Mapping and verification of susceptibility loci for smoking quantity using permutation linkage analysis

Wang, D; Z, J; Li, M D

doi:10.1038/sj.tpj.6500304

Cited by 47 publications

(53 citation statements)

References 40 publications

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“…Using the criteria established by Lander and Kruglyak [87], suggestive linkage has been found for smoking initiation on chromosome 6 in a sample of Dutch twins [178]; other research has implicated chromosomes 16 and 20, but p values were below the criteria for suggestive linkage [120]. In addition, significant linkage to smoking quantity has been found in regions located on chromosomes 1 and 10-12, whereas chromosomes 3-5, 7-9, 13, 16, 17, 18, and 20 exhibit suggestive linkage to smoking quantity [92,96,95,120,165,182]. Several linkage studies have also evaluated nicotine dependence (defined using the Fagerström Test for Nicotine Dependence; FTND, or defined using the DSM-IV), and suggestive linkage for nicotine dependence has been found in regions of chromosomes 3-11, and 20 [50,96,95,98,165].…”

Section: Genome-wide Linkage Analysesmentioning

confidence: 92%

“…Four loci associated with oral nicotine consumption (located on chromosomes 1, 4, 7, and 15) were identified in F2 hybrid mice [97]. The locus found on chromosome 1 is syntenic with the human chromosome 1, and this region has also been associated with smoking quantity in humans [182]. Together, these data suggest that nAChR subunit genes play an important role in mediating sensitivity to nicotine, and reveal that some loci associated with nicotine phenotypes may be common across multiple species.…”

Section: The Effects Of Nicotine In Inbred Rodent Strainsmentioning

confidence: 99%

“…Linkage studies have evaluated several smoking phenotypes, such as smoking initiation [120,178], the number of cigarettes smoked daily (smoking quantity) [92,96,95,120,165,182], nicotine dependence [50,96,95,98,165], and withdrawal severity [165], and overall, one or more regions in nearly all chromosomes have been implicated in smoking-related behaviors. Furthermore, nAChR subunit genes have been found within some of the loci identified in linkage studies, suggesting that these genes may warrant further investigation.…”

Section: Genome-wide Linkage Analysesmentioning

confidence: 99%

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Genetic variability in nicotinic acetylcholine receptors and nicotine addiction: Converging evidence from human and animal research

Portugal

Gould

2008

Behavioural Brain Research

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Tobacco smoking is a leading preventable cause of death in the United States and produces a major health and economic burden. Although the majority of smokers want to quit, few are successful. These data highlight the need for additional research into the neurobiology of tobacco dependence. Addiction to nicotine, the main psychoactive component of tobacco, is influenced by multiple factors that include individual differences in genetic makeup. Twin studies have demonstrated that genetic factors can influence vulnerability to nicotine addiction, and subsequent research has identified genes that may alter sensitivity to nicotine. In humans, genome-wide and candidate gene association studies have demonstrated that genes encoding nicotinic acetylcholine receptor (nAChR) proteins are associated with multiple smoking phenotypes. Similarly, research in mice has provided evidence that naturally occurring variability in nAChR genes is associated with changes in nicotine sensitivity. Furthermore, the use of genetic knockout mice has allowed researchers to determine the nAChR genes that mediate the effects of nicotine, whereas research with knockin mice has demonstrated that changes to nAChR genes can dramatically alter nicotine sensitivity. This review will examine the genetic factors that alter susceptibility to nicotine addiction, with an emphasis on the genes that encode nAChR proteins.

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Section: Genome-wide Linkage Analysesmentioning

confidence: 92%

Section: The Effects Of Nicotine In Inbred Rodent Strainsmentioning

confidence: 99%

Section: Genome-wide Linkage Analysesmentioning

confidence: 99%

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Genetic variability in nicotinic acetylcholine receptors and nicotine addiction: Converging evidence from human and animal research

Portugal

Gould

2008

Behavioural Brain Research

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“…[22][23][24][25][26][27][28][29][30][31][32][33][34] Only a few of the results of these studies have converged convincingly, with the major linkage peak produced by a number of studies being poorly, if at all, supported by subsequent data (e.g., see [22][23][24][25][26] ). Indeed, assemblies of current results from at least some linkage-based genomes can produce results that cover the majority of the genome with data that derive from at least some reported linkage peak in at least one study (C Johnson, GR Uhl, unpublished observations, 2005).…”

Section: The Scope Of Current Molecular Genetic Data For Addictionsmentioning

confidence: 99%

Molecular genetics of addiction vulnerability

Uhl

2006

NeuroRX

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Summary:Classical genetic studies document strong complex genetic contributions to abuse of multiple addictive substances, to mnemonic processes that are likely to include those involved in substance dependence, and to the volumes of brain gray matter in regions that are likely to contribute to mnemonic/ cognitive and to addictive processes. The working idea that these three heritable phenotypes are likely to share some of the same complex genetic underpinnings is presented. This review contains association-based molecular genetic studies of addiction that largely derive from my laboratory and their fit with linkage data from other laboratories. These combined results now identify many of the loci and genes that contain allelic variants that are likely to provide the heritable components of human addiction vulnerability. These data are also likely to have broad implications for neurotherapeutics. Drugs with potential abuse liabilities are widely used for indications that include pain, anxiety, sleep, seizure, and attentional disorders. There is increasing nonmedical use of these prescribed substances. Increasing information about addiction vulnerability gene variants should help to improve management of risks of dependence in individuals who receive such therapeutics. In addition, since mnemonic components that correlate well with individual differences in brain regional volumes are likely to play major roles in addiction processes, many addiction vulnerability genes are also good candidates to contribute to individual differences in mnemonic processes. Recently elucidation of addiction-associated haplotypes for the "cell adhesion" Nr-CAM gene illustrate several of these points.

