Genome-Wide Association Study of Alcohol Dependence Implicates KIAA0040 on Chromosome 1q

Zuo, Lingjun; Gelernter, Joel; Zhang, Clarence K.; Zhao, Hongyu; Lu, Lingeng; Kranzler, Henry R.; Malison, Robert T.; Li, Chiang‐Shan R.; Wang, Fei; Zhang, Xiang Yang; Deng, Hong−Wen; Krystal, John H.; Zhang, Fengyu; Luο, Xingguang

doi:10.1038/npp.2011.229

Cited by 105 publications

(139 citation statements)

References 29 publications

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“…Another voltage gated K + channel identified through GWAS explora tion was KCND2 that encodes for the K V 4.2 channel that regulate rapidly inactivating Atype K + current (I A ). A SNP in KCND2 was found in the top ten SNPs associated with alcohol and nicotine dependence and alcohol dependence alone [104][105][106]. And finally, an SNP in the KCNMA1 gene, which encodes the α1 subunit of K Ca 1.1 was significantly associated with the develop ment of alcohol dependence [89,90] and subjective response to alcohol [107].…”

Section: Preclinical Pharamcogenetic Targets For Treating Alcohol Addmentioning

confidence: 97%

Promising Pharmacogenetic Targets for Treating Alcohol Use Disorder: Evidence from Preclinical Models

Rinker

Mulholland

2017

Pharmacogenomics

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Inherited genetic variants contribute to risk factors for developing an alcohol use disorder, and polymorphisms may inform precision medicine strategies for treating alcohol addiction. Targeting genetic mutations linked to alcohol phenotypes has provided promising initial evidence for reducing relapse rates in alcoholics. Although successful in some studies, there are conflicting findings and the reports of adverse effects may ultimately limit their clinical utility, suggesting that novel pharmacogenetic targets are necessary to advance precision medicine approaches. Here, we describe promising novel genetic variants derived from preclinical models of alcohol consumption and dependence that may uncover disease mechanisms that drive uncontrolled drinking and identify novel pharmacogenetic targets that facilitate therapeutic intervention for the treatment of alcohol use disorder. Alcohol use disorder (AUD) is a chronic neurological disorder characterized by an inability to regulate alcohol intake despite a host of serious and harmful health, soci etal and personal consequences [1]. The cur rent pharmacotherapies available for AUD treatment have been met with variable out comes that are modest at best and thus have not been widely embraced by the medical community. This gap in treatment options provides an opportunity to explore new avenues toward identifying novel pharmaco therapeutic targets. As with other addictive disorders, AUD is influenced, to a consid erable degree, by genetics, with heritability estimates upward of 60% [2,3]. Despite the comparatively large influence of genetics, the exact etiology of AUD is by no means simple or straightforward, which under scores the difficulty in effective treatment of this disorder. In this review, we provide an evaluation of our understanding of the genet ics of AUD in relation to current precision medicine approaches. Demonstrating the considerable heterogeneity that exists within the AUD population and understanding the contribution of genetic variation to treatment response provides a framework for promot ing a pharmacogenetic approach. Moreover, understanding the genetic variation among individuals with AUD in treatment response will provide valuable information that will allow for personalized treatment plans.A diagnosis of AUD is based strictly on a set of clinical diagnostic criteria, because as of yet, there are no reliable biomarkers to identify AUD or subpopulations that might be more or less responsive to certain medica tions. This means that, at best, we are treat ing AUD by trial and error on a, presumably, largely heterogeneous population. There are currently only three US FDA approved pharmaco therapies for treating AUD, nal trexone, acamprosate and disulfiram, all of

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Section: Preclinical Pharamcogenetic Targets For Treating Alcohol Addmentioning

confidence: 97%

Promising Pharmacogenetic Targets for Treating Alcohol Use Disorder: Evidence from Preclinical Models

Rinker

Mulholland

2017

Pharmacogenomics

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“…Interestingly, the NKAIN1 gene at 1p35.2, which encodes the member protein NKAIN1 from the same family as NKAIN2, is closely located to the serine incorporator 2 gene ( SERINC2 ) that was a top-ranked risk gene (p=2.3×10 −7 ) for alcohol dependence reported by one of our recent GWASs [9]. In the present study, we comprehensively examined the rare variants [minor allele frequency (MAF) < 0.05] in the NKAIN1-SERINC2 region, in order to confirm our previous GWAS finding that was based on common variant analysis (MAF > 0.05).…”

Section: Introductionmentioning

confidence: 99%

Rare SERINC2 variants are specific for alcohol dependence in individuals of European descent

Zuo

Wang

Zhang

et al. 2013

Pharmacogenetics and Genomics

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Objectives We previously reported a top-ranked risk gene [i.e., serine incorporator 2 gene (SERINC2)] for alcohol dependence in the subjects of European descent by analyzing the common variants in a genome-wide association study. In the present study, we comprehensively examined the rare variants [minor allele frequency (MAF) < 0.05] in the NKAIN1-SERINC2 region, in order to confirm our previous finding. Methods A discovery sample (1,409 European-American cases with alcohol dependence and 1,518 European-American controls) and a replication sample (6,438 European-Australian family subjects with 1,645 alcohol dependent probands) underwent association analysis. A total of 39,903 subjects from 19 other cohorts with 11 different neuropsychiatric and neurological disorders served as contrast groups. The entire NKAIN1-SERINC2 region was imputed in all cohorts using the same reference panels of genotypes that included rare variants from the whole-genome sequencing data. We stringently cleaned the phenotype and genotype data, and obtained a total of about 220 SNPs in the subjects with European descent and about 450 SNPs in the subjects with African descent with 0

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“…Alkol ve nikotin komorbiditesi için "MAP/microtubule affinity regulating kinase 1" (MARK1) yakınındaki rs753030, "DEAD box helicase 6" (DDX6) yakınıdaki rs1784300 ve KIAA1409'daki rs12882384 polimorfizmleri genom çapı anlamlı olarak bulunmuştur (68). Benzer bir şekilde "SH3 domain binding protein" (5SH3BP5), "nuclear receptor subfamily 2 group C member 2" (NR2C2), "Plasminogen-like B2" (PLGLB2)'deki SNP'ler ve kromozom 5q'da bulunan IPO11-HRT1A bölgesindeki rs7445832 alkol ve nikotin birlikte bağımlılığı ile ilişkili bulunmuştur (71,77). 12 populasyon temelli örneklemden 26.316 kişinin dahil edildiği bir çalışmada AUT2 rs6943555 alkol tüketimi ile genom boyu anlamlı bulunmuştur (78).…”

Section: Genom Boyu Bağlantı çAlışmaları [Genome Wide Association Stuunclassified

Genetics of Alcohol Use Disorder

Kaya¹,

Kaya²,

Dılbaz³

2017

CAR

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Genome-Wide Association Study of Alcohol Dependence Implicates KIAA0040 on Chromosome 1q

Cited by 105 publications

References 29 publications

Promising Pharmacogenetic Targets for Treating Alcohol Use Disorder: Evidence from Preclinical Models

Promising Pharmacogenetic Targets for Treating Alcohol Use Disorder: Evidence from Preclinical Models

Rare SERINC2 variants are specific for alcohol dependence in individuals of European descent

Genetics of Alcohol Use Disorder

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