Gene-Centric Analysis of Serum Cotinine Levels in African and European American Populations

Hamidovic, Ajna; Goodloe, Robert; Bergen, Andrew W.; Benowitz, Neal L.; Styn, Mindi A.; Kasberger, Jay; Choquet, Hélène; Young, Taylor; Meng, Yan; Palmer, Cameron D.; Pletcher, Mark J.; Kertesz, Stefan G.; Hitsman, Brian; Spring, Bonnie; Jorgenson, Eric

doi:10.1038/npp.2011.280

Cited by 8 publications

(6 citation statements)

References 46 publications

(47 reference statements)

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“…www.nature.com/scientificreports www.nature.com/scientificreports/ Marginally higher (i.e., trend significance) addiction severity in OUD comorbidity with MetS would support this sort of an interaction regardless of the primary index event. Of note, insulin mediates the homeostatic and reward systems' cross-talk (impairment of which might underlie the chronically relapsing nature of addictive disorders) and it has been successfully tried in nicotine 116,117 and cocaine 118 addiction. It would be of interest to test whether insulin is also able to improve metabolic and reward dysfunction in patients with OUD.…”

Section: Discussionmentioning

confidence: 99%

Metabolic and Addiction Indices in Patients on Opioid Agonist Medication-Assisted Treatment: A Comparison of Buprenorphine and Methadone

Elman

Howard²,

Borodovsky

et al. 2020

Sci Rep

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Metabolic hormones stabilize brain reward and motivational circuits, whereas excessive opioid consumption counteracts this effect and may impair metabolic function. Here we addressed the role of metabolic processes in the course of the agonist medication-assisted treatment for opioid use disorder (OUD) with buprenorphine or methadone. Plasma lipids, hemoglobin A1C, body composition, the oral glucose tolerance test (oGtt) and the Sweet taste test (Stt) were measured in buprenorphine-(n = 26) or methadone (n = 32)-treated subjects with OUD. On the whole, the subjects in both groups were overweight or obese and insulin resistant; they displayed similar oGtt and Stt performance. As compared to methadone-treated subjects, those on buprenorphine had significantly lower rates of metabolic syndrome (MetS) along with better values of the high-density lipoproteins (HDL). Subjects with-vs. without MetS tended to have greater addiction severity. correlative analyses revealed that more buprenorphine exposure duration was associated with better HDL and opioid craving values. in contrast, more methadone exposure duration was associated with worse triglycerides-, HDL-, blood pressure-, fasting glucose-and hemoglobin A1C values. Buprenorphine appears to produce beneficial HDL-and craving effects and, contrary to methadone, its role in the metabolic derangements is not obvious. our data call for further research aimed at understanding the distinctive features of buprenorphine metabolic effects vis-à-vis those of methadone and their potential role in these drugs' unique therapeutic profiles. Opioid use disorder (OUD) is an ominous public health problem afflicting about 16 million people worldwide 1. In the US, OUD constitutes the seventh cause for disability-adjusted life-years 2-4 ; including opioids' propensity 5 for the excessive body weight gain (BWG) and its medical sequelae in the form of the 'Metabolic Syndrome' (MetS) 5-7 , that is to say, a cluster of interrelated cardiometabolic risk factors comprised of insulin resistance, impaired glucose tolerance, dyslipidemia, abdominal adiposity and hypertension 8-10. Consequently, even though medication-assisted treatment (MAT) via opioid agonist replacement with long-acting opioids namely, buprenorphine and methadone, usually yields positive clinical outcomes in terms of overdose mortality, infectious diseases, crime, and societal ties 11-14 concerns have been raised about further worsening of the metabolic status 5. There are several lines of evidence that link OUD to metabolic derangements. With regard to genetic antecedents, the TCF7L2 gene codes a transcription factor implicated 15,16 in non-insulin-dependent

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Section: Discussionmentioning

confidence: 99%

Metabolic and Addiction Indices in Patients on Opioid Agonist Medication-Assisted Treatment: A Comparison of Buprenorphine and Methadone

Elman

Howard²,

Borodovsky

et al. 2020

Sci Rep

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“…Finally, we assessed statistical power to detect a priori genetic loci of interest from an example of a large-scale (1000 s) candidate gene association scan, and an example from a locus nominated by genome-wide association scans (GWAS), with genome-wide significance (GWS) as the statistical threshold. For self-identified non-Hispanic Black current smokers, we selected rs11187065 as an example, identified in the insulin-degrading enzyme gene as the gene-centric SNP most significantly associated with serum cotinine in the Coronary Artery Risk Development in Young Adults (CARDIA) study by Hamidovic et al [ 36 ]. The influence of rs11187065 on serum cotinine was substantial with a β of −85.1 ng/ml, with mean (SE) of 236.5 (8.1) ng/ml from 365 African American smokers [ 36 ].…”

Section: Resultsmentioning

confidence: 99%

“…For self-identified non-Hispanic Black current smokers, we selected rs11187065 as an example, identified in the insulin-degrading enzyme gene as the gene-centric SNP most significantly associated with serum cotinine in the Coronary Artery Risk Development in Young Adults (CARDIA) study by Hamidovic et al [ 36 ]. The influence of rs11187065 on serum cotinine was substantial with a β of −85.1 ng/ml, with mean (SE) of 236.5 (8.1) ng/ml from 365 African American smokers [ 36 ]. Mean (SD) CPD in the CARDIA sample was 10.5 (7.4), similar to that of the TES (Table 4 ).…”

