include having reduced receptors for serotonin and/or dopamine, or a rapid rate of synaptic dopamine breakdown due to a high catabolic genotype of the COMT gene.67 A hypodopaminergic state can be the result of the toxic effects of drugs like alcohol or even stress.68,69 The hypodopaminergic state or trait predisposes individuals to behave or medicate themselves in ways that stimulate dopamine release. Methods may include the use of cannabis, stimulants, opiates, alcohol, gambling, sex, nicotine, and even extreme internet gaming activities. Imaging studies70,71 document that individuals who abuse drugs have marked reductions in dopamine receptors and dopamine release and decreased dopamine activity is associated with increased impulsivity.72 The reduction in DA activity is correlated with reduced activity in several brain regions important for the regulation of behavior. The orbitofrontal cortex, a region of the brain that is involved in salience attribution, demonstrates decreased activity which results in compulsive behaviors. The cingulate gyrus, which is involved in inhibitory control, also shows decreased activity. Reduced cingulate activation contributes to impulsivity. Finally, the dorsolateral prefrontal cortex, which is involved in executive function, is disrupted which results in impaired regulation of intentional actions.70

Current treatment approaches to psychoactive substance abuse have not been very successful which provides an opportunity for new approaches to this problem. Chronic in vivo research with a D2 receptor agonist produces down-regulation,73 which is consistent with chronic treatment with an established D2 agonist, Quinpirole.74 In contrast, in vitro studies demonstrated that regardless of genetic antecedents, acute stimulation with Bromocriptine, a known D2 agonist, produces a notable increase in D2 receptors within the DA system.75–81 Stimulation of D2/D3 receptors signal negative-feedback-mechanisms that induce mRNA expression82 in the mesolimbic system and cause a proliferation of D2 receptors that results in significant clinical benefits for alcoholics.83 These results support the proposition that excessive craving behavior may be due to reduced numbers of DRD2 receptors. In contrast, drug cravings and the likelihood of relapse may be decreased by a normal or adequate number of D2 receptors. Thus, a treatment goal to prevent relapse of substance abuse might be the induction of increased (but balanced) D2 receptors in genetically vulnerable individuals.70 In addition, humans with alcohol use disorder have demonstrated reduced DRD2 receptor ligand binding in the striatum.84,85 Feltman et al86 have noted that chronic alcohol use might be an expression of reduced levels of D2 receptors, resulting from a reduction in DRD2-DRD2 homoreceptor complexes and gene expression. In addition, these authors suggest that given the antagonistic relationship between the adenosine A2A receptor (A2AR) and DRD2 receptors, reduced affinity and signaling of the DRD2 receptor population might result from the increased density of A2AR-DRD2 heteroceptor complexes. Thus, in humans with Alcohol Use Disorder (AUD), decreased levels of striatal DRD2 and decreased protomer affinity in the striatal A2AR-D2R heteroceptor complex offers a promising target of treatment for AUD.

Prior theories about dopamine and SUD as well as current animal models of drug dependence suggest that normalizing dopamine activity in the brain’s reward system is a productive approach to treatment.87 Compounds that selectively act on DA receptors affect long lasting cellular and intracellular adaptations, like desensitization and super sensitivity, causing therapeutic agents to fail to normalize dopamine at the level of neural circuitry.88 The challenge is to use “gentle” DA agonist therapy to activate D2 receptors in the mesolimbic pathway. The nutraceutical KB220Z was developed to accomplish this task in the brain reward cascade.89 The idea that KB220, and its enhanced variant KB220Z, possibly regulate DA is best described in an annotated bibliography that lists the studies showing the clinical effects of KB220Z.90 Please note that several project names/codes have been used over the years for the KB220Z formula such as SG8839, LG839, SAAVE, Synaptamine, PCAL-I03, and KB220.