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“…2 A number of linkage and association studies have identified susceptibility genes for ND; 3,4 however, few association studies of candidate genes and/or linkage analyses for susceptibility loci have been replicated in independent samples. 3,5 Previously, we identified several chromosomal regions that are likely to harbor susceptibility loci for ND in the Framingham Heart Study (FSH) and Mid-South Tobacco Family (MSTF) samples, including one region on chromosome 11q13 and one on chromosome 17p13, 3,[6][7][8] where the two genes of interest, b-arrestins 1 and 2 (ARRB1 and ARRB2), are located, 9,10 respectively. b-arrestins are key negative regulators and scaffolds for G-protein-coupled receptor (GPCR) signaling, one of the most fundamental cellular signal transduction processes.…”

Section: Introductionmentioning

confidence: 99%

β-Arrestins 1 and 2 are associated with nicotine dependence in European American smokers

Sun

Payne

et al. 2007

Mol Psychiatry

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On the basis of our previous identified linkage regions for nicotine dependence (ND), we selected seven and four single nucleotide polymorphisms (SNPs) in the b-arrestins 1 (ARRB1) and 2 (ARRB2), respectively, to determine the associations of the two genes with ND in a total of 2037 subjects from 602 nuclear families of European American (EA) and African American (AA) origin. ND was assessed by Smoking Quantity (SQ), the Heaviness of Smoking Index (HSI) and the Fagerströ m Test for ND (FTND) score. Individual SNP analysis indicated that SNPs rs472112 within ARRB1 and rs4790694 within ARRB2 in the EA sample was significantly associated with HSI and FTND score, and the association of rs4790694 for ARRB2 remained significant after correction for multiple testing. Haplotype analysis revealed that haplotype C-G-C-G-G-T within ARRB1 at a frequency of 20%, formed by SNPs rs528833, rs1320709, rs480174, rs5786130, rs611908 and rs472112, was positively associated with HSI and FTND in EAs. We also found a haplotype within ARRB2, C-C-A-T at a frequency of 10.7%, formed by SNPs rs3786047, rs4522461, rs1045280 and rs4790694, that showed a significant positive association with HSI and FTND in the EA sample. No significant associations for either individual SNPs or major haplotype of both ARRB1 and ARRB2 were found in the AA sample. Further, the strength of these associations increased after removing the SQ component from HSI and FTND scores in both the EA and AA samples, suggesting that ARRB1 and ARRB2 play an important role in biological processes involved in the regulation of smoking urgency (that is time to smoke first cigarette). In summary, our results provide the first evidence of a significant association for ARRB1 and ARRB2 variants with ND in an EA sample. Molecular Psychiatry (2008) 13, 398-406; doi:10.1038/sj.mp.4002036; published online 19 June 2007Keywords: haplotype; SNP; ARRB1; ARRB2; association analysis; nicotine dependence Introduction Tobacco use is a leading preventable cause of death in the United States, with one in every five deaths attributable to smoking. 1 Nicotine is believed to be the primary addictive component of cigarette smoke. Nicotine dependence (ND) is a complex quantitative trait that is influenced by both genetic and environmental factors. 2 A number of linkage and association studies have identified susceptibility genes for ND; 3,4 however, few association studies of candidate genes and/or linkage analyses for susceptibility loci have been replicated in independent samples. 3,5 Previously, we identified several chromosomal regions that are likely to harbor susceptibility loci for ND in the Framingham Heart Study (FSH) and Mid-South Tobacco Family (MSTF) samples, including one region on chromosome 11q13 and one on chromosome 17p13, 3,[6][7][8] where the two genes of interest, b-arrestins 1 and 2 (ARRB1 and ARRB2), are located, 9,10 respectively. b-arrestins are key negative regulators and scaffolds for G-protein-coupled receptor (GPCR) signaling, one of the most fundamental cellular signal ...

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Mapping and verification of susceptibility loci for smoking quantity using permutation linkage analysis

Cited by 47 publications

References 40 publications

Genetic variability in nicotinic acetylcholine receptors and nicotine addiction: Converging evidence from human and animal research

Genetic variability in nicotinic acetylcholine receptors and nicotine addiction: Converging evidence from human and animal research

Molecular genetics of addiction vulnerability

β-Arrestins 1 and 2 are associated with nicotine dependence in European American smokers

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