Section: Resultsmentioning

confidence: 99%

Total Exposure Study Analysis consortium: a cross-sectional study of tobacco exposures

et al. 2015

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BackgroundThe Total Exposure Study was a stratified, multi-center, cross-sectional study designed to estimate levels of biomarkers of tobacco-specific and non-specific exposure and of potential harm in U.S. adult current cigarette smokers (≥one manufactured cigarette per day over the last year) and tobacco product non-users (no smoking or use of any nicotine containing products over the last 5 years). The study was designed and sponsored by a tobacco company and implemented by contract research organizations in 2002–2003. Multiple analyses of smoking behavior, demographics, and biomarkers were performed. Study data and banked biospecimens were transferred from the sponsor to the Virginia Tobacco and Health Research Repository in 2010, and then to SRI International in 2012, for independent analysis and dissemination.MethodsWe analyzed biomarker distributions overall, and by biospecimen availability, for comparison with existing studies, and to evaluate generalizability to the entire sample. We calculated genome-wide statistical power for a priori hypotheses. We performed clinical chemistries, nucleic acid extractions and genotyping, and report correlation and quality control metrics.ResultsVital signs, clinical chemistries, and laboratory measures of tobacco specific and non-specific toxicants are available from 3585 current cigarette smokers, and 1077 non-users. Peripheral blood mononuclear cells, red blood cells, plasma and 24-h urine biospecimens are available from 3073 participants (2355 smokers and 719 non-users). In multivariate analysis, participants with banked biospecimens were significantly more likely to self-identify as White, to be older, to have increased total nicotine equivalents per cigarette, decreased serum cotinine, and increased forced vital capacity, compared to participants without. Effect sizes were small (Cohen’s d-values ≤ 0.11). Power for a priori hypotheses was 57 % in non-Hispanic Black (N = 340), and 96 % in non-Hispanic White (N = 1840), smokers. All DNA samples had genotype completion rates ≥97.5 %; 68 % of RNA samples yielded RIN scores ≥6.0.ConclusionsTotal Exposure Study clinical and laboratory assessments and biospecimens comprise a unique resource for cigarette smoke health effects research. The Total Exposure Study Analysis Consortium seeks to perform molecular studies in multiple domains and will share data and analytic results in public repositories and the peer-reviewed literature. Data and banked biospecimens are available for independent or collaborative research.Electronic supplementary materialThe online version of this article (doi:10.1186/s12889-015-2212-5) contains supplementary material, which is available to authorized users.

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“…Insulin‐degrading enzyme mRNA was significantly decreased in α7 KO mice, and previous rodent studies have demonstrated that functional disruption of this gene, results in hyperinsulinemia and glucose intolerance (Fakhrai‐Rad et al ; Farris et al ). Additionally, Ide mRNA expression is altered in rats following nicotine treatment (Polesskaya et al ), whereas an allele of the Ide gene is associated with plasma cotinine levels in both European and African American smokers (Hamidovic et al ). Together with the present study, these data implicate a possible role of Ide in nicotine addiction.…”

Section: Discussionmentioning

confidence: 99%

Genetic variation within the Chrna7 gene modulates nicotine reward‐like phenotypes in mice

Harenza

Muldoon

Biasi

et al. 2013

Genes Brain and Behavior

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Mortality from tobacco smoking remains the leading cause of preventable death in the world, yet current cessation therapies are only modestly successful, suggesting new molecular targets are needed. Genetic analysis of gene expression and behavior identified Chrna7 as potentially modulating nicotine place conditioning in the BXD panel of inbred mice. We used gene targeting and pharmacological tools to confirm the role of Chrna7 in nicotine CPP. To identify molecular events downstream of Chrna7 that may modulate nicotine preference, we performed microarray analysis of α7 KO and WT nucleus accumbens tissue, followed by confirmation with quantitative PCR and immunoblotting. In the BXD panel, we found a putative cis eQTL for Chrna7 in nucleus accumbens that correlated inversely to nicotine CPP. We observed that gain-of-function α7 mice did not display nicotine preference at any dose tested, while conversely, α7 KO mice showed nicotine place preference at a dose below that routinely required to produce preference. In B6 mice, the α7 nAChR-selective agonist, PHA-543613, dose-dependently blocked nicotine CPP, which was restored using the α7 nAChR-selective antagonist, MLA. Our genomic studies implicated an mRNA co-expression network regulated by Chrna7 in nucleus accumbens. Mice lacking Chrna7 demonstrate increased insulin signaling in the nucleus accumbens, which may modulate nicotine place preference. Our studies provide novel targets for future work on development of more effective therapeutic approaches to counteract the rewarding properties of nicotine for smoking cessation.

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Gene-Centric Analysis of Serum Cotinine Levels in African and European American Populations

Cited by 8 publications

References 46 publications

Metabolic and Addiction Indices in Patients on Opioid Agonist Medication-Assisted Treatment: A Comparison of Buprenorphine and Methadone

Metabolic and Addiction Indices in Patients on Opioid Agonist Medication-Assisted Treatment: A Comparison of Buprenorphine and Methadone

Total Exposure Study Analysis consortium: a cross-sectional study of tobacco exposures

Genetic variation within the Chrna7 gene modulates nicotine reward‐like phenotypes in mice

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