The following information provides evidence of the clinical benefit of KB220Z, without addressing the issue of the neural mechanisms involved in achieving dopamine homeostasis. KB220 variants are formulations of a nutraceutical complex that have been studied extensively in both animals and humans. A detailed review article,90 as well as other articles,17,91–104 provide information on pre-clinical and human trials. The supplement () provides references for research directed with KB220Z variants. In summary, Gondré-Lewis’ group showed that KB220Z, when administered to genetically alcohol-preferring (P) rats, significantly attenuated ethanol consumption and operant-responding for 10% ethanol. Behavioral traits that mimic human neuropsychiatric conditions, including risk-taking behavior and hyperactivity were also attenuated in P rats. Although effective when delivered subcutaneously, intraperitoneally, and orally, this work showed that KB220 can act faster depending on route of administration105 The supplement () provides data supporting the role of KB220Z in reducing symptoms of drug and alcohol withdrawal in humans. Patients in recovery experienced reduced stress, measured by skin conductance level (SCL), and they demonstrated improved behavioral, emotional, social and spiritual well-being (BESS scores). Following detoxification, patients using KB220Z, compared to placebo, showed a six-fold reduction in leaving treatment against medical advice. After one month of treatment with KB220Z, healthy participants showed increased concentration. They also showed a decreased craving for nicotine, cocaine, heroin and alcohol (for an update of these studies see reference.90)

A few clinical benefits of KB220Z merit highlighting. Reduction in inappropriate sexual behavior has also been demonstrated.96 In addition, use of KB220Z has reduced the frequency of lucid nightmares, a symptom of Post-traumatic Stress Disorder (PTSD) in patients with PTSD.97 Human studies with quantitative electroencephalography (qEEG) revealed that KB220Z moderated theta frequencies in the anterior cingulate cortex.98 An fMRI pilot study of 5 substance dependent individuals, abstinent from heroin, showed that a single dose of KB220Z, compared to placebo, produced improvement in a prefrontal-cerebellar-occipital neural network, and increased activation of the NAc.99 Also, known obese patients, who were carriers of the D2 receptor A1 allele, had a significant correlation with KB220Z treatment compliance, compared to participants with the normal DA D2 receptors.100 An attenuation of craving and relapse prevention, has been shown in double-blind, controlled studies, as well as other research.101–104 Indeed, the compensatory overexpression of DRD2 receptors reduces alcohol and cocaine self-administration in in DRD2-deficient or drug preferring rodents.105–107

The current research literature supports the need for new approaches to treating RDS. Current therapeutic approaches have not addressed the reduced brain connectivity patterns often observed in individuals with SUD. Existing approaches have had only modest success in treating substance dependence and in preventing relapse.108 We hypothesized that high-resolution fMRI would show that KB220Z increases resting-state functional connectivity (rsFC, the correlation of activation between brain areas) and enhances connectivity between the cognitive and reward areas of the brain.109 In the Febo et al109 placebo-controlled study, the authors used fMRI and a new state of the art, annotated and segmented rat brain atlas to test the network-level actions of a novel complex mixture of KB220Z. As expected, KB220Z, a dopaminergic agonist, produced enhanced resting functional connectivity and volume recruitment (increase in the volume of brain areas affected by a treatment) between cognitive and reward centers of the rodent brain. These changes in the functional organization of the rodent brain, caused by KB220Z are relevant to the KB220Z-induced reduction of ethanol drinking, in rodents, observed by Solanki et al.105

mRNA Profiling

Many neural pathways and drugs interact to affect mRNA’s expression of enzymes that produce neurotransmitters, consequent neurotransmission, and the neuronal receptors responsible for feelings of well-being in animals and humans.110 Convergent input of the indirect striatopallidal and the direct striatonigral pathways, to the basal ganglia, and the dopaminergic modulation of these pathways, are very important in reward and aversion learning and substance dependence.111,112

To understand the role of the basal ganglia in processing information from these two pathways, Hikida et al113 developed a selective, reversible technique for blocking the activity of each pathway. Their results indicated that the effect of dopamine mediated psychostimulants required the coordinated modulation of the striatonigral and striatopallidal pathways. The direct striatonigral pathway was predominant in reward learning and cocaine sensitization, whereas the indirect, striatopallidal pathway was involved in aversive learning. These two pathways have different functional roles, the striatonigral pathway discriminating stimuli associated with reward and non-reward, and the striatopallidal pathway supporting memory for aversive stimuli.

“What is the role of drugs of abuse on mRNA in these pathways?” We have carefully explored this concept especially since it has an important function in helping to determine treatment outcomes pre- and post-treatment. This has culminated in the development of the a map yielding for the first time a comprehensive test involving multiple mRNA expressions utilizing array analysis to detect the type of expression (up or down) dependent upon the drug in question for a particular subject (Supplement, ).

Therefore, utilizing GARS, the mRNA outcome test for each patient follows the GARS test result as they enter the treatment facility or primary care program followed by a number of weekly retests to pinpoint any formidable changes in mRNA expression.

An early example of mRNA gene expression and SUD was the Noble et al114 discovery that the brains of alcoholic and non-alcoholic subjects differed in the binding affinity and number of binding sites of the dopamine D2 receptor in the caudate nucleus. The binding affinity of the D2 receptor and the number of D2 receptor binding sites were lower in alcoholics compared to non-alcoholics. Furthermore, subjects with the A1 allele who also had alcoholism showed significantly reduced dopamine D2 receptor sites. The number of these sites was progressively reduced as the involvement of the A1 allele increased from the A2/A2, to A2/A1 to A1/A1 genotypes. Subjects with the A2/A2 genotype had the highest number of dopamine D2 receptor sites whereas subjects with the A1/A1 genotype had the lowest number of D2 binding sites. In fact, the A1/A1 subjects demonstrated decreased protein expression in association with a 30–40% reduction in dopamine D2 receptors. The differential expression of dopamine D2 receptors as a function of the polymorphic pattern of the dopamine D2 receptor gene supports the involvement of the dopamine system in vulnerability to a subtype of severe alcoholism.

The Noble et al114 study is an example of the effect of the dopamine receptor gene alleles on Reward Deficiency Syndrome. There are ten genes and eleven alleles21 that influence RDS behaviors. Each allele changes the expression of RNA transcription with the effect of decreasing protein synthesis. In Noble et al,114 the A1/A1 allele showed reduced protein expression in association with reduced dopamine D2 receptors in the caudate nucleus.

Overcoming “Genomic Disparity” with Precision Medicine

Given the advent of precision medicine, the authors contend that the term “race”, as a definition of the biology of individuals and populations is obsolete and should be dropped from current usage. We suggest the use of genome-based terminology in the definition of individuals and/or populations, associated with their country/continent of origin (eg, African-Americans, Euro, Anglo or Caucasian-Americans, Mexican-Americans, etc.). Current human populations exhibit continuous genetic variations (polymorphisms) that defy clear division into race/racial groups or subgroups. The authors propose associating biological and/or clinical phenotypes with the genetic variation that underlies biological pathways, processes and/or mechanisms, rather than using “race” as a biological group or subgroup in human genome research. This is crucially important in this time of precision medicine when the power of research on genetic variation, to reveal the biological bases of clinical phenotypes, is reduced by outmoded descriptions of populations as “race(s)”. The latter point is especially relevant for African-Americans, a population that displays wide genetic variation reflective of its more recent population history in America.115

In this article, we have selected the term “ethnicity” instead of race. However, we are cognizant that “race” is so entrenched in the American mindset as a surrogate for biology, that it has been almost impossible to “change the mindset” of the American people who are deeply rooted in the appearance of “race” as a biological construct.

Prevalence of the DRD2 Taq A1 Allele as a Function of Ethnicity: An Example of Variation

Barr and Kidd35 have raised an important issue with early research on the frequency of the DRD2 Taq1 allele in various ethnic groups. Their concern is that variations in this allele in Caucasians have not effectively reflected stratification by ethnic groups, and, this has produced heterogeneity in samples of participants included in research studies. Barr and Kidd’s35 views are supported by studies of German, American Indian and Finish alcoholics. However, deeper analysis indicates that proper categorization of subjects in terms of severity of alcoholism was not completely addressed. The presence of the DRD2 A1 allele, in and of itself, may not necessarily produce alcoholism. One must also consider environmental factors, including the epigenetic effect of the social environment on gene expression. In this regard, Goldman et al116 failed to find a correlation between a high frequency of the A1 allele of the DRD2 gene in Cheyenne Indians, and alcoholism and drug abuse, using subjective interviewing. This result is understandable, given that Levy and Kunitz117 found a 60% rate of abstention among Native Americans who had taken an oath not to use drugs, compared to 25% in the general population. In contrast, Ishiguro et al118 reported that severe alcoholics, compared to less severe alcoholics had a significantly higher frequency of the DRD2 A1 allele. These researchers also found that all of the alcoholics with the A1/A1 genotype were in the severe alcoholism category.119

Barr and Kidd35 highlighted ethnic variation in the frequency of the DRD2 A1 allele with a gene map demonstrating that Yemeni Jews, known to have low rates of alcoholism, had an A1 allele frequency of 0.09. American Cheyenne Indians, in contrast, known in most research to have high rates of alcoholism, had an A1 allele frequency of 0.75. It is important to note that the DRD2 A1 allele frequency in African Pygmies is 0.25, compared to 0.5–0.75 in Colombian, Mayan, and other ethnicities in the Americas. The allelic frequency of the DRD2 A1 allele in African Americans likely varies due to admixture effects, and an interracial impact on the frequency of the DRD2 A1 allele. Albeit social and economic disparities can influence the epigenetic landscape and interact with gene variations to influence RDS behaviors, it has not been shown that African-Americans experience a higher risk for RDS behaviors compared to Euro-Americans.7,120,121 The authors are mindful of the fact that human behavior reflects a complex interaction between genetic, epigenetic mechanisms and the powerful influences of the social environment.

The DRD2 Taq A1 or B1 are good examples of how frequency across ethnicity must be addressed in future association studies. Specifically, O’Hara et al121 clearly provided pervasive evidence from 616 substance abusing and control participants underscoring the differences between A1 restriction fragment length polymorphism (RFLP) frequencies for black and white Americans. The data revealed the nearly exclusive occurrence of the A3 RFLP in African-Americans as well as a low frequency of rare A4 and B3 RFLP’s. For African-Americans, neither the A1 nor the B1 RFLP’s demonstrated a correlation with substance abuse, whereas Caucasian-Americans had significant correlations with abuse of multiple substances. As a proportion of the maximum potential disequilibrium, Caucasian-Americans and African-Americans display a strong disequilibrium of linkage between these loci. However, African-American individuals display many more A1/B2 chromosomes. The authors warn that ethnic/racial variations in Taq1 RFLP haplotypes emphasize the importance of caution in understanding allelic correlations when careful matching for ethnicity has not been accomplished. Abijo et al7 point to novel and/or unique gene variations in African-Americans and to the disparities in research specifically to understand the biology of SUD in this group. Cognizant that genetic risk polymorphisms can influence drug susceptibility and metabolism differently, they also proposed that ethnicity-informed genetics is necessary to provide real precision-guided therapeutics.

Finally, generally speaking, dopamine D2 receptor gene alleles are notable for their polymorphic A and B Taq1 locations, about 10 kb 3ʹ to the final exon and bordering the second exon, respectively. Some studies, but not all, have found that these alleles are more common in heavy substance users, compared to controls. A significant association has been revealed by meta-analyses of combined data from available studies.121–123

Precision Medicine

Based on evidence from, Ettienne et al123,124 utilization of pharmacogenetic testing has paved the way for “precision” dosing of buprenorphine to a highly substance dependent African-American population in Washington DC. Buprenorphine, a partial μ agonist, is considered by many as a safe and effective Opiate Substitution Therapy (OST) for opioid dependence. However, limitations on dosing differ greatly among the states and among insurance plans, including state Medicaid programs and federal Medicare part D pharmaceutical benefits plans. These limitations are often attributed to “federal guidelines” when they are often covert costs and/or supposed diversion reduction schemes.125 For example, the statewide Massachusetts-forced decrease of buprenorphine to 16 mg produced limited savings, an uncertain reduction in diversion and increased relapse in patients who were previously stable. This dosing discrepancy was reviewed by Accurso and Rastegar126 who found that; (1) the optimal dose of buprenorphine, administered in office settings is not known; (2) The imposition of a decrease in buprenorphine doses was correlated with increases in abnormal drug tests; and (3) Control group patients with higher buprenorphine doses showed greater treatment retention. Finally, the data suggested that some patients benefitted from doses above 16 mgs and doses below 16 mgs were harmful. In preliminary studies, the National Human Genome Center (NHGC) at Howard University and Howard University College of Pharmacy applied pharmacogenetic testing of buprenorphine (+Naloxone) metabolism in a study population consisting of 98% African-Americans, specifically using CYP3A4, the major metabolizing enzyme for Buprenorphine. Genotyping 144 patients revealed a wide polymorphic variation. Eighty-five percent of the population had the extended metabolic 1*B allele. They found that 43% had the *1/*1B; and 42% carried the *1B/*1B homozygote.123,124

Compared to over approximately 9000 samples, the same laboratory employed by Ettienne-Chapman’s group found a mixed population to carry 17% *1/*1B and 9% *1B/*1B or only 26% carried the extended *1B metabolizer. This acknowledges that for Caucasians the promoter variant CYP3A4*1B (−392A>G), has an allelic frequency of 2.9%, but for African-Americans, the allelic frequency of the promoter variant is 35–67%.121 Therefore, the take home message, based on genetics alone, is that these patients are unlikely to experience adverse effects from increased buprenorphine dosing (ie, greater than 16 mg per day), because they metabolize buprenorphine rapidly. In their clinic, they have seen intermediate metabolizers of Buprenorphine tolerate up to 24 mg daily. While they are cognizant that prescribed multiple pharmaceuticals are taken besides buprenorphine in their patient population, and possible drug–gene interactions and epigenetic impacts can occur on chromosomes, Chapman’s group have proposed routine pharmacogenetic profiling. This will at least determine more personalized or precision pharmacologically based buprenorphine dosing that will reduce relapse by increasing drug efficacy, thereby reducing diversion and poly-pharmacy adverse effects. Finally, the Ettienne et al123 data suggest that higher doses of buprenorphine will be needed in some subpopulations to decrease treatment failures; and (1) are unlikely due to widespread patient diversion of medication; (2) should not be limited by the cost of medication; and (3) should be guided by the patients’ genetic/epigenetic variations and needs regarding metabolism of drugs.

However, there is the opportunity to also evoke pharmacogenomic induced precision medicine as well.126,127 DNA Customization of nutraceutical products, which “nourish” the potential for optimized gene expression, can be achieved. The pro-dopamine regulator, KB220Z is an example. Continuing discoveries have been an important catalyst for the evolution, expansion, and scientific recognition of the significance of nutrigenomics and its contributions to human health. Truly, “Gene Guided Precision Nutrition” variations of KB220Z, which are mixtures of amino acids, herbals and trace metals, are pioneering innovations and standard-bearers for dose adjusted DNA customization. Research results from Blum et al,10 regarding genetic shaping of cravings and pleasure-seeking was the first step in our understanding of how genetics influences our actions and our physical and mental health. In addition, the technology represented by KB220Z and its variants that seeks to modify gene expression to control or eliminate cravings, is a cornerstone of the practical application of nutrigenomics. Ongoing research findings have catalyzed the evolution and scientific recognition of nutrigenomics and its important contribution to human health.

The Genetic Addiction Risk Severity (GARS) test, which has the capability of predicting the severity of alcohol and drug use, as well as non-substance dependent behavior, is part of an important, new field of scientific investigation. Neuro-nutrigenomics has the potential for improving human well-being. Notwithstanding the need for more research, neuro-neutrogenomics may provide clinical benefit for addiction medicine. There are, however, 3 studies published on customization of KB220Z a neuro-neutrigenomic compound, to combat obesity based on targeting DNA polymorphisms. Through 15 variant formulas, Blum’s team100,128,129 used polymorphic targets of reward genes (Dopaminergic, Opioidergic, Serotonergic and GABAergic) to customize KB220Z a neuro-neutrigenomic compound [Neuroadaptogen amino-acid therapy (NAAT)] with specific algorithms. A small sample of obese subjects in the Netherlands, selected from a larger group of 1000, was given KB220Z formulas which were tailored to their personal profile of DNA polymorphisms. The group demonstrated a substantial drop in Body Mass Index (BMI) and weight (lb.).100

We are proposing a generalized approach called “Precision Behavioral Management”. This approach consists of 1) Early pre-disposition assessment and determination (even in children) with the GARS, a 10 candidate polymorphic gene panel shown to predict ASI-alcohol and drug severity; 2) validated RDS questionnaire; 3) Utilization of the Comprehensive Analysis of Reported Drugs (CARD™) during actual treatment to determine compliance with prescribed medications and abstinence from non-prescribed and illicit drugs of abuse, and importantly; 4) Utilization of a “Pro-dopamine regulator (KB220)” (via IV and oral [KB220Z] delivery systems) to prevent relapse by induction of dopamine homeostasis, and; 5) Utilization of targeted DNA polymorphic reward genes to direct mRNA genetic expression profiling during the treatment process.

Incorporation of these events can be applied not only to, for example, the African–American community, but for all victims of RDS as a demonstration of a paradigm shift that uniquely provides a novel putative “standard of care” based on DNA guided precision nutrigenomic therapy to induce “dopamine homeostasis.” (see Figure 1). Indeed, some of the work implementing the Behavioral Management System in African-Americans has already begun via a grant awarded to Gondré-Lewis and Blum by the National Institutes of Health.

Figure 1

Reward Deficiency Syndrome SolutionTM for identification of risk alleles with the Genetic Addiction Risk Severity (GARS). The figure describes the Reward Deficiency Syndrome Solution SystemTM that proposes using the Genetic Addiction Risk Severity (GARS) to identify and stratify risk alleles for targeting by individualized nutrigenomic preparations. Our approach called “Precision Behavioral Management” consists of; 1) Early pre-disposition assessment and determination (even in children) with the Genetic Addiction Risk Severity (GARS), a 10 candidate polymorphic gene panel shown to predict ASI-alcohol and drug severity; 2) validated RDS questionnaire; 3) Utilization of the Comprehensive Analysis of Reported Drugs (CARD™) during actual treatment to determine compliance with prescribed medications and abstinence from non-prescribed and illicit drugs of abuse, and importantly; 4) Utilization of a “Pro-Dopamine Regulator (KB220)” (via IV and oral [KB220Z] delivery systems) to prevent relapse by induction of dopamine homeostasis, and; 5) Utilization of targeted DNA polymorphic reward genes to direct mRNA genetic expression profiling during the treatment process.

Conclusion

Blum et al99 reported in research with abstinent heroin dependent individuals that a variant of KB220Z increased resting state functional connectivity and enhanced activation in a network including the medial frontal gyrus, dorsal anterior cingulate and posterior cingulate gyri, nucleus accumbens, occipital cortices and the cerebellum. Febo et al, using rodents, demonstrated that KB220Z, compared to placebo, activated regions of interest including the left nucleus accumbens, anterior thalamic nuclei, cingulate gyrus, hippocampus, prelimbic and infra-limbic locations.109 This effect of KB220Z reveals increased functional connectivity, restoration of healthy aerobic metabolism evidenced by increased blood oxygen level dependent signaling/functioning (BOLD), increased brain volume recruitment and increased function of dopamine in the brain’s reward system, even as a clear reduction in motivation for drug-seeking activity was evident, in ethanol preferring rodents.105 This strong, specific reaction is clearly clinically relevant.

After considerable research the authors offer a Reward Deficiency Syndrome Solution System TM that proposes the use of GARS for early identification and stratification of risk alleles to develop individualized neuronutrient amino-acid therapy, created to match the individual’s profile of DNA SNP’s. With additional research, this unique approach could produce the first nutrigenomic solution for addiction, pain and RDS behaviors and introduce an era of genomic addiction medicine.

Finally, we are cognizant of the work of others130 who found that compared to Native Americans, African-Americans and Asians have a lower prevalence of alcohol abuse and dependence. Furthermore, relative to European-Americans, African-Americans have lower consumption across all ages, a later onset of drinking, but greater health problems associated with alcohol. This is where the social determinants of health become important. Even though African Americans consume less alcohol, they face greater health risks, possibly due to co-occurring medical conditions. When the reward circuitry is inadequately funded with nutritional resources to optimize gene expression, as is prevalent in today’s modern agribusiness, food processing and fast food systems environment, those individuals can participate in potentially unhealthy and even dangerous excessive reward-seeking or self-medicating behaviors, such as substance abuse, to achieve reward satisfaction.

In terms of genetic studies, we must be careful to include various ethnic groups when trying to determine candidate genes as well as utilizing Genome Wide Association Studies as antecedents to RDS behaviors. Two possible hypotheses may account for the correlation of any allele (DRD2 A1,B1) with RDS behavior: (1) linkage disequilibrium of A1 and B1 RFLP’s with an allelic determinant that affects behavior; (2) the individuals affected disproportionately come from populations stratified by a factor such as ethnicity that is associated with greater A1 and B1 RFLP frequencies.

In this regard, we are proposing the paradigmatic shift called “Reward Deficiency Syndrome Solution System” and its requirement to encourage more research in this fundamental area of investigation.131,132

By definition, all inventions are outside the realm of conventional thinking. Inventions generally go through 3 stages towards acceptance: 1. Outright criticism and rejection (as it threatens to change the way things are or are done); 2.Virulent cynicism and opposition; 3. Gradual and popular acceptance as self-evident. The invention of the KB220Z and the GARS technology many decades after the discovery of the genetic link to severe alcoholism, represents another bold disruptive technological breakthrough by the same scientist that made the previous discovery and one of our coauthors (KB). These technologies represent unprecedented advancements in the nutrigenomics of neuroscience; achieving dopamine homeostasis and a promising ability to restore a life characterized by greater self-control, greater stress tolerance, improved mental sharpness and cognition, better decision-making capabilities, and overall mood improvement and a greater sense of happiness. We have gone through the first two stages and are in the 3rd and final stage of acceptance. We encourage clinicians to step outside the “box of conventional dogma”; critically review the more than 40 clinical studies on this technology; and begin adopting its use for clinical applications by physicians and treatment centers alike, especially for those ethnicities that evidence suggest have a higher risk of indulging in life threatening RDS behavioral octopus.7,41,131–134

Finally, it is of interest that most recently, Levey et al135 reported on a transcriptome-wide association study analyses and revealed significant associations with expression of NEGR1 in the hypothalamus and DRD2 in the nucleus accumbens, among others linked to approximately 1.2 million veterans and 59,000 African-Americans, with major depression. This is particularly important because the original work by Blum, Noble & Sheridan in 199010 also suggested that the DRD2 A1 allele was not specific for alcoholism but was linked to a non-specific reward phenotype like depression.