Genome-wide scan and fine-mapping of rare nonsynonymous associations implicates intracellular lipolysis genes in fat distribution and cardio-metabolic risk

AbstractDifficulties in identifying causal variants and genes underlying genetic associations have limited the translational potential of genetic studies of body fat distribution, an important, partly-heritable risk factor for cardio-metabolic disease. Rare variant associations facilitate fine-mapping of causal alleles, but their contribution to fat distribution is understudied. We performed a genome-wide scan of rare nonsynonymous variants for body mass index-adjusted waist-to-hip-ratio (BMI-adjusted WHR; a widely-used measure of fat distribution) in 450,562 European ancestry individuals, followed by systematic Bayesian fine-mapping at six genome-wide (p<5×10−08; main-analysis) and two subthreshold signals (significant at a Bonferroni-corrected p<1.3×10−06). We found strong statistical evidence of causal association for nonsynonymous alleles in CALCRL (p.L87P, pconditional=5.9×10−12; posterior-probability of association [PPA]=52%), PLIN1 (p.L90P, pconditional=5.5×10−13; PPA>99%), PDE3B (p.R783X, pconditional=6.2×10−15; PPA>99%), ACVR1C (p.I195T; pconditional=5.4×10−12; PPA>99%), and FGF1 (p.G21E, pconditional=1.6×10−07; PPA=98%). Alleles at the four likely-causal main-analysis genes affected fat distribution primarily via larger hip-rather than smaller waist-circumference and six of nine conditionally-independent WHR-lowering index-variants were associated with protection from cardiovascular or metabolic disease. All four genes are expressed in adipose tissue and have been linked with the regulation of intracellular lipolysis, which controls fat retention in mature cells. Targeted follow-up analyses of key intracellular-lipolysis genes revealed associations for a variant in the initiator of intracellular lipolysis PNPLA2 (p.N252K) with higher BMI-adjusted-WHR and higher cardio-metabolic risk. This study provides human genetic evidence of a link between intracellular lipolysis, fat-distribution and its cardio-metabolic complications in the general population.

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Meta-analysis of genome-wide association studies for body fat distribution in 694 649 individuals of European ancestry

Human Molecular Genetics ◽

10.1093/hmg/ddy327 ◽

2018 ◽

Vol 28 (1) ◽

pp. 166-174 ◽

Cited By ~ 109

Author(s):

Sara L Pulit ◽

Charli Stoneman ◽

Andrew P Morris ◽

Andrew R Wood ◽

Craig A Glastonbury ◽

...

Keyword(s):

Body Fat ◽

Association Studies ◽

Meta Analysis ◽

Fat Distribution ◽

Body Fat Distribution ◽

Genome Wide Association ◽

European Ancestry ◽

Genome Wide Association Studies ◽

Genome Wide ◽

A Genome

Abstract More than one in three adults worldwide is either overweight or obese. Epidemiological studies indicate that the location and distribution of excess fat, rather than general adiposity, are more informative for predicting risk of obesity sequelae, including cardiometabolic disease and cancer. We performed a genome-wide association study meta-analysis of body fat distribution, measured by waist-to-hip ratio (WHR) adjusted for body mass index (WHRadjBMI), and identified 463 signals in 346 loci. Heritability and variant effects were generally stronger in women than men, and we found approximately one-third of all signals to be sexually dimorphic. The 5% of individuals carrying the most WHRadjBMI-increasing alleles were 1.62 times more likely than the bottom 5% to have a WHR above the thresholds used for metabolic syndrome. These data, made publicly available, will inform the biology of body fat distribution and its relationship with disease.

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Genetic associations and architecture of asthma-chronic obstructive pulmonary disease overlap

10.1101/2020.11.26.20236760 ◽

2020 ◽

Author(s):

C. John ◽

A.L. Guyatt ◽

N. Shrine ◽

R. Packer ◽

T.A. Olafsdottir ◽

...

Keyword(s):

Genome Wide Association Study ◽

Meta Analysis ◽

European Ancestry ◽

Chronic Obstructive ◽

Genetic Associations ◽

Obstructive Pulmonary Disease ◽

Genome Wide ◽

A Genome ◽

Stage 1

AbstractSome individuals have characteristics of both asthma and COPD (asthma-COPD overlap, ACO), and evidence suggests they experience worse outcomes than those with either condition alone. Improved knowledge of the genetic architecture would contribute to understanding whether determinants of risk in this group differ from those in COPD or asthma.We conducted a genome-wide association study in 8,068 cases and 40,360 controls of European ancestry from UK Biobank (stage 1). After excluding variants only associated with asthma or COPD we selected 31 variants for further investigation in 12 additional cohorts (stage 2), and discovered eight novel signals for ACO in a meta-analysis of stage 1 and 2 studies.Our signals include an intergenic signal on chromosome 5 not previously associated with asthma, COPD or lung function, and suggest a spectrum of shared and distinct genetic influences in asthma, COPD and ACO. A number of signals may represent loci that predispose to serious long-term consequences in people with asthma.

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Meta-analysis of genome-wide association studies for body fat distribution in 694,649 individuals of European ancestry

10.1101/304030 ◽

2018 ◽

Cited By ~ 1

Author(s):

Sara L. Pulit ◽

Charli Stoneman ◽

Andrew P. Morris ◽

Andrew R. Wood ◽

Craig A. Glastonbury ◽

...

