Expanding the Genetic Architecture of Nicotine Dependence and its Shared Genetics with Multiple Traits: Findings from the Nicotine Dependence GenOmics (iNDiGO) Consortium

Quach, Bryan C.; Bray, Michael J.; Gaddis, Nathan; Liu, Mengzhen; Palviainen, Teemu; Minică, Camelia C.; Zellers, Stephanie; Sherva, Richard; Alıev, Fazil; Nothnagel, Michael; Young, Kendra A.; Marks, Jesse; Young, Hannah; Guo, Yuelong; Waldrop, Alex; Sey, Nancy Y A; Landi, Maria T.; McNeil, Daniel W.; Farrer, Lindsay A.; Markunas, Christina A.; Vink, Jacqueline M.; Hottenga, Jouke Jan; Iacono, William G.; Kranzler, Henry R.; Saccone, Nancy L.; Neale, Michael C.; Madden, Pamela A. F.; Rietschel, Marcella; Marazita, Mary L.; McGue, Matthew; Won, Hyejung; Winterer, Georg; Grucza, Richard A.; Dick, Danielle M.; Gelernter, Joel; Caporaso, Neil E.; Baker, Timothy B.; Boomsma, Dorret I.; Kaprio, Jaakko; Hokanson, John E.; Vrieze, Scott; Bierut, Laura J.; Johnson, Eric O.; Hancock, Dana B.

doi:10.1101/2020.01.15.898858

Cited by 10 publications

(8 citation statements)

References 92 publications

(123 reference statements)

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“…In this case, though lacking other important aspects of the clinical presentation such as craving or loss of control, the dichotomized heavy/light phenotype is comparing individuals who may find overnight abstinence less aversive and start smoking later in the day, and endorse lower levels of nicotine dependence (light) to those who meet criteria for severe nicotine dependence (heavy), whereas the standard continuous CPD encoding includes intermediate levels of smoking heaviness that may or may not correlate with clinical presentations of nicotine dependence. Our GREML-based estimate of common, well-tagged h 2 SNP (∼0.09) is approximately the same as one recently reported LDSC-based estimate of nicotine dependence(15), consistent with this hypothesis.…”

Section: Discussionsupporting

confidence: 90%

“…While additional common variants of very small effect are likely to be identified as sample sizes grow, some of the unexplained variability undoubtedly arises from uncommon and rare variants (MAF<0.01), though their relative contribution is uncertain. The most recent large GWASs(11, 15) of smoking behaviors and nicotine dependence, using LD score regression (LDSC), estimate the SNP-based heritability ( h 2 SNP ) due to common variants as 0.05-0.09 across traits(16). A related exome sequencing study(17) estimated that rare coding variants explained approximately 1-2% of the phenotypic variance.…”

Section: Introductionmentioning

confidence: 99%

“…Furthermore, the allele frequency spectrum and contribution of functional annotations related to LD, allele frequency, recombination and related genomic features for smoking behaviors has not been fully explored. One study applied partitioned h 2 SNP approaches to evaluate tissue-specific effects, with results indicating that genes expressed in the cerebellum are enriched in their contribution to nicotine dependence(15). The only published work has examined a single trait, smoking status, finding contributions of low-LD and -MAF variants consistent with negative or purifying selection(20, 21).…”

Section: Introductionmentioning

confidence: 99%

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Genetic architecture of four smoking behaviors using partitioned h²_SNP

Evans

Jang

Ehringer

et al. 2020

Preprint

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Background and Aims: Smoking is a leading cause of premature death. Although genome-wide association studies have identified many loci that influence smoking behaviors, much of the genetic variance in these traits remains unexplained. We sought to characterize the genetic architecture of four smoking behaviors through SNP-based heritability (h2SNP) analyses. Design: We applied recently-developed partitioned h2SNP approaches to smoking behavior traits assessed in the UK Biobank. Setting: UK Biobank. Participants: UK Biobank participants of European ancestry. The number of participants varied depending on the trait, from 54,792 to 323,068. Measurements: Smoking initiation, age of initiation, cigarettes per day (CPD; count, log-transformed, binned, and dichotomized into heavy versus light), and smoking cessation. Imputed genome-wide SNPs. Findings: We estimated h2SNP(SE)=0.18(0.01) for smoking initiation and 0.12(0.02) for smoking cessation, which were more than twice the previously reported estimates. Estimated age of initiation h2SNP=0.05(0.01) and binned CPD h2SNP=0.1(0.01) were similar to previous reports. These estimates remained substantially below published twin-based h2 of roughly 50%. CPD encoding strongly influenced estimates, with dichotomized CPD h2SNP=0.28. We found significant contributions of low-frequency variants and variants in low linkage-disequilibrium (LD) with surrounding genomic regions. Functional annotations related to LD, allele frequency, sequence conservation, and selective constraint also contributed significantly to the partitioned heritability. We found no evidence of dominance genetic variance for any trait. Conclusion: h2SNP of these four specific smoking behaviors is modest overall. The patterns of partitioned h2SNP for these highly polygenic traits is consistent with negative selection. We found a predominant contribution of common variants, and our results suggest a role of low-frequency or rare variants, poorly tagged by surrounding regions. Deep sequencing of large samples and/or improved imputation will be required to fully assess the role of rare variants.

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Section: Discussionsupporting

confidence: 90%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Genetic architecture of four smoking behaviors using partitioned h²_SNP

Evans

Jang

Ehringer

et al. 2020

Preprint

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“…One useful application of PGSs is the ability to draw the boundaries of genetic influences on psychiatric disorders. For example, there is significant overlap among PGSs for schizophrenia, bipolar, autism spectrum disorder, attention-deficit/hyperactivity disorder (ADHD), and major depression (Cross-Disorder Group of the Psychiatric Genomics Consortium, 2013a, 2013b) and among alcohol, nicotine, and cannabis use (Liu et al, 2019;Quach et al, 2020;Zhou et al, 2019), and there is some evidence of genetic specificity (Byrne et al, 2021). Relatedly, childhood symptoms are associated with PGSs for adult disorders, indicating that these genetic influences contribute to the expression of psychiatric problems early in life.…”

mentioning

confidence: 99%

Polygenic Score for Smoking Is Associated With Externalizing Psychopathology and Disinhibited Personality Traits but Not Internalizing Psychopathology in Adolescence

Hicks

Clark

Deak

et al. 2021

Clinical Psychological Science

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We examined whether a polygenic score (PGS) for smoking measured genetic risk for general behavioral disinhibition by estimating its associations with externalizing and internalizing psychopathology and related personality traits at multiple time points in adolescence (ages 11, 14, and 17 years; N = 3,225). The smoking PGS had strong associations with the stable variance across time for all the externalizing measures (mean standardized β = 0.27), agreeableness (β = −0.22, 95% confidence interval [CI] = [−0.28, −0.16]), and conscientiousness (β = −0.19, 95% CI = [−0.24, −0.13]) but was not significantly associated with internalizing measures (mean β = 0.06) or extraversion (β = 0.01, 95% CI = [−0.05, 0.07]). After controlling for smoking at age 17 years, the associations with externalizing, low agreeableness, and low conscientiousness remained statistically significant. The smoking PGS measures genetic influences that contribute to a spectrum of phenotypes related to behavioral disinhibition, including externalizing psychopathology and normal-range personality traits related to behavioral control but not internalizing psychopathology.

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“…Other variants may affect common pathways, such as variants associating with two or more classes of psychoactive substances (e.g. BDNF 7,19,20 , PDE4B 7,20,21 or DRD2 7,15,18,20,22 ) or behavioural phenotypes (e.g., the top variant identified for cannabis use disorder, which also associates with ADHD and risk-taking 23 ).…”

Section: Introductionmentioning

confidence: 99%

Novel insights into the common heritable liability to addiction: a multivariate genome-wide association study

Schoeler

Baldwin

Allegrini

et al. 2021

Preprint

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Addiction to nicotine, alcohol and cannabis commonly co-occurs, which is thought to partly stem from a common heritable liability. To elucidate its genetic architecture, we modelled the common liability to addiction, inferred from genetic correlations among six measures of dependence and frequency of use of nicotine, alcohol and cannabis. Forty-two genetic variants were identified in the multivariate genome-wide association study on the common liability to addiction, of which 67% were novel and not associated with the six phenotypes. Mapped genes highlighted the role of dopamine (e.g., dopamine D2 gene), and showed enrichment for several components of the central nervous systems (e.g., mesocorticolimbic brain regions) and molecular pathways (dopaminergic, glutamatergic, GABAergic) that are thought to modulate drug reinforcement. Genetic correlations with other traits were most prominent for reward-related behaviours (e.g., risk-taking, cocaine and heroin use) and mood (e.g., depression, insomnia). These genome-wide results triangulate and expand previous preclinical and human studies focusing on the neurobiological substrates of addiction, and help to elucidate the common genetic architecture underlying addiction.

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Expanding the Genetic Architecture of Nicotine Dependence and its Shared Genetics with Multiple Traits: Findings from the Nicotine Dependence GenOmics (iNDiGO) Consortium

Cited by 10 publications

References 92 publications

Genetic architecture of four smoking behaviors using partitioned h²_SNP

Genetic architecture of four smoking behaviors using partitioned h²_SNP

Polygenic Score for Smoking Is Associated With Externalizing Psychopathology and Disinhibited Personality Traits but Not Internalizing Psychopathology in Adolescence

Novel insights into the common heritable liability to addiction: a multivariate genome-wide association study

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Expanding the Genetic Architecture of Nicotine Dependence and its Shared Genetics with Multiple Traits: Findings from the Nicotine Dependence GenOmics (iNDiGO) Consortium

Cited by 10 publications

References 92 publications

Genetic architecture of four smoking behaviors using partitioned h2SNP

Genetic architecture of four smoking behaviors using partitioned h2SNP

Polygenic Score for Smoking Is Associated With Externalizing Psychopathology and Disinhibited Personality Traits but Not Internalizing Psychopathology in Adolescence

Novel insights into the common heritable liability to addiction: a multivariate genome-wide association study

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Resources

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Genetic architecture of four smoking behaviors using partitioned h²_SNP

Genetic architecture of four smoking behaviors using partitioned h²_SNP