Your search keyword '"Wilhelmsen Kirk C"' showing total 6 results

1. Common genetic substrates of alcohol and substance use disorder severity revealed by pleiotropy detection against GWAS catalog in two populations.

Author

Peng Q, Wilhelmsen KC, and Ehlers CL

Subjects

Adult, Alcoholism genetics, Female, Genetic Pleiotropy, Genome-Wide Association Study, Humans, Machine Learning, Male, Indians, North American genetics, Mexican Americans genetics, Substance-Related Disorders genetics

Abstract

Alcohol and other substance use disorders (AUD and SUD) are complex diseases that are postulated to have a polygenic inheritance and are often comorbid with other disorders. The comorbidities may arise partially through genetic pleiotropy. Identification of specific gene variants accounting for large parts of the variance in these disorders has yet to be accomplished. We describe a flexible strategy that takes a variant-trait association database and determines if a subset of disease/straits are potentially pleiotropic with the disorder under study. We demonstrate its usage in a study of use disorders in two independent cohorts: alcohol, stimulants, cannabis (CUD), and multi-substance use disorders (MSUD) in American Indians (AI) and AUD and CUD in Mexican Americans (MA). Using a machine learning method with variants in GWAS catalog, we identified 229 to 246 pleiotropic variants for AI and 153 to 160 for MA for each SUD. Inflammation was the most enriched for MSUD and AUD in AIs. Neurological disorder was the most significantly enriched for CUD in both cohorts, and for AUD and stimulants in AIs. Of the select pleiotropic genes shared among substances-cohorts, multiple biological pathways implicated in SUD and other psychiatric disorders were enriched, including neurotrophic factors, immune responses, extracellular matrix, and circadian regulation. Shared pleiotropic genes were significantly up-regulated in brain regions playing important roles in SUD, down-regulated in esophagus mucosa, and differentially regulated in adrenal gland. This study fills a gap for pleiotropy detection in understudied admixed populations and identifies pleiotropic variants that may be potential targets of interest for SUD., (© 2020 Society for the Study of Addiction.)

Published

2021

2. Genetic variation in FAAH is associated with cannabis use disorders in a young adult sample of Mexican Americans.

Author

Melroy-Greif WE, Wilhelmsen KC, and Ehlers CL

Subjects

Adult, Alleles, Female, Gene Frequency, Genetic Predisposition to Disease genetics, Humans, Linkage Disequilibrium genetics, Male, Phenotype, Young Adult, Amidohydrolases genetics, Marijuana Abuse ethnology, Marijuana Abuse genetics, Mexican Americans genetics, Mexican Americans psychology, Polymorphism, Single Nucleotide genetics

Abstract

Background: Cannabis is a commonly used drug and studies have shown that a significant portion of the variation in cannabis use disorders (CUDs) is heritable. Five genes known to play a role in the endocannabinoid system and CUDs were examined in a community sample of young adult Mexican Americans (MAs): CNR1, MGLL, FAAH, DAGLA, and DAGLB., Methods: Gene-based tests were run to test for association between each gene and two DSM-5 cannabis phenotypes. Subsequent linear regressions were run in PLINK using an additive model to determine which single nucleotide polymorphisms (SNPs) were driving the association., Results: FAAH was significantly associated with DSM-5 cannabis use disorder group count (DSM-5 CUD) using a gene-based test (p=0.0035). This association survived Bonferroni correction for multiple testing at p<0.004. Post hoc analyses suggested this association was driven by two common (minor allele frequency >5%) SNPs in moderate linkage disequilibrium, rs324420 and rs4141964, at p=0.0014 and p=0.0023, respectively. In both cases the minor allele increased risk for DSM-5 CUD., Conclusions: Genetic variation in FAAH was associated with DSM-5 CUD in MAs. This association was primarily driven by the missense SNP rs324420. In vitro work has provided evidence that the risk allele generates an enzyme with decreased expression and cellular stability. Although this SNP has been previously associated with substance use in the literature, this is the first association in a young adult MA sample., (Copyright © 2016 Elsevier Ireland Ltd. All rights reserved.)

Published

2016

3. Variants Near CCK Receptors are Associated With Electrophysiological Responses to Pre-pulse Startle Stimuli in a Mexican American Cohort.

Author

Norden-Krichmar TM, Gizer IR, Phillips E, Wilhelmsen KC, Schork NJ, and Ehlers CL

Subjects

Adolescent, Adult, Cohort Studies, Electrophysiological Phenomena, Female, Humans, Male, Risk Assessment, Young Adult, Mexican Americans genetics, Receptor, Cholecystokinin A genetics, Receptor, Cholecystokinin B genetics, Reflex, Startle genetics

Abstract

Neurophysiological measurements of the response to pre-pulse and startle stimuli have been suggested to represent an important endophenotype for both substance dependence and other select psychiatric disorders. We have previously shown, in young adult Mexican Americans (MA), that presentation of a short delay acoustic pre-pulse, prior to the startle stimuli can elicit a late negative component at about 400 msec (N4S), in the event-related potential (ERP), recorded from frontal cortical areas. In the present study, we investigated whether genetic factors associated with this endophenotype could be identified. The study included 420 (age 18-30 years) MA men (n = 170), and women (n = 250). DNA was genotyped using an Affymetrix Axiom Exome1A chip. An association analysis revealed that the CCKAR and CCKBR (cholecystokinin A and B receptor) genes each had a nearby variant that showed suggestive significance with the amplitude of the N4S component to pre-pulse stimuli. The neurotransmitter cholecystokinin (CCK), along with its receptors, CCKAR and CCKBR, have been previously associated with psychiatric disorders, suggesting that variants near these genes may play a role in the pre-pulse/startle response in this cohort.

Published

2015

4. Protective variant associated with alcohol dependence in a Mexican American cohort.

Author

Norden-Krichmar TM, Gizer IR, Wilhelmsen KC, Schork NJ, and Ehlers CL

Subjects

Adolescent, Adult, Alcohol Dehydrogenase genetics, Cohort Studies, Diagnostic and Statistical Manual of Mental Disorders, Female, Gene Frequency, Genome-Wide Association Study, Genotype, Genotyping Techniques, Humans, Linkage Disequilibrium, Male, Multigene Family, Phenotype, Sequence Analysis, DNA, United States, Young Adult, Alcoholism genetics, Genetic Variation, Mexican Americans genetics

Abstract

Background: Mexican Americans, particularly those born in the United States, are at greater risk for alcohol associated morbidity and mortality. The present study sought to investigate whether specific genetic variants may be associated with alcohol use disorder phenotypes in a select population of Mexican American young adults., Methods: The study evaluated a cohort of 427 (age 18 - 30 years) Mexican American men (n = 171) and women (n = 256). Information on alcohol dependence was obtained through interview using the Semi-Structured Assessment for the Genetics of Alcoholism (SSAGA). For all subjects, DNA was extracted from blood samples, followed by genotyping using an Affymetrix Axiom Exome1A chip., Results: A protective variant (rs991316) located downstream from the ADH7 (alcohol dehydrogenase 7) gene showed suggestive significance in association with alcohol dependence symptom counts derived from DSM-III-R and DSM-IV criteria, as well as to clustered alcohol dependence symptoms. Additional linkage analysis suggested that nearby variants in linkage disequilibrium with rs991316 were not responsible for the observed association with the alcohol dependence phenotypes in this study., Conclusions: ADH7 has been shown to have a protective role against alcohol dependence in previous studies involving other ethnicities, but has not been reported for Mexican Americans. These results suggest that variants near ADH7 may play a role in protection from alcohol dependence in this Mexican American cohort.

Published

2014

5. Indexing the 'dark side of addiction': substance‐induced affective symptoms and alcohol use disorders.

Author

Ehlers, Cindy L., Gilder, David A., Gizer, Ian R., and Wilhelmsen, Kirk C.

Subjects

AFFECTIVE disorders, ALEXITHYMIA, MENTAL depression, MENTAL illness, SUICIDE, PHENOTYPES, COMORBIDITY, ANXIETY disorders, RETROSPECTIVE studies, SEVERITY of illness index, DISEASE progression, ALCOHOL-induced disorders

Abstract

Background and aims: The emergence of negative affective symptoms during the course of alcohol use disorders (AUDs) (e.g. 'dark side' symptoms) has been suggested theoretically; however, the description of their occurrence is limited. This study operationalized two negative affect symptoms and tested the strength of association between these phenotypes and (1) indicators of the clinical course of the severity of AUD, (2) comorbid Axis I psychiatric disorders, suicidal behaviors and trait neuroticism and (3) whether participants reported drinking to relieve the negative affective symptoms. Design A retrospective cross‐sectional study was used to evaluate associations, using logistic regression, between the two negative affective symptoms and clinical measures of AUD severity and progression as well as comorbidity with other psychiatric disorders and conditions, adjusted for demographic characteristics. Setting: US community‐based studies. Participants: A total of 2568 individuals with AUDs obtained from larger population studies that targeted individuals of European American (n = 1663), Mexican American and American Indian (n = 905) ancestry. Measurements Semi‐Structured Assessment for the Genetics of Alcoholism was used to ascertain the two 'dark side' phenotypes, clinical diagnoses, the clinical course of AUD and associated symptoms. The two phenotypes were: (1) being anxious or depressed when trying to cut down or stop drinking and (2) experiencing disabling depression for more than 24 hours while drinking. Findings Both phenotypes were found to be rare in mild and moderate use disorder and highly prevalent in severe AUDs. Having an independent anxiety or affective disorder and elevated scores on trait neuroticism were also associated significantly with the occurrence of both symptoms, as was alcohol 'craving', elevated treatment‐seeking, suicidal behaviors and drinking to relieve the symptoms. Conclusions: Affective symptoms are common in severe alcohol use disorders are associated with a history of independent affective/anxiety disorders, neuroticism and suicidal behaviors; and may promote further heavy drinking. [ABSTRACT FROM AUTHOR]

Published

2019

6. Genome-Wide Association Study of Post-Traumatic Stress Disorder in Two High-Risk Populations.

Author

Melroy-Greif, Whitney E., Wilhelmsen, Kirk C., Yehuda, Rachel, and Ehlers, Cindy L.

Subjects

*POST-traumatic stress disorder, *MEXICAN Americans, *INDIGENOUS peoples of the Americas, *G protein coupled receptors, *HUMAN genetic variation, *OLFACTORY receptors, *GENETICS, *CELL receptors, *DISEASE susceptibility, *GENETIC polymorphisms, *HISPANIC Americans, *NATIVE Americans, *META-analysis, *RESEARCH funding, *SYMPTOMS, *SEQUENCE analysis

Abstract

Mexican Americans (MAs) and American Indians (AIs) constitute conspicuously understudied groups with respect to risk for post-traumatic stress disorder (PTSD), especially in light of findings showing racial/ethnic differences in trauma exposure and risk for PTSD. The purpose of this study was to examine genetic influences on PTSD in two minority cohorts. A genome-wide association study (GWAS) with sum PTSD symptoms for trauma-exposed subjects was run in each cohort. Six highly correlated variants in olfactory receptor family 11 subfamily L member 1 (OR11L1) were suggestively associated with PTSD in the MA cohort. These associations remained suggestively significant after permutation testing. A signal in a nearby olfactory receptor on chromosome 1, olfactory receptor family 2 subfamily L member 13 (OR2L13), tagged by rs151319968, was nominally associated with PTSD in the AI sample. Although no variants were significantly associated after correction for multiple testing in a meta-analysis of the two cohorts, pathway analysis of the top hits showed an enrichment cluster of terms related to sensory transduction, olfactory receptor activity, G-protein coupled receptors, and membrane. As previous studies have proposed a role for olfaction in PTSD, our results indicate this influence may be partially driven by genetic variation in the olfactory system. [ABSTRACT FROM PUBLISHER]

Published

2017