Keyword(s):

Body Fat ◽

Association Studies ◽

Meta Analysis ◽

Fat Distribution ◽

Body Fat Distribution ◽

Genome Wide Association ◽

European Ancestry ◽

Genome Wide Association Studies ◽

Genome Wide ◽

A Genome

AbstractOne in four adults worldwide are either overweight or obese. Epidemiological studies indicate that the location and distribution of excess fat, rather than general adiposity, is most informative for predicting risk of obesity sequellae, including cardiometabolic disease and cancer. We performed a genome-wide association study meta-analysis of body fat distribution, measured by waist-to-hip ratio adjusted for BMI (WHRadjBMI), and identified 463 signals in 346 loci. Heritability and variant effects were generally stronger in women than men, and we found approximately one-third of all signals to be sexually dimorphic. The 5% of individuals carrying the most WHRadjBMI-increasing alleles were 1.62 times more likely than the bottom 5% to have a WHR above the thresholds used for metabolic syndrome. These data, made publicly available, will inform the biology of body fat distribution and its relationship with disease.

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A genome-wide linkage scan for familial partial lipodystrophy susceptibility genes in a German kindreds

Clinical & Investigative Medicine ◽

10.25011/cim.v30i4.2861 ◽

2007 ◽

Vol 30 (4) ◽

pp. 86

Author(s):

M. Lanktree ◽

J. Robinson ◽

J. Creider ◽

H. Cao ◽

D. Carter ◽

...

Keyword(s):

Subcutaneous Fat ◽

Visceral Obesity ◽

Fat Distribution ◽

Dominant Negative ◽

Molecular Forms ◽

Partial Lipodystrophy ◽

Genome Wide ◽

A Genome ◽

Familial Partial Lipodystrophy ◽

Promoter Mutations

Background: In Dunnigan-type familial partial lipodystrophy (FPLD) patients are born with normal fat distribution, but subcutaneous fat from extremities and gluteal regions are lost during puberty. The abnormal fat distribution leads to the development of metabolic syndrome (MetS), a cluster of phenotypes including hyperglycemia, dyslipidemia, hypertension, and visceral obesity. The study of FPLD as a monogenic model of MetS may uncover genetic risk factors of the common MetS which affects ~30% of adult North Americans. Two molecular forms of FPLD have been identified including FPLD2, resulting from heterozygous mutations in the LMNA gene, and FPLD3, resulting from both heterozygous dominant negative and haploinsufficiency mutations in the PPARG gene. However, many patients with clinically diagnosed FPLD have no mutation in either LMNA or PPARG, suggesting the involvement of additional genes in FPLD etiology. Methods: Here, we report the results of an Affymetrix 10K GeneChip microarray genome-wide linkage analysis study of a German kindred displaying the FPLD phenotype and no known lipodystrophy-causing mutations. Results: The investigation identified three chromosomal loci, namely 1q, 3p, and 9q, with non-parametric logarithm of odds (NPL) scores >2.7. While not meeting the criteria for genome-wide significance, it is interesting to note that the 1q and 3p peaks contain the LMNA and PPARG genes respectively. Conclusions: Three possible conclusions can be drawn from these results: 1) the peaks identified are spurious findings, 2) additional genes physically close to LMNA, PPARG, or within 9q, are involved in FPLD etiology, or 3) alternative disease causing mechanisms not identified by standard exon sequencing approaches, such as promoter mutations, alternative splicing, or epigenetics, are also responsible for FPLD.

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Age by Single Nucleotide Polymorphism Interactions on Bronchodilator Response in Asthmatics

Journal of Personalized Medicine ◽

10.3390/jpm11010059 ◽

2021 ◽

Vol 11 (1) ◽

pp. 59

Author(s):

Kirsten Voorhies ◽

Joanne E. Sordillo ◽

Michael McGeachie ◽

Elizabeth Ampleford ◽

Alberta L. Wang ◽

...

Keyword(s):

Candidate Genes ◽

P Value ◽

Genome Wide Association Studies ◽

Genetic Associations ◽

Single Nucleotide ◽

Significance Level ◽

Bronchodilator Response ◽

Genome Wide ◽

A Genome ◽

Β2 Agonists

An unaddressed and important issue is the role age plays in modulating response to short acting β2-agonists in individuals with asthma. The objective of this study was to identify whether age modifies genetic associations of single nucleotide polymorphisms (SNPs) with bronchodilator response (BDR) to β2-agonists. Using three cohorts with a total of 892 subjects, we ran a genome wide interaction study (GWIS) for each cohort to examine SNP by age interactions with BDR. A fixed effect meta-analysis was used to combine the results. In order to determine if previously identified BDR SNPs had an age interaction, we also examined 16 polymorphisms in candidate genes from two published genome wide association studies (GWAS) of BDR. There were no significant SNP by age interactions on BDR using the genome wide significance level of 5 × 10−8. Using a suggestive significance level of 5 × 10−6, three interactions, including one for a SNP within PRAG1 (rs4840337), were significant and replicated at the significance level of 0.05. Considering candidate genes from two previous GWAS of BDR, three SNPs (rs10476900 (near ADRB2) [p-value = 0.009], rs10827492 (CREM) [p-value = 0.02], and rs72646209 (NCOA3) [p-value = 0.02]) had a marginally significant interaction with age on BDR (p < 0.05). Our results suggest age may be an important modifier of genetic associations for BDR in asthma.

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A genome-wide scan identifies mutations in the gene encoding phosphodiesterase 11A4 (PDE11A) in individuals with adrenocortical hyperplasia

Nature Genetics ◽

10.1038/ng1809 ◽

2006 ◽

Vol 38 (7) ◽

pp. 794-800 ◽

Cited By ~ 205

Author(s):

Anelia Horvath ◽

Sosipatros Boikos ◽

Christoforos Giatzakis ◽

Audrey Robinson-White ◽

Lionel Groussin ◽

...

Keyword(s):

Gene Encoding ◽

Genome Wide ◽

A Genome ◽

Adrenocortical Hyperplasia ◽

Genome Wide Scan

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A Genome-Wide Scan for Evidence of Selection in a Maize Population Under Long-Term Artificial Selