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1. Precision Behavioral Management (PBM) and Cognitive Control as a Potential Therapeutic and Prophylactic Modality for Reward Deficiency Syndrome (RDS): Is There Enough Evidence?

Author

Margaret A. Madigan, Ashim Gupta, Abdalla Bowirrat, David Baron, Rajendra D. Badgaiyan, Igor Elman, Catherine A. Dennen, Eric R. Braverman, Mark S. Gold, and Kenneth Blum

Subjects
Behavior, Addictive, Cognition, Reward, Health, Toxicology and Mutagenesis, Streptothricins, Public Health, Environmental and Occupational Health, Humans, Syndrome
Abstract

This brief commentary aims to provide an overview of the available and relatively new precision management of reward deficiencies manifested as substance and behavioral disorders. Current and future advances, concepts, and the substantial evidential basis of this potential therapeutic and prophylactic treatment modality are presented. Precision Behavioral Management (PBM), conceptualized initially as Precision Addiction Management (PAM), certainly deserves consideration as an important modality for the treatment of impaired cognitive control in reward processing as manifested in people with neurobiologically expressed Reward Deficiency Syndrome (RDS).

Published
2022

2. Rapid Anti-Depressant Relief by Ketamine: Exploring A Complex Mechanism of Action

Author

Scott Worrich, Kenneth Blum, Mark Moran, Bryan Clifton, Todd C. Pappas, David Baron, Abdalla Bowirrat, Lisa Lott, Cannon Clifton, Ervey Clarke, Brent Boyett, Mark S. Gold, and Margaret A. Madigan

Subjects
0301 basic medicine, Pharmacology, business.industry, 03 medical and health sciences, Psychiatry and Mental health, 030104 developmental biology, 0302 clinical medicine, Mechanism of action, medicine, Pharmacology (medical), Anti depressant, Ketamine, medicine.symptom, business, 030217 neurology & neurosurgery, medicine.drug
Abstract

Background: Suicide rates and narcotic overdose have doubled since 2000. At least 30 percent of people with major depression are Treatment-Resistant (TR) and require novel therapeutics. ketamine at low doses has been shown in clinical trials to induce a rapid, short-lived anti-suicide and anti-depressant effect. Objective: To review the potential mechanism of action of ketamines’ alleviation of depressive symptoms from both animal and available human literature. Methods: This is a synthesis of information from papers listed in PUBMED Central. Although not exhaustive, this review highlights the most compelling work in the field related to this remarkable clinical rapid anti-depressant effect. Results: While there have been several theories and with some scientific evidence to date, the conclusion here is that currently, an exact and acceptable mechanism of action (MOA) for ketamines’ rapid anti-depressant effect is not apparent. The MOA of this compound with psychoactive abuse potential at a higher dosage and acute antidepressive effect in the most resistant patients is unknown. Discussion: Possible MOAs reviewed, include dopamine receptor modulation through epigenetic neuroadaptation via specific D1/D2 antagonism, D1 activation using optogenetic stimulation, and the role of D2/D3 availability in the ketamine therapeutic action. Conclusion: Unraveling MOA could guide the development of other unique Psychoplastogens capable of rapidly promoting structural and functional neural plasticity in cases of TR Major Depressive Episodes (MDE) and unipolar Major Depression Disorder (MDD).

Published
2019

3. Pilot clinical observations between food and drug seeking derived from fifty cases attending an eating disorder clinic

Author

Kenneth Blum, Mona Li, Margaret A. Madigan, Mark S. Gold, Eric R. Braverman, Marcelo Febo, John Giordano, Rajendra D Badgaiyan, Harriet Beitscher-Campbell, and Kristina Dushaj

Subjects
Adult, Male, 0301 basic medicine, medicine.medical_specialty, Substance-Related Disorders, media_common.quotation_subject, Drug-Seeking Behavior, Medicine (miscellaneous), Pilot Projects, Case Report, Dopamine agonist, Cohort Studies, Feeding and Eating Disorders, Young Adult, 03 medical and health sciences, 0302 clinical medicine, food and drug addictions, Interview, Psychological, mental disorders, medicine, Humans, Psychiatry, media_common, Addiction, Dopaminergic, Feeding Behavior, General Medicine, Middle Aged, medicine.disease, Comorbidity, 3. Good health, Substance abuse, Psychiatry and Mental health, Clinical Psychology, Eating disorders, 030104 developmental biology, Reward dependence, Anorexia nervosa (differential diagnoses), eating disorder, Dopamine Agonists, dopamine pathways, reward deficiency syndrome, Female, commonality, Psychology, 030217 neurology & neurosurgery, medicine.drug, Clinical psychology
Abstract

Background The reward deficiency syndrome hypothesis posits that genes are responsible for reward dependence and related behaviors. There is evidence that both bulimia and anorexia nervosa, especially in women, have been linked to a lifetime history of substance use disorder (SUD). There are difficulties in accepting food as an addiction similar to drugs; however, increasingly neuroimaging studies favor such an assertion. Case presentations We are reporting the evidence of comorbidity of eating disorders with SUD found within these case presentations. We show 50 case reports derived from two independent treatment centers in Florida that suggest the commonality between food and drug addictions. In an attempt to provide data from this cohort, many participants did not adequately respond to our questionnaire. Discussion We propose that dopamine agonist therapy may be of common benefit. Failure in the past may reside in too powerful D2 agonist activity leading to D2 receptor downregulation, while the new methodology may cause a reduction of “dopamine resistance” by inducing “dopamine homeostasis.” While this is not a definitive study, it does provide some additional clinical evidence that these two addictions are not mutually exclusive. Conclusion Certainly, it is our position that there is an overlap between food- and drug-seeking behavior. We propose that the studies focused on an effort to produce natural activation of dopaminergic reward circuitry as a type of common therapy may certainly be reasonable. Additional research is warranted.

Published
2016

5. NIDA-Drug Addiction Treatment Outcome Study (DATOS) Relapse as a Function of Spirituality/Religiosity

Author

Rajendra D Badgaiyan, Mark S. Gold, Stephen J. Schoenthaler, Kristina Dushaj, Marlene Oscar-Berman, Roger L. Waite, Mona Li, Eric R. Braverman, Kenneth Blum, Zsolt Demotrovics, John Giordano, Margaret A. Madigan, and Ben Thompson

Subjects
Reward Deficiency Syndrome (RDS), Spiritual practice, Logistic regression, Genospirituality, Article, Religiosity, 03 medical and health sciences, 0302 clinical medicine, Anomie, medicine, Social Bonds, Spirituality, 030212 general & internal medicine, Relapse, Social control theory, medicine.disease, Social relation, 3. Good health, Substance abuse, Religion, Neurogentics, Psychology, 030217 neurology & neurosurgery, Deviance (sociology), Clinical psychology
Abstract

BACKGROUND The connection between religion/spirituality and deviance, like substance abuse, was first made by Durkheim who defined socially expected behaviors as norms. He explained that deviance is due in large part to their absence (called anomie), and concluded that spirituality lowers deviance by preserving norms and social bonds. Impairments in brain reward circuitry, as observed in Reward Deficiency Syndrome (RDS), may also result in deviance and as such we wondered if stronger belief in spirituality practice and religious belief could lower relapse from drugs of abuse. METHODS The NIDA Drug Addiction Treatment Outcome Study data set was used to examine post hoc relapse rates among 2,947 clients who were interviewed at 12 months after intake broken down by five spirituality measures. RESULTS Our main findings strongly indicate, that those with low spirituality have higher relapse rates and those with high spirituality have higher remission rates with crack use being the sole exception. We found significant differences in terms of cocaine, heroin, alcohol, and marijuana relapse as a function of strength of religious beliefs (x2 = 15.18, p = 0.028; logistic regression = 10.65, p = 0.006); frequency of attending religious services (x2 = 40.78, p < 0.0005; logistic regression = 30.45, p < 0.0005); frequency of reading religious books (x2 = 27.190, p < 0.0005; logistic regression = 17.31, p < 0.0005); frequency of watching religious programs (x2 = 19.02, p = 0.002; logistic regression = ns); and frequency of meditation/prayer (x2 = 11.33, p = 0.045; logistic regression = 9.650, p = 0.002). Across the five measures of spirituality, the spiritual participants reported between 7% and 21% less alcohol, cocaine, heroin, and marijuana use than the non-spiritual subjects. However, the crack users who reported that religion was not important reported significantly less crack use than the spiritual participants. The strongest association between remission and spirituality involves attending religious services weekly, the one marker of the five that involves the highest social interaction/social bonding consistent with Durkheim's social bond theory. CONCLUSIONS Stronger spiritual/religious beliefs and practices are directly associated with remission from abused drugs except crack. Much like the value of having a sponsor, for clients who abuse drugs, regular spiritual practice, particularly weekly attendance at the religious services of their choice is associated with significantly higher remission. These results demonstrate the clinically significant role of spirituality and the social bonds it creates in drug treatment programs.

Published
2015

6. Critical Analysis of White House Anti-Drug Plan

Author

Kenneth Blum, Bruce Steinberg, John Giordano, Thomas J. McLaughlin, Rajendra D Badgaiyan, Mary Hauser, Lyle Fried, Margaret A. Madigan, David Baron, Michael DeLeon, and Edward J Modestino

Subjects
Drug, medicine.medical_specialty, Opioid epidemic, Prescription drug, White (horse), business.industry, media_common.quotation_subject, MEDLINE, Article, 3. Good health, Family medicine, Revenue, Medicine, Medical prescription, Opiate, business, media_common
Abstract

There is no question that America is experiencing a horrific opiate/opioid epidemic whereby thousands of people are unfortunately dying, and the rate of people seeking treatment is at all -time high. One major problem can be linked to the fact that legal prescriptions for powerful opioid analgesics reached 297 million in 2016. One company that manufactures Oxycontin generated $3.1 billion in revenue in 2017. Moreover, that deaths from prescription drug overdoses have been called the “silent epidemic†for many years.

Published
2017

8. KB220Z™ a Pro-Dopamine Regulator Associated with the Protracted, Alleviation of Terrifying Lucid Dreams. Can We Infer Neuroplasticity-induced Changes in the Reward Circuit?

Author

Debmalya Barh, Marcelo Febo, Eric R. Braverman, Kristina Dushaj, Rajendra D Badgaiyan, Thomas J. McLaughlin, Mona Li, Kenneth Blum, and Margaret A. Madigan

Subjects
medicine.medical_specialty, Lucid dreams, Dopamine, Rapid eye movement sleep, Alcohol abuse, Lucid dream, Article, 03 medical and health sciences, 0302 clinical medicine, Neuroplasticity, Medicine, Attention deficit hyperactivity disorder, Psychiatry, Recall, medicine.diagnostic_test, business.industry, KB220z, 16. Peace & justice, medicine.disease, 030227 psychiatry, Brain stimulation reward, Connectivity volume, business, Functional magnetic resonance imaging, 030217 neurology & neurosurgery, psychological phenomena and processes
Abstract

Background Recent reports by our laboratory have indicated that lucid dreams may be linked to psychiatric conditions, including Attention Deficit Hyperactivity Disorder (ADHD) and other Reward Deficiency Syndrome-related diagnoses. In the latter case, it has been our observation that such lucid dreams can be unpleasant and frequently terrifying. Case presentations We present four cases of a dramatic and persistent alleviation of terrifying, lucid dreams in patients diagnosed with ADHD/PTSD and/or opiate/opioid addiction. The amelioration of such dreams could well be permanent, since the patients had stopped taking the nutraceutical for between 10 to 12 months, without their recollection or recurrence. In the first case, the patient is a 47-year-old, married male who required continued Buprenorphine/ Naloxone (Suboxone) treatment. The second case involved a 32-year-old female with the sole diagnosis of ADHD. The third case involves a 38-year-old male who carried the diagnoses of Substance Use Dependence and ADHD. The fourth case involved a 50-year-old female with the diagnoses of Alcohol Abuse, ADHD and Posttraumatic Stress Disorder. Results In order to attempt to understand the possibility of neuroplasticity, we evaluated the effect of KB220Z in non-opioid-addicted rats utilizing functional Magnetic Resonance Imaging methodology. While we cannot make a definitive claim because rat brain functional connectivity may not be exactly the same as humans, it does provide some interesting clues. We did find following seeding of the dorsal hippocampus, enhanced connectivity volume across several Regions of Interest (ROI), with the exception of the pre- frontal cortex. Interestingly, the latter region is only infrequently activated in lucid human dreaming, when the dreamer reports that he/she had the thought that they were dreaming during the lucid dream. Conclusions The four patients initially reported a gradual but, then, complete amelioration of their long-term, terrifying, lucid dreams, while taking KB220Z. The persistent amelioration of these dreams continued for up to 12 months, after a self-initiated, cessation of use of KB220Z. These particular cases raise the scientific possibility that KB200Z increases both dopamine stability as well as functional connectivity between networks of brain reward circuitry in both rodents and humans. The increase in connectivity volume in rodents suggest the induction of neuroplasticity changes, which may be analogous to those involved in human lucid dreaming as well as Rapid Eye Movement sleep. The possibility that the complex induces long-term, neuroplasticity changes must await more intensive investigations, involving large-population, double-blinded studies.

Published
2017

9. Drug Abuse Relapse Rates Linked to Level of Education: Can We Repair Hypodopaminergic-Induced Cognitive Decline With Nutrient Therapy?

Author

Margaret A. Madigan, Eric R. Braverman, John Giordano, Marlene Oscar-Berman, David K. Han, Kenneth Blum, and Stephen J. Schoenthaler

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, Substance-Related Disorders, Dopamine, media_common.quotation_subject, Decision Making, Poison control, Pilot Projects, Physical Therapy, Sports Therapy and Rehabilitation, Academic achievement, Affect (psychology), Reward, Recurrence, Risk Factors, Surveys and Questionnaires, Internal medicine, Injury prevention, medicine, Humans, Orthopedics and Sports Medicine, Cognitive decline, Psychiatry, media_common, business.industry, Addiction, Brain, Human factors and ergonomics, Middle Aged, medicine.disease, Behavior, Addictive, Substance abuse, Treatment Outcome, Athletes, Athletic Injuries, Dietary Supplements, Florida, Educational Status, Female, business
Abstract

It is well known that athletes and other individuals who have suffered painful injuries are at increased risk for all reward deficiency syndrome (RDS) behaviors, including substance use disorder (SUD). Comparing patient demographics and relapse rates in chemical dependence programs is pertinent because demographics may affect outcomes. Increased risk for relapse and lower academic achievement were found to have a significant association in recent outcome data from a holistic treatment center (HTC) located in North Miami Beach, FL. Relapse outcomes from the Drug Addiction Treatment Outcome Study (DATOS; n = 1738) and HTC (n = 224) were compared for a 12-month period. Post-discharge relapse was reported by 26% of HTC patients and 58% of patients in DATOS. When broken out by education level-less than high school, high school diploma, college degree, and graduate degree-HTC patient relapse was 50%, 36%, 33%, and 16%, respectively, and demonstrated an inverse linear association (F = 5.702; P = 0.017). Looking at DATOS patient relapse rates broken down by educational grades/years completed, patients who attended school between 7th grade and 4 years of college also demonstrated an inverse linear association (F = 5.563; P = 0.018). Additionally, the lowest performers, patients who reported their academic performance as "not so good," had the highest relapse (F = 4.226; P = 0.04). Albeit certain limitations, compared with DATOS patients, HTC patients produced significantly larger net differences in relapse rates (X 2 = 84.09; P = 0.0001), suggesting that other variables, such as the treatment model may also affect patient relapse. Our results implicate the use of vitamin and mineral supplements coupled with a well-researched natural dopamine agonist nutrient therapy; both have been shown to improve cognition and behavior, and thus academic achievement. That relapse is highest among addicts who have less education and who report lower grades is a factor that can be useful when considering treatment type and controlled for when comparing treatment outcomes.

Published
2014

10. Hypothesizing 'Reward' Gene Polymorphisms May Predict High Rates of Injury and Addiction in the Workforce: A Nutrient and Electrotherapeutic Based Solution

Author

Seth H. Blum, Kenneth Blum, Kristina Dushaj, Thomas Simpaatico, Eric R. Braverman, Roger L. Waite, Marlene Oscar-Bermanm, and Margaret A. Madigan

Subjects
medicine.medical_specialty, business.industry, Addiction, media_common.quotation_subject, Chronic pain, Craving, medicine.disease, Work related, Substance abuse, Pain assessment, mental disorders, medicine, Genetic predisposition, Brain stimulation reward, medicine.symptom, Psychiatry, business, media_common
Abstract

We hypothesize that individuals with genetic predisposition to Substance Use Disorder (SUD) may have greater likelihood of experiencing work related accidents. We further hypothesize that high risk populations will carry single or multiple polymorphisms associated with brain reward circuitry and/or brain reward cascade, including: Dopaminergic (i.e. DRD2 receptor genes); Serotonergic (i.e. 5-HTT2 receptor genes); Endorphinergic (i.e. pre-enkephalin genes); Gabergic (i.e. GABAA receptor genes); Neurotransmitter Metabolizing genes (i.e. MAO and COMT genes) among others (GARSRXTM). Analgesic addiction as well as “pseudoaddiction” must be treated to improve pain control and its management. We propose that non-pharmacological alternatives to pain relief, in high risk, addiction-prone individuals, are Electrotherapeutic Device(s) and Programs. We further propose patented KB220Z, a nutraceutical designed to release dopamine at the nucleus accumbens, will reduce craving behavior, in genetically programmed individuals. By utilizing both alternatives in DNA analyzed injured workers, a reduction in analgesic addiction (genuine or pseudo) leads to improved health and quicker return to work. We also hypothesize that this novel approach will impact costs related to injuries in the workforce. Effective management of chronic pain, especially in high addiction-prone workforce populations, is possible in spite of being particularly elusive. A series of factors encumber pain assessment and management, including analgesia addiction, pharmacogenomic response to pain medications, and genetically inherited factors involving gene polymorphisms. Additional research is required to test these stipulated hypotheses related to genetic proneness to addiction, but also proneness to accidents in the workplace and reduction of craving behavior. Our hypothesis that genotyping coupled with both KB220ZTM and the pharmaceutical-free Electrotherapy, will reduce iatrogenic induced analgesia addiction. This approach will achieve attainable effective pain management and quicker return to work. We propose outcomes such as the Reward Deficiency System SolutionTM may become an adjunct in the war against iatrogenic pain medication addiction.

Published
2014

11. Hypothesizing repetitive paraphilia behavior of a medication refractive Tourette's syndrome patient having rapid clinical attenuation with KB220Z-nutrigenomic amino-acid therapy (NAAT)

Author

Scot Jones, Raquel Lohmann, Thomas Simpatico, Roger L. Waite, Debmayla Barh, Kenneth Blum, Margaret A. Madigan, Thomas McLaughlin, Marlene Oscar-Berman, John Giordano, Eric R. Braverman, Kristina Dushaj, William B. Downs, and David K. Han

Subjects
Pediatrics, medicine.medical_specialty, Medicine (miscellaneous), Craving, General Medicine, Placebo, medicine.disease, Dopamine agonist, Psychiatry and Mental health, Clinical Psychology, medicine.anatomical_structure, Ropinirole, Dopaminergic pathways, Dopamine receptor, Neuroplasticity, medicine, Paraphilia, medicine.symptom, Psychology, Psychiatry, medicine.drug
Abstract

Background and aims Many patients presenting multiple behaviors including drug and food abuse as well as other pathological repetitive unwanted activities such as gambling, self-mutilation and paraphilias may not be appropriately diagnosed. Here we present a case of a male presenting many of these seemingly diverse behaviors and finally diagnosed with reward deficiency syndrome (RDS) by his attending physician. Methods The use of the dopamine agonist, ropinirole after two weeks showed improvement in terms of sexual behavior but tolerance set in and was discontinued especially when an infraction occurred with the patient's insurance. In this article, we carefully explore the potential of ropinirole to downregulate dopamine receptors causing adenylate cyclase receptor supersensitivity and tolerance a feature of neurotransmitter cross-talk. Based on previous scientific evidence showing KB220Znutrigenomic amino-acid therapy (NAAT) to rapidly (post one-hour) activate dopaminergic pathways in both the pre-frontal cortex cingulate gyrus (relapse loci) and ventral tegmental area-caudate-accumbens-putamen (craving and emotion loci) the patient was prescribed NAAT. Results and discussion Within one week of utilization the repetitive paraphilia was eliminated. There were also a number of other positive effects such as enhanced focus that persisted even after the patient stopped using KB220Z suggesting neuroplasticity (e.g. altruistic thoughts). However, these observed profound benefits require more in-depth study, especially in a large cohort against a placebo. While this report focused on a rapid response rather than long-term benefits previously associated with NAAT, it is somewhat encouraging and longer term required follow-up and larger placebo controlled studies are warranted before any definitive conclusions could be gleaned from this case report.

Published
2013

12. Iatrogenic opioid dependence is endemic and legal: Genetic addiction risk score (GARS) with electrotherapy a paradigm shift in pain treatment programs

Author

Joan Borsten, Nicholas A. DiNubile, John Giordano, Marlene Oscar-Berman, Thomas Simpatico, Bernard W. Downs, Kristina Dushaj, Debmayla Barh, David K. Han, Anish Bajaj, Gary Reinl, Thomas McLaughlin, Wayne L. Westcott, Margaret A. Madigan, Leonard Smith, Mary Hauser, Eric R. Braverman, and Kenneth Blum

Subjects
Framingham Risk Score, Human studies, Narcotic, business.industry, Addiction, media_common.quotation_subject, medicine.medical_treatment, Pain medication, Edema reduction, Opioid, Electrotherapy, Anesthesia, medicine, business, media_common, medicine.drug
Abstract

The mounting endemic of prescription iatrogenic opioid dependence in pain patients provoked this treatise about an alternative method that can be used to treat pain, improve function and reduce the risk of opioid dependence. It is well known that as well as the side effects reported for chronic opioid therapy, genetically predisposed individuals are at risk for opioid dependence. We propose the use of the Genetic Addiction Risk Score (GARS) assessment to identify patients early in treatment who should avoid narcotic pain medications. Primarily, this review will be an exploration of the mechanisms of action of an electrotherapeutic alternative to narcotic treatment that can be used to augment tissue healing and reduce the pain associated with human injuries and neuropathies. This particular electrotherapeutic device was developed at the Electronic Waveform Laboratory in Huntington Beach, California and is called the H-Wave? device. The primary effect of the H-Wave?device is stimulation (HWDS) of small diameter fibers of “red-slow-twitch” skeletal muscle. Mechanisms of action of HWDS have been investigated in both animal and human studies. They include edema reduction, induction of nitric oxide dependent augmented microcirculation and angiogenesis, small muscle contraction that eliminates transcapillary fluid shifts, reducing the painful effects of tetanizing fatigue and gradual loading of healing injured muscle tissue that helps repair and remodeling. A recent metaanalysis found a moderate-to-strong-positive effect of the HWDS in providing pain relief, reducing the requirement for pain medication, with the most robust effect being increased functionality. We are proposing that GARS can be used to identify those at risk of developing opioid dependence and that the need for opioid analgesia can be reduced by use of this electro therapeutic alternative to opioid analgesia in the treatment of pain and injuries.

Published
2013

17. OMICS

Author

Kenneth Blum, Debmalya Barh, and Margaret A. Madigan

Subjects
Cancer chemotherapy, Nutrigenomics, Systems biology, Pharmacogenomics, Genomics, Computational biology, Biology, Omics, Proteomics, Bioinformatics, Immunomics
Abstract

SECTION I: Methodology and Application Bioinformatics: A Brief Introduction to Changing Trends in Modern Biology, A.A. Singh and P. Somvanshi Nutrigenomics, M. Verghese and J. Boateng Omics Approaches in Toxicology Research and Biomedical Applications, N.L. Lopez-Corrales, A. Miyoshi, V. Azevedo, T. Stuztman, and D. Barh Stem Cells: Basics and Therapeutic Applications, A.K. Arya and K. Tripathi Emerging Trends of Nanotechnology in Omics-Based Drug Discovery and Development, S. Selvarajan Magnetic Nanoparticles in Biomedical Applications, R. Zhang and H. Olin High-Throughput Screening in Medical Diagnosis and Prognosis, M. El Sayed Zaki High-Throughput Omics: The Application of Automated High-Throughput Methods and Systems for Solutions in Systems Biology, U. Kolukisaoglu and K. Thurow Safety in Diagnostic Imaging Techniques Used in Omics, R. Visaria, S. Prakash, J.T. Vaughan, and D. Shrivastava SECTION II: Empirical Research Molecular Genetics of Human Cancers: Modulation of the Tumor Suppressor Function of RB1 Gene Product in Human Vestibular Schwannomas, M.L. Gope, R. Mitra, and R. Gope Forward Genetics Approach in Genomics: Functional Identifi cation of Unknown Genes, B. Chatterjee Proteomics of Phagosomal Pathogens: Lessons from Listeria monocytogens and New Tools in Immunology, E. Rodriguez-Del Rio, C. Carranza-Cereceda, L. Fernandez-Prieto, J. Ramos-Vivas, and C. Alvarez-Dominguez SECTION III: Computational and Systems Biology In a Quest to Uncover Governing Principles of Cellular Networks: A Systems Biology Perspective, K. Selvarajoo and M. Tsuchiya Intermolecular Interaction in Biological Systems, Y. Fukunishi Implanted Brain-Machine Interfaces in Rats: A Modern Application of Neuromics, W. Chen, J. Dai, S. Zhang, X. Zheng, and X. Hu SECTION IV: Therapeutics Pharmacogenomics in Development of Disease-Specifi c Therapeutic Strategy, S. Sharma and A. Munshi Omics Approaches in Cancer Biomarker and Targeted Anticancer Drug Discovery, D. Dhawan and H. Padh Recent Advances in MicroRNA Expression Profiling Toward a Molecular Anatomy of Tumorigenesis and Applications for Diagnosis, Prognosis, and Therapeutics, H. Ohdaira and K. Yoshida Marine Metabolomics in Cancer Chemotherapy, D.M. Pereira, G. Correia-da-Silva, P. Valentao, N. Teixeira, and P.B. Andrade Genome-Wide Association Studies of Type 2 Diabetes: Current Status, Open Challenges, and Future Perspectives, H. Hong, L. Xu, D.L. Mendrick, and W. Tong Cardiac Channelopathies: Applications of Genomics and Proteomics in Diagnosis and Therapy, C. Viero Toward an Omic Perspective on Infectious Disease and Its Therapy: Integrating Immunoinformatics, Immunomics, and Vaccinomics, M.N. Davies and D.R. Flower NeuroAIDS and Omics of HIV Vpr, A. Swarup Verma, U. Pratap Singh, P. Mallick, P. Dhar Dwivedi, and A. Singh Epigenetics in Neuropsychiatry, T. Archer and K. Blum Neurogenetics and Nutrigenomics of Reward Deficiency Syndrome, K. Blum SECTION V: Future Perspective Future Perspective: Paving a Path to Optimization of Health, D. Barh, M.A. Madigan, and K. Blum

Published
2016

18. Early Intervention of Intravenous KB220IV- Neuroadaptagen Amino-Acid Therapy (NAAT)™ Improves Behavioral Outcomes in a Residential Addiction Treatment Program: A Pilot Study

Author

Debra Manka, Roger L. Waite, Eric R Braverman, Uma Damle, John Giordano, Marlene Oscar-Berman, Kenneth Blum, John A. Bailey, Siobhan Morse, Stan D Stokes, Matthew Manka, Debmalya Barh, Amanda L C Chen, William B. Downs, Kenneth Perrine, David Miller, Merlene Miller, Susan Silverman, Mallory Kerner, Abdalla Bowirrat, Thomas J H Chen, and Margaret A. Madigan

Subjects
Adult, Male, Agonist, medicine.medical_specialty, Substance-Related Disorders, medicine.drug_class, Emotions, Administration, Oral, Medicine (miscellaneous), Pilot Projects, Neuropsychological Tests, Culprit, Article, Cognition, Reward, Paired samples, Recurrence, Internal medicine, Intervention (counseling), medicine, Humans, Amino Acids, General Psychology, Addiction treatment, Behavior, Dopaminergic, Middle Aged, Additional research, Substance Withdrawal Syndrome, Chronic Disease, Dopamine Agonists, Injections, Intravenous, Physical therapy, Female, Substance Abuse Treatment Centers, Psychology
Abstract

Substance use disorders (SUD) are inheritable and the culprit is hypodopaminergic function regulated by reward genes. We evaluated a natural dopaminergic agonist; KB220 intravenous (IV) and oral variants, to improve dopaminergic function in SUD. Our pilot experiment found a significant reduction of chronic symptoms, measured by the Chronic Abstinence Symptom Severity (CASS) Scale. The combined group (IV and oral) did significantly better than the oral-only group over the first week and 30-day follow-up period. Next, the combination was given to 129 subjects and three factors; Emotion, Somatic, and Impaired Cognition, with eigenvalues greater than one were extracted for baseline CASS-Revised (CASS-R) variables. Paired sample t-tests for pre and post-treatment scales showed significant declines (p = .00001) from pre- to post-treatment: t = 19.1 for Emotion, t = 16.1 for Somatic, and t = 14.9 for Impaired Cognition. In a two-year follow-up of 23 subjects who underwent KB220IV therapy (at least five IV treatments over seven days) plus orals for 30+ days: 21 (91%) were sober at six months, 19 (82%) having no relapse; 19 (82%) were sober at one year, 18 (78%) having no relapse; and 21 (91%) were sober two-years post-treatment, 16(70%) having no relapse. We await additional research and advise caution in interpreting these encouraging results.

Published
2012

19. Generational Association Studies of Dopaminergic Genes in Reward Deficiency Syndrome (RDS) Subjects: Selecting Appropriate Phenotypes for Reward Dependence Behaviors

Author

Caroline Davis, John Giordano, John Schoolfield, Joel F. Lubar, John Femino, Frank Fornari, Eric R. Braverman, Abdalla Bowirrat, Thomas J H Chen, John A. Bailey, Kenneth Blum, Marlene Oscar-Berman, David E. Comings, Bernard W. Downs, Nancy White, Tomás Palomo, Siobhan Morse, Mallory Kerner, Margaret A. Madigan, Debmalya Barh, Amanda L C Chen, Jennifer Knopf, Judith O. Lubar, and Roger L. Waite

Subjects
gene polymorphisms, Male, Candidate gene, Genotype, phenotype, Reward Deficiency Syndrome (RDS), Health, Toxicology and Mutagenesis, media_common.quotation_subject, lcsh:Medicine, Dopamine beta-Hydroxylase, Biology, dopamine, generational association studies, “super normal” controls, Article, 03 medical and health sciences, 0302 clinical medicine, Reward, Dopamine receptor D2, Humans, Alleles, 030304 developmental biology, media_common, Genetic association, Dopamine transporter, Genetics, 0303 health sciences, Dopamine Plasma Membrane Transport Proteins, Polymorphism, Genetic, Receptors, Dopamine D2, Addiction, Receptors, Dopamine D1, Dopaminergic, lcsh:R, Public Health, Environmental and Occupational Health, Pedigree, Behavior, Addictive, Reward dependence, biology.protein, Brain stimulation reward, Female, 030217 neurology & neurosurgery
Abstract

Abnormal behaviors involving dopaminergic gene polymorphisms often reflect an insufficiency of usual feelings of satisfaction, or Reward Deficiency Syndrome (RDS). RDS results from a dysfunction in the “brain reward cascade,” a complex interaction among neurotransmitters (primarily dopaminergic and opioidergic). Individuals with a family history of alcoholism or other addictions may be born with a deficiency in the ability to produce or use these neurotransmitters. Exposure to prolonged periods of stress and alcohol or other substances also can lead to a corruption of the brain reward cascade function. We evaluated the potential association of four variants of dopaminergic candidate genes in RDS (dopamine D1 receptor gene [DRD1]; dopamine D2 receptor gene [DRD2]; dopamine transporter gene [DAT1]; dopamine beta-hydroxylase gene [DBH]). Methodology: We genotyped an experimental group of 55 subjects derived from up to five generations of two independent multiple-affected families compared to rigorously screened control subjects (e.g., N = 30 super controls for DRD2 gene polymorphisms). Data related to RDS behaviors were collected on these subjects plus 13 deceased family members. Results: Among the genotyped family members, the DRD2 Taq1 and the DAT1 10/10 alleles were significantly (at least p < 0.015) more often found in the RDS families vs. controls. The TaqA1 allele occurred in 100% of Family A individuals (N = 32) and 47.8% of Family B subjects (11 of 23). No significant differences were found between the experimental and control positive rates for the other variants. Conclusions: Although our sample size was limited, and linkage analysis is necessary, the results support the putative role of dopaminergic polymorphisms in RDS behaviors. This study shows the importance of a nonspecific RDS phenotype and informs an understanding of how evaluating single subset behaviors of RDS may lead to spurious results. Utilization of a nonspecific “reward” phenotype may be a paradigm shift in future association and linkage studies involving dopaminergic polymorphisms and other neurotransmitter gene candidates.

Published
2011

20. Overcoming qEEG Abnormalities and Reward Gene Deficits during Protracted Abstinence in Male Psychostimulant and Polydrug Abusers Utilizing Putative Dopamine D2Agonist Therapy: Part 2

Author

Roger L. Waite, Thomas J H Chen, Siobhan Morse, Eric Stice, John Giordano, Eric R Braverman, Mallory Kerner, Andrew Smolen, Joel F. Lubar, Amanda Lih Chaun Chen, Frank Fornari, Kenneth Blum, Margaret A. Madigan, Cameron Allen, B. William Downs, and James E. Thompson

Subjects
Agonist, medicine.medical_specialty, medicine.diagnostic_test, business.industry, medicine.drug_class, General Medicine, Electroencephalography, Placebo, Crossover study, law.invention, Endocrinology, Randomized controlled trial, law, Dopamine, Internal medicine, Medicine, Allele, Beta wave, business, Psychiatry, medicine.drug
Abstract

Background: It is well established that in both food- and drug-addicted individuals there is “dopamine resistance” associated with the DRD2 gene A1 allele. Based on earlier studies, evidence is emerging wherein the potential of utilizing a natural, nonaddicting, safe, putative D2 agonist may play a significant role in the recovery of individuals with reward deficiency syndrome, including those addicted to psychoactive chemicals. Findings: Positive outcomes demonstrated by quantitative electroencephalographic (qEEG) imaging in a randomized, triple-blind, placebo-controlled, crossover study involving oral Synaptose Complex KB220Z™ showed an increase of alpha waves and low beta wave activity in the parietal brain region. Using t statistics, significant differences observed between placebo and Synaptose Complex KB220Z™ consistently occurred in the frontal regions after week 1 and then again after week 2 of analyses (P = 0.03). This is the first report to demonstrate involvement of the prefrontal corte...

Published
2010

21. Do dopaminergic gene polymorphisms affect mesolimbic reward activation of music listening response? Therapeutic impact on Reward Deficiency Syndrome (RDS)

Author

Thomas J H Chen, Eric R Braverman, Roger L. Waite, Harry Henshaw, Amanda L.H. Chen, Abdalla Bowirrat, Kenneth Blum, John Giordano, Mallory Kerner, Margaret A. Madigan, Mark S. Gold, and B. William Downs

Subjects
media_common.quotation_subject, Models, Neurological, Nucleus accumbens, Polymorphism, Single Nucleotide, Reward, Dopamine, Dopamine receptor D2, Limbic System, medicine, Humans, Genetic Predisposition to Disease, Music Therapy, media_common, Models, Genetic, Mental Disorders, Addiction, Dopaminergic, General Medicine, humanities, Ventral tegmental area, medicine.anatomical_structure, Auditory Perception, Brain stimulation reward, Orbitofrontal cortex, Psychology, Neuroscience, Music, psychological phenomena and processes, medicine.drug
Abstract

Using fMRI, Menon and Levitin [9] clearly found for the first time that listening to music strongly modulates activity in a network of mesolimbic structures involved in reward processing including the nucleus accumbens (NAc) and the ventral tegmental area (VTA), as well as the hypothalamus, and insula, which are thought to be involved in regulating autonomic and physiological responses to rewarding and emotional stimuli. Importantly, responses in the NAc and VTA were strongly correlated pointing to an association between dopamine release and NAc response to music. Listing to pleasant music induced a strong response and significant activation of the VTA-mediated interaction of the NAc with the hypothalamus, insula, and orbitofrontal cortex. Blum et al. [10] provided the first evidence that the dopamine D2 receptor gene (DRD2) Taq 1 A1 allele significantly associated with severe alcoholism whereby the author's suggested that they found the first "reward gene" located in the mesolimbic system. The enhanced functional and effective connectivity between brain regions mediating reward, autonomic, and cognitive processing provides insight into understanding why listening to music is one of the most rewarding and pleasurable human experiences. However, little is known about why some people have a more or less powerful mesolimbic experience when they are listening to music. It is well-known that music may induce an endorphinergic response that is blocked by naloxone, a known opioid antagonist (Goldstein [19]). Opioid transmission in the NAc is associated with dopamine release in the VTA. Moreover, dopamine release in the VTA is linked to polymorphisms of the DRD2 gene and even attention-deficit hyperactivity disorder (ADHD), whereby carriers of the DRD2 A1 allele show a reduced NAc release of dopamine (DA). Thus it is conjectured that similar mechanisms in terms of adequate dopamine release and subsequent activation of reward circuitry by listening to music might also be affected by an individual's D2 density in the VTA mediated interaction of the NAc. It is therefore hypothesized that carriers of DRD2 A1 allele may respond significantly differently to carriers of the DRD2 A2 genotype. In this regard, carriers of the D2 A1 allele have a blunted response to glucose and monetary rewards. In contrast powerful D2 agonists like bromocryptine show a heightened activation of the reward circuitry only in DRD2 A1 allele carriers. If music causes a powerful activation in spite of the DRD2 A1 allele due to a strong DA neuronal release which subsequently impinges on existing D2 receptors, then it is reasonable to assume that music is a strong indirect D2 agonist (by virtue of DA neuronal release in the NAc) and may have important therapeutic applicability in Reward Deficiency Syndrome (RDS) related behaviors including Substance Use Disorder (SUD). Ross et al. [18] found that music therapy appears to be a novel motivational tool in a severely impaired inpatient sample of patients with co-occurring mental illness and addiction.

Published
2010

22. Neuro-psychopharmacogenetics and Neurological Antecedents of Posttraumatic Stress Disorder: Unlocking the Mysteries of Resilience and Vulnerability

Author

John A. Bailey, John Giordano, Amanda Lih Chuan Chen, Roger L. Waite, Eric R. Braverman, Thomas J H Chen, Kenneth Blum, Margaret A. Madigan, Marlene Oscar-Berman, Mallory Kerner, Shahien Radi, B. William Downs, Mark S. Gold, Abdalla Bowirrat, and Siohban Morse

Subjects
Post-traumatic Stress Disorder (PTSD), media_common.quotation_subject, Serotonergic, Article, neurotransmitters, 03 medical and health sciences, 0302 clinical medicine, Neurochemical, Neurotrophic factors, Medicine, Pharmacology (medical), Reward Deficiency Syndrome (RDS), media_common, Genetic testing, Post-traumatic stress disorder (PTSD), Pharmacology, medicine.diagnostic_test, business.industry, Dopaminergic, General Medicine, medicine.disease, 3. Good health, 030227 psychiatry, Psychiatry and Mental health, genes and environment, Neurology, Neurology (clinical), Psychological resilience, business, 030217 neurology & neurosurgery, Glucocorticoid, medicine.drug, Clinical psychology
Abstract

Background and Hypothesis: Although the biological underpinnings of immediate and protracted trauma- related responses are extremely complex, 40 years of research on humans and other mammals have demonstrated that trauma (particularly trauma early in the life cycle) has long-term effects on neurochemical responses to stressful events. These effects include the magnitude of the catecholamine response and the duration and extent of the cortisol response. In addition, a number of other biological systems are involved, including mesolimbic brain structures and various neuro- transmitters. An understanding of the many genetic and environmental interactions contributing to stress-related responses will provide a diagnostic and treatment map, which will illuminate the vulnerability and resilience of individuals to Posttraumatic Stress Disorder (PTSD). Proposal and Conclusions: We propose that successful treatment of PTSD will involve preliminary genetic testing for specific polymorphisms. Early detection is especially important, because early treatment can improve outcome. When genetic testing reveals deficiencies, vulnerable individuals can be recommended for treatment with "body friendly" pharmacologic substances and/or nutrients. Results of our research suggest the following genes should be tested: serotoninergic, dopaminergic (DRD2, DAT, DBH), glucocorticoid, GABAergic (GABRB), apolipoprotein systems (APOE2), brain-derived neurotrophic factor, Monamine B, CNR1, Myo6, CRF-1 and CRF-2 receptors, and neuropeptide Y (NPY). Treatment in part should be developed that would up-regulate the expression of these genes to bring about a feeling of well being as well as a reduction in the frequency and intensity of the symptoms of PTSD.

Published
2010

23. Can Genetic Testing Coupled with Enhanced Dopaminergic Activation Reduce Recidivism Rates in the Workers Compensation Legacy Cases?

Author

Seth H. Blum, Kenneth Blum, Roger L. Waite, Debmalya Barh, Marlene Oscar-Berman, Margaret A. Madigan, and Thomas McLaughlin

Subjects
medicine.medical_specialty, education.field_of_study, medicine.diagnostic_test, Operations research, Recidivism, Dopaminergic, Population, Multiple sex partners, Workers' compensation, Behavioral addictions, Article, 3. Good health, medicine, Genetic predisposition, Psychiatry, education, Psychology, Genetic testing
Abstract

An overwhelming segment of the world’s population possesses certain genetic variations that increase risk for genetic predispositions to substance seeking and even behavioral addictions (e.g. gambling, internet gaming, multiple sex partners etc.) that preclude them from reaching their optimum health potential, contribute to impaired health, and/or can cause involuntary indulgence in detrimental and self-destructive behaviors.

Published
2014

24. OMICS : Biomedical Perspectives and Applications

Author

Debmalya Barh, Kenneth Blum, Margaret A. Madigan, Debmalya Barh, Kenneth Blum, and Margaret A. Madigan

Subjects
Proteomics, Glycomics, Biotechnology, Bioinformatics, Computational biology, Genomics, Bioengineering
Abstract

A reflection of the explosion of research and development in this field, OMICS: Biomedical Perspectives and Applications explores applications of omics in bioinformatics, cancer research and therapy, diabetes research, plant science, molecular biology, and neurosciences. A select editorial panel of experts discusses their cutting edge omics researc

Published
2012

25. Declinol, a Complex Containing Kudzu, Bitter Herbs (Gentian, Tangerine Peel) and Bupleurum, Significantly Reduced Alcohol Use Disorders Identification Test (AUDIT) Scores in Moderate to Heavy Drinkers: A Pilot Study

Author

Kenneth Blum, Thomas Beley, Raquel Lohmann, Stephen J. Schoenthaler, David K. Han, Kristina Dushaj, David Ellison, Marlene Oscar-Berman, Thomas Simpatico, Scott Jones, Eric R. Braverman, Debmayla Barh, William Downs B, Steven Kushner, Margaret A. Madigan, and John Giordano

Subjects
Ethanol, Alcohol Use Disorders Identification Test, biology, business.industry, Acetaldehyde, Stimulation, Craving, Alcohol, Pharmacology, biology.organism_classification, Kudzu, Article, chemistry.chemical_compound, chemistry, medicine, medicine.symptom, Daidzin, business
Abstract

It is well established that inherited human aldehyde dehydrogenase 2 (ALDH-2) deficiency reduces the risk for alcoholism. Kudzu plants and extracts have been used for 1,000 years in traditional Chinese medicine to treat alcoholism. Kudzu contains daidzin, which inhibits ALDH-2 and suppresses heavy drinking in rodents. Decreased drinking due to ALDH-2 inhibition is attributed to aversive properties of acetaldehyde accumulated during alcohol consumption. However not all of the anti-alcohol properties of diadzin are due to inhibition of ALDH-2. This is in agreement with our earlier work showing significant interaction effects of both pyrozole (ALDH-2 inhibitor) and methyl-pyrozole (non-inhibitor) and ethanol's depressant effects. Moreover, it has been suggested that selective ALDH 2 inhibitors reduce craving for alcohol by increasing dopamine in the nucleus accumbens (NAc). In addition there is significant evidence related to the role of the genetics of bitter receptors (TAS2R) and its stimulation as an aversive mechanism against alcohol intake. The inclusion of bitters such as Gentian & Tangerine Peel in Declinol provides stimulation of gut TAS2R receptors which is potentially synergistic with the effects of Kudzu. Finally the addition of Radix Bupleuri in the Declinol formula may have some protective benefits not only in terms of ethanol induced liver toxicity but neurochemical actions involving endorphins, dopamine and epinephrine. With this information as a rationale, we report herein that this combination significantly reduced Alcohol Use Disorders Identification Test (AUDIT) scores administered to ten heavy drinkers (M=8, F=2; 43.2 ± 14.6 years) attending a recovery program. Specifically, from the pre-post comparison of the AUD scores, it was found that the score of every participant decreased after the intervention which ranged from 1 to 31. The decrease in the scores was found to be statistically significant with the p-value of 0.00298 (two-sided paired test; p-value = 0.00149 for one-sided test). Albeit this being a small pilot, we are encouraged about these significant results, and caution any interpretation until larger controlled studies are executed.

Published
2013

26. Audio Therapy Significantly Attenuates Aberrant Mood in Residential Patient Addiction Treatment: Putative Activation of Dopaminergic Pathways in the Meso-Limbic Reward Circuitry of Humans

Author

Kenneth Blum, Kenneth Perrine, Holistic Addiction, Margaret A. Madigan, Uma Damle, John Giordano, Thomas Simpatico, Eric R. Braverman, Siobhan Morse, Debmalya Barh, B. William Downs, Roger L. Waite, Jennifer Knopf, Monty D. Moeller, and John A. Bailey

Subjects
Music therapy, Relaxation (psychology), Addiction, media_common.quotation_subject, Mood swing, Nucleus accumbens, behavioral disciplines and activities, humanities, Ventral tegmental area, medicine.anatomical_structure, Mood, Dopaminergic pathways, medicine, medicine.symptom, Psychology, media_common, Clinical psychology
Abstract

Using fMRI, Menon and Levitin and Salimpoor et al. clearly show that listening to music strongly modulates activity in a network of mesolimbic structures involved in reward processing including the nucleus accumbens (NAc) and the ventral tegmental area (VTA), as well as the hypothalamus, and insula, which are thought to be involved in regulating autonomic and physiological responses to rewarding and emotional stimuli. We hypothesized that patients exposed to Stress & Deep Relaxation using Audio Therapy (music & sound) would show significant improvements in ten withdrawal symptoms systematically assessed supporting a role for this modality in recovery of patients with co-occurring mental illness and addiction. Thus our laboratory embarked on the evaluation of pleasant audio therapy in addicted patients undergoing recovery in our in-patient facility. We found significant pre to post Stress & Deep Relaxation using Audio Therapy (music & sound) in 76 drug dependent patients. Significant (at least p

Published
2013

27. Neurogenetics and Nutrigenomics of Reward Deficiency Syndrome (RDS): Stratification of Addiction Risk and Mesolimbic Nutrigenomic Manipulation of Hypodopaminergic Function

Author

Downs Bw, Margaret A. Madigan, John Giordano, Thomas Simpatico, Mary Hauser, Kenneth Blum, David K. Han, Raquel Lohmann, Eric R. Braverman, Debmalya Barh, and John Femino

Subjects
medicine.medical_specialty, Framingham Risk Score, media_common.quotation_subject, Addiction, Dopaminergic, Neurogenetics, Biology, Abstinence, Nutrigenomics, medicine, Brain stimulation reward, Function (engineering), Psychiatry, Neuroscience, media_common
Abstract

We have entered the genomics era with hope for the future of medicine including psychiatry. Understanding the role of DNA and polymorphic associations with brain reward circuitry has led to a new understanding of all addictive behaviors. We present here a brief review of the role of both neurogenetics and nutrigenomics as cornerstones that link more accurate genetic diagnosis and dopamine D2 agonist therapy to induce dopaminergic activation. Based on numerous experiments we are indeed proposing a novel approach. We challenge the entire recovery field to use these tools, the result of years of scientific research into the nature of addiction, and to incorporate them into treatment programs for patients attending inpatient/outpatient addiction clinics, such as the Genetic Addiction Risk Score (GARS)™ for appropriate RDS diagnosis, Comprehensive Analysis of Reported Drugs (CARD)™ to determine both compliance and abstinence during treatment, natural D2 agonistic therapy (NAAT-KB220™), and, eventually, mRNA (patent pending) to determine pre- and post-candidate gene expressions in reward deficiency syndrome (RDS). We are, therefore, proposing a paradigm shift we have called “Reward Deficiency Solutions System (RDSS)™.”

Published
2013

28. Have We Hatched the Addiction Egg: Reward Deficiency Syndrome Solution System™

Author

Marlene Oscar-Berman, Kristina Dushaj, ST Schoenthaler, Mary Hauser, Eric R Braverman, David K. Han, Roger L. Waite, S Jones, Thomas Simpatico, Kenneth Blum, Joan Borsten, M Helman, F Marcelo, John Giordano, Debmayla Barh, Beley Tg, Downs Bw, Raquel Lohmann, and Margaret A. Madigan

Subjects
medicine.medical_specialty, Deficiency syndrome, Social work, business.industry, Addiction, media_common.quotation_subject, Alternative medicine, Bioinformatics, Article, humanities, Solution system, Treatment center, Treatment targets, Paradigm shift, medicine, business, Psychiatry, health care economics and organizations, media_common
Abstract

This article co-authored by a number of scientists, ASAM physicians, clinicians, treatment center owners, geneticists, neurobiologists, psychologists, social workers, criminologists, nurses, nutritionist, and students, is dedicated to all the people who have lost loved ones in substance-abuse and “reward deficiency syndrome” related tragedies. Why are we failing at reducing the incidence of ‘Bad Behaviors’? Are we aiming at the wrong treatment targets for behavioral disorders? We are proposing a paradigm shift and calling it “Reward Deficiency Solution System” providing evidence for its adoption.

Published
2013

29. Neuropsychiatric Genetics of Happiness, Friendships, and Politics: Hypothesizing Homophily ('Birds of a Feather Flock Together') as a Function of Reward Gene Polymorphisms

Author

Kenneth Blum, Marlene Oscar-Berman, Eric R Braverman, Abdalla Bowirrat, Debmayla Barh, Mary Hauser, Joan Borsten, Thomas Simpatico, Margaret A. Madigan, and John Giordano

Subjects
business.industry, media_common.quotation_subject, Addiction, Poison control, Turnout, Conservatism, Homophily, Article, Voting, Happiness, Medicine, Ideology, business, Social psychology, media_common
Abstract

Mindful of the new evolutionary ideas related to an emerging scientific focus known as omics, we propose that spiritual, social, and political behaviors may be tied in part to inheritable reward gene polymorphisms, as has been demonstrated for the addictions. If so, analyses of gene polymorphisms may assist in predicting liberalism or conservatism in partisan attachments. For example, both drinking (alcohol) and obesity seem to cluster in large social networks and are influenced by friends having the same genotype, in particular the DRD2 A1 allele. Likewise, voting, voting turnout and attachment to a particular political ideology is differentially related to various reward genes (e.g., 5HTT, MOA, DRD2, and DRD4), possibly predicting liberalism or conservatism. Moreover, voters' genetic information may predict presidential outcomes more than the actual issues at hand or the presidential candidates themselves. Thus, political discussions on TV, radio, or other media may be morphed by one's reward gene polymorphisms and as such, may explain the prevalence of generations of die-hard republicans and equally entrenched democratic legacies. Indeed, even in politics, birds of a feather (homophily) flock together. We caution that our proposal should be viewed mindfully awaiting additional research before definitive statements or conclusions can be derived from the studies to date, and we encourage large scale studies to confirm these earlier reports.

Published
2012

30. Neuropsychopharmacology and Neurogenetic Aspects of Executive Functioning: Should Reward Gene Polymorphisms Constitute a Diagnostic Tool to Identify Individuals at Risk for Impaired Judgment?

Author

Roger L. Waite, Abdalla Bowirrat, Eric R Braverman, Marlene Oscar-Berman, Thomas J H Chen, John A. Bailey, Frank Fornari, Mallory Kerner, John Giordano, Kenneth Blum, B. William Downs, Siobhan Morse, Margaret A. Madigan, Amanda Lh Chen, and Zaher Armaly

Subjects
Brain Chemistry, medicine.medical_specialty, Neurology, Polymorphism, Genetic, Neuroscience (miscellaneous), Cognition, Executive functions, Article, Neuropsychopharmacology, Cellular and Molecular Neuroscience, Executive Function, Environmental risk, Molecular Diagnostic Techniques, Reward, medicine, Impaired judgment, Animals, Humans, Genetic Predisposition to Disease, Prefrontal cortex, Psychology, Cognition Disorders, Neuroscience, Executive dysfunction
Abstract

Executive functions are processes that act in harmony to control behaviors necessary for maintaining focus and achieving outcomes. Executive dysfunction in neuropsychiatric disorders is attributed to structural or functional pathology of brain networks involving prefrontal cortex (PFC) and its connections with other brain regions. The PFC receives innervations from different neurons associated with a number of neurotransmitters, especially dopamine (DA). Here we review findings on the contribution of PFC DA to higher-order cognitive and emotional behaviors. We suggest that examination of multifactorial interactions of an individual’s genetic history, along with environmental risk factors, can assist in the characterization of executive functioning for that individual. Based upon the results of genetic studies, we also propose genetic mapping as a probable diagnostic tool serving as a therapeutic adjunct for augmenting executive functioning capabilities. We conclude that preservation of the neurological underpinnings of executive functions requires the integrity of complex neural systems including the influence of specific genes and associated polymorphisms to provide adequate neurotransmission.

Published
2012

31. Future Perspective

Author

Kenneth Blum, Debmalya Barh, and Margaret A. Madigan

Subjects
Future perspective, Operations research, Management science, Computer science, Path (graph theory)
Published
2011

32. Overcoming qEEG abnormalities and reward gene deficits during protracted abstinence in male psychostimulant and polydrug abusers utilizing putative dopamine D₂ agonist therapy: part 2

Author

Kenneth, Blum, Thomas J H, Chen, Siobhan, Morse, John, Giordano, Amanda Lih Chaun, Chen, James, Thompson, Cameron, Allen, Andrew, Smolen, Joel, Lubar, Eric, Stice, B William, Downs, Roger L, Waite, Margaret A, Madigan, Mallory, Kerner, Frank, Fornari, and Eric R, Braverman

Subjects
Adult, Male, Cross-Over Studies, Polymorphism, Genetic, Receptors, Dopamine D2, Substance-Related Disorders, Administration, Oral, Electroencephalography, Risk Assessment, Substance Withdrawal Syndrome, Behavior, Addictive, Treatment Outcome, Reward, Dopamine Agonists, Humans, Central Nervous System Stimulants, Follow-Up Studies
Abstract

It is well established that in both food- and drug-addicted individuals there is "dopamine resistance" associated with the DRD2 gene A1 allele. Based on earlier studies, evidence is emerging wherein the potential of utilizing a natural, nonaddicting, safe, putative D2 agonist may play a significant role in the recovery of individuals with reward deficiency syndrome, including those addicted to psychoactive chemicals.Positive outcomes demonstrated by quantitative electroencephalographic (qEEG) imaging in a randomized, triple-blind, placebo-controlled, crossover study involving oral Synaptose Complex KB220Z™ showed an increase of alpha waves and low beta wave activity in the parietal brain region. Using t statistics, significant differences observed between placebo and Synaptose Complex KB220Z™ consistently occurred in the frontal regions after week 1 and then again after week 2 of analyses (P = 0.03). This is the first report to demonstrate involvement of the prefrontal cortex in the qEEG response to a natural putative D2 agonist (Synaptose Complex KB220Z™), especially evident in dopamine D2 A1 allele subjects. Independently, we have further supported this finding with an additional study of 3 serious polydrug abusers undergoing protracted abstinence who carried the DRD2 A1 allele. Significant qEEG differences were found between those who received 1 dose of placebo compared with those who were administered Synaptose Complex KB220Z™. Synaptose Complex KB220Z™ induced positive regulation of the dysregulated electrical activity of the brain in these addicts. The results are indicative of a phase change from low amplitude or low power in the brain to a more regulated state by increasing an average of 6.169 mV(2) across the prefrontal cortical region. In the first experiment we found that while 50% of the subjects carried the DRD2 A1 allele, 100% carried ≥ 1 risk allele. Specifically, based on the proposed addiction risk score for these 14 subjects, 72% had moderate-to-severe addiction risk. Similar findings were obtained by repeating the experiment in 3 additional currently abstinent polydrug abusers carrying the DRD2 A1 allele.This seminal work will provide important information that may ultimately lead to significant improvement in the recovery of individuals with psychostimulant and polydrug abuse problems, specifically those with genetically induced dopamine deficiency. Based on this small sample size, we are proposing that with necessary large populations supporting these initial results, and possibly even additional candidate genes and single nucleotide polymorphisms, we may eventually have the clinical ability to classify severity according to genotype and possession of risk alleles, along with offering a safe, nonaddicting, natural dopaminergic receptor agonist that potentially upregulates instead of downregulates dopaminergic receptors, preferably the D2 subtype.

Published
2010

33. Adult growth hormone deficiency treatment with a combination of growth hormone and insulin-like growth factor-1 resulting in elevated sustainable insulin-like growth factor-1 and insulin-like growth factor binding protein 3 plasma levels: a case report

Author

Eric R Braverman, Kenneth Blum, Uma Damle, Stanley X Huang, Margaret A. Madigan, Mallory Kerner, Swetha Yeldandi, Stella Savarimuthu, Abdalla Bowirrat, and Thomas Jh Chen

Subjects
Medicine(all), medicine.medical_specialty, biology, business.industry, Binding protein, medicine.medical_treatment, Growth factor, lcsh:R, lcsh:Medicine, Case Report, General Medicine, Bedtime, Insulin-like growth factor-binding protein, Growth hormone treatment, Insulin-like growth factor, Endocrinology, Surgical oncology, Internal medicine, medicine, biology.protein, Amenorrhea, medicine.symptom, business
Abstract

Introduction Adult Growth hormone Deficiency is a well known phenomenon effecting both males and females. Adult Growth Hormone Deficiency is marked by a number of neuropsychiatric, cognitive performance, cardiac, metabolic, muscular, and bone symptoms and clinical features. There is no known standardized acceptable therapeutic modality to treat this condition. A recent meta-analysis found that after 16 years of Growth Hormone replacement therapy a large proportion of the patients still had Growth Hormone associated symptoms especially related to executive functioning. A major goal is to increase plasma levels of both insulin-like growth factor (insulin-like growth factor-1) and insulin-like growth factor binding protein 3. Case Presentation We report a case of a 45-year-old caucasian woman with early ovarian failure for 2 years and amenorrhea since the age of 43, who presented with Adult Growth Hormone Deficiency and an IGF-1 of 126 ng/mL. Since her insulin-like growth factor-1 was lowest at 81 ng/mL, she was started on insulin-like growth factor-1 Increlex at 0.2 mg at bedtime, which immediately raised her insulin-like growth factor-1 levels to 130 ng/mL within 1 month, and 193 ng/mL, 249 ng/mL, and 357 ng/mL, after 3, 4, and 5 months, respectively, thereafter. Her insulin-like growth factor binding protein 3 continued to decrease. It was at this point when we added back the Growth Hormone and increased her Increlex dosage to 1.3 - 1.5 mg that her insulin-like growth factor binding protein 3 began to increase. Conclusion It appears that in some patients with Adult Growth Hormone Deficiency, insulin-like growth factor-1 elevation is resistant to direct Growth Hormone treatment. Furthermore, the binding protein may not rise with insulin-like growth factor-1. However, a combination of Growth Hormone and insulin-like growth factor-1 treatment may be a solution.

Published
2010

34. Healing enhancement of chronic venous stasis ulcers utilizing H-WAVE®device therapy: a case series

Author

Seth H. Blum, Mallory Kerner, John Giordano, Kenneth Blum, Gary Reinl, Stella Savarimuthu, Margaret A. Madigan, B. William Downs, Thomas Jh Chen, Eric R. Braverman, Nicholas A. DiNubile, Amanda Lh Chen, and Anish Bajaj

Subjects
Medicine(all), medicine.medical_specialty, business.industry, medicine.medical_treatment, Venous Stasis Ulcers, Case Report, General Medicine, Disease, medicine.disease, Surgery, Microcirculation, Venous stasis, Amputation, Device therapy, Diabetes mellitus, Medicine, business, Healed ulcer
Abstract

Introduction Approximately 15% (more than 2 million individuals, based on these estimates) of all people with diabetes will develop a lower-extremity ulcer during the course of the disease. Ultimately, between 14% and 20% of patients with lower-extremity diabetic ulcers will require amputation of the affected limb. Analysis of the 1995 Medicare claims revealed that lower-extremity ulcer care accounted for $1.45 billion in Medicare costs. Therapies that promote rapid and complete healing and reduce the need for expensive surgical procedures would impact these costs substantially. One such example is the electrotherapeutic modality utilizing the H-Wave® device therapy and program. It has been recently shown in acute animal experiments that the H-Wave® device stimulation induces a nitric oxide-dependent increase in microcirculation of the rat Cremaster skeletal muscle. Moreover, chronic H-wave® device stimulation of rat hind limbs not only increases blood flow but induces measured angiogenesis. Coupling these findings strongly suggests that H-Wave® device stimulation promotes rapid and complete healing without need of expensive surgical procedures. Case presentation We decided to do a preliminary evaluation of the H-Wave® device therapy and program in three seriously afflicted diabetic patients. Patient 1 had chronic venous stasis for 6 years. Patient 2 had chronic recurrent leg ulcerations. Patient 3 had a chronic venous stasis ulcer for 2 years. All were dispensed a home H-Wave® unit. Patient 1 had no other treatment, patient 2 had H-Wave® therapy along with traditional compressive therapy, and patient 3 had no other therapy. For patient 1, following treatment the ulcer completely healed with the H-Wave® device and program after 3 months. For patient 2, by one month complete ulcer closure occurred. Patient 3 had a completely healed ulcer after 9 months. Conclusions While most diabetic ulcers can be treated successfully on an outpatient basis, a significant proportion will persist and become infected. Based on this preliminary case series investigation we found that three patients prescribed H-Wave® home treatment demonstrate accelerated healing with excellent results. While these results are encouraging, additional large scale investigation is warranted before any interpretation is given to these interesting outcomes.

Published
2010

35. Neurogenetics of dopaminergic receptor supersensitivity in activation of brain reward circuitry and relapse: proposing 'deprivation-amplification relapse therapy' (DART)

Author

Margaret A. Madigan, Roger L. Waite, John Giordano, Abdalla Bowirrat, Eric Stice, B. William Downs, Mark S. Gold, Eric R Braverman, Nicholas A. DiNubile, Siobhan Morse, Kenneth Blum, Marlene Oscar-Berman, and Thomas J H Chen

Subjects
Agonist, medicine.medical_specialty, medicine.drug_class, Substance-Related Disorders, Neurogenetics, Dopamine agonist, Euphoriant, Article, Reward, Dopamine receptor D2, medicine, Secondary Prevention, Animals, Humans, Psychiatry, Polymorphism, Genetic, business.industry, Receptors, Dopamine D2, Dopaminergic, General Medicine, Models, Theoretical, Bromocriptine, Rats, Behavior, Addictive, Dopamine Agonists, Brain stimulation reward, business, Neuroscience, medicine.drug
Abstract

It is well known that after prolonged abstinence, individuals who use their drug of choice experience a powerful euphoria that often precipitates relapse. While a biological explanation for this conundrum has remained elusive, we hypothesize that this clinically observed "supersensitivity" might be tied to genetic dopaminergic polymorphisms. Another therapeutic conundrum relates to the paradoxical finding that the dopaminergic agonist bromocriptine induces stronger activation of brain reward circuitry in individuals who carry the DRD2 A1 allele compared with DRD2 A2 allele carriers. Because carriers of the A1 allele relative to the A2 allele of the DRD2 gene have significantly lower D2 receptor density, a reduced sensitivity to dopamine agonist activity would be expected in the former. Thus, it is perplexing that with low D2 density there is an increase in reward sensitivity with the dopamine D2 agonist bromocriptine. Moreover, under chronic or long-term therapy with D2 agonists, such as bromocriptine, it has been shown in vitro that there is a proliferation of D2 receptors. One explanation for this relates to the demonstration that the A1 allele of the DRD2 gene is associated with increased striatal activity of L-amino acid decarboxylase, the final step in the biosynthesis of dopamine. This appears to be a protective mechanism against low receptor density and would favor the utilization of an amino acid neurotransmitter precursor like L-tyrosine for preferential synthesis of dopamine. This seems to lead to receptor proliferation to normal levels and results in significantly better treatment compliance only in A1 carriers.We propose that low D2 receptor density and polymorphisms of the D2 gene are associated with risk for relapse of substance abuse, including alcohol dependence, heroin craving, cocaine dependence, methamphetamine abuse, nicotine sensitization, and glucose craving. With this in mind, we suggest a putative physiological mechanism that may help to explain the enhanced sensitivity following intense acute dopaminergic D2 receptor activation: "denervation supersensitivity." Rats with unilateral depletions of neostriatal dopamine display increased sensitivity to dopamine agonists estimated to be 30 to 100 x in the 6-hydroxydopamine (6-OHDA) rotational model. Given that mild striatal dopamine D2 receptor proliferation occurs (20%-40%), it is difficult to explain the extent of behavioral supersensitivity by a simple increase in receptor density. Thus, the administration of dopamine D2 agonists would target D2 sensitization and attenuate relapse, especially in D2 receptor A1 allele carriers. This hypothesized mechanism is supported by clinical trials utilizing amino acid neurotransmitter precursors, enkephalinase, and catechol-O-methyltransferase (COMT) enzyme inhibition, which have resulted in attenuated relapse rates in reward deficiency syndrome (RDS) probands. If future translational research reveals that dopamine agonist therapy reduces relapse in RDS, it would support the proposed concept, which we term "deprivation-amplification relapse therapy" (DART). This term couples the mechanism for relapse, which is "deprivation-amplification," especially in DRD2 A1 allele carriers with natural D2 agonist therapy utilizing amino acid precursors and COMT and enkepalinase inhibition therapy.

Published
2009

36. A Multi-Locus Approach to Treating Fibromyalgia by Boosting Dopaminergic Activity in the Meso-Limbic System of the Brain

Author

Kristina Dushaj, Thomas Simpatico, Debmalya Barh, Margaret A. Madigan, Florian Kreuk, Roger L. Waite, Mona Li, Mary Hauser, Kenneth Blum, Marlene Oscar-Berman, and Eric R. Braverman

Subjects
030203 arthritis & rheumatology, Boosting (doping), medicine.medical_specialty, Exacerbation, business.industry, Dopaminergic, Cognition, medicine.disease, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Limbic system, medicine.anatomical_structure, chemistry, Dopamine, Fibromyalgia, medicine, Psychiatry, business, Neurotransmitter, Neuroscience, 030217 neurology & neurosurgery, medicine.drug
Abstract

Fibromyalgia (FM), is associated with fatigue, chronic diffuse pain, and cognitive/mood disturbances [1,2]. FM patients have greater healthcare costs and reduced workplace productivity. Stress and the neurotransmitter dopamine may interact, and this interaction may induce FM. Interestingly, FM has been called a ‘stress-related disorder’ presenting an exacerbation of symptoms on the context of stressful events [3].Certainly, many genes are involved in FM causation and potential predisposition. However, it is important to realize that epigenetics may also be involved in the progression of this disorder. Specifically, Menzies

Published
2014

37. Nutrigenomics of Neuradaptogen Amino-Acid-Therapy and Neurometabolic Optimizers: Overcoming carbohydrate bingeing and overeating through neurometabolic mechanisms

Author

Eric R. Braverman, Kenneth Blum, Debasis Bagchi, Debmayla Barh, Jaclyn M. Downs, Thomas Simpatico, Margaret A. Madigan, B. William Downs, Margaret Polanin, Abdalla Bowirrat, John Giordano, Frank Fornari, Roger L. Waite, and Siohban Morse

Subjects
medicine.medical_specialty, Dopamine, Medicine (miscellaneous), lcsh:TX341-641, Craving, Bioinformatics, Biochemistry, Norepinephrine, Internal medicine, medicine, NAAT, Obesity, Overeating, Catecholaminergic, lcsh:R5-920, Nutrition and Dietetics, business.industry, Reward Deficiency Syndome, medicine.disease, Nutrigenomics, Review article, Craving Behavior, Endocrinology, Genes, medicine.symptom, Polymorphisms, lcsh:Medicine (General), business, lcsh:Nutrition. Foods and food supply, Food Science, medicine.drug
Abstract

Despite progress that has been made in the treatment of obesity, the epidemic continues to rise worldwide. While pharmacological treatment of obesity may be effective, medications may have significant side effects and can be potentially fatal. This review will provide significant evidence to substantiate the existence of Reward Deficiency Syndrome in Obesity and the role of catecholaminergic pathways in aberrant substance seeking behavior, in particular cravings for carbohydrates. The genetic basis for generalized craving behavior will be established. Evidence to support the augmentation of precursor amino acid therapy and enkephalinase, MOA and COMT inhibition leading to enhanced levels of neurotransmitters: serotonin, enkephalins, GABA and dopamine/norepinephrine as well increasing insulin sensitivity (affecting dopamine neuronal synthesis regulation) through the use of certain neurometabolic optimizers will also be provided. This review article cites many published studies to support a conceptual paradigm shift towards the use of this proposed nutrigenomic formula. The analysis and research preceding this formulation is outlined. This formulation has a generalized anti-craving effect and can inhibit carbohydrate bingeing, inducing significant healthy fat loss and prevention of relapse. This is the first time that components of this formula have been combined, at the dosage levels indicated with the goal of promoting successful and sustainable body recomposition. We are encouraging other laboratories to further evaluate Neuroadtagen Amino-Acid Therapy (NAAT)/Nurometabolic optimizers as a putative anti-obesity complex in larger controlled blinded studies and await interpretation of must these needed studies. Keywords: NAAT, Dopamine, Genes, Polymorphisms, Obesity, Craving Behavior, Overeating, Reward Deficiency Syndome, Nutrigenomics.

Published
2011

38. 'Cold' X5 Hairlaser™ used to treat male androgenic alopecia and hair growth: an uncontrolled pilot study

Author

Margaret A. Madigan, Kenneth Blum, Eric R. Braverman, Raquel Lohmann, and David K. Han

Subjects
Adult, Male, medicine.medical_specialty, Randomization, Time Factors, Population, Physiology, Pilot Projects, Monochromatic light, General Biochemistry, Genetics and Molecular Biology, law.invention, Hair growth, Randomized controlled trial, law, Linear regression, medicine, Humans, education, Device failure, Medicine(all), education.field_of_study, integumentary system, business.industry, Biochemistry, Genetics and Molecular Biology(all), Repeated measures design, Alopecia, General Medicine, Middle Aged, medicine.disease, Distributed laser light, Surgery, Hair loss, Treatment Outcome, Feasibility Studies, Laser Therapy, business, Androgenic alopecia, Hair, Research Article
Abstract

Background Various trials have been conducted on the management and treatment of androgenic alopecia (AGA) or male pattern hair loss using a variety of laser and light sources. Methods For this feasibility study, the population was composed of males between the ages of 20 and 60 years who have been experiencing active hair loss within the last 12 months and the diagnosis of AGA. They also had a Norwood-Hamilton classification of 3, 3A, 3 V, 4, 4A, or 5 for the hair thinning patterns and skin type I, II, III, or IV on the Fitzpatrick skin type scale. This two-arm randomized, parallel group study design employed stratifying randomization to balance treatment assignment within three investigational centers with at least 2 subjects enrolled in each Fitzpatrick skin type. Results A statistically significant positive trend in hair growth was observed from this pilot study, to evaluate the efficacy of the novel cold X5 hairlaser device for treating male androgenic alopecia. From the repeated measures analysis of variance, difference in mean hair counts over time was statistically significant (F = 7.70; p-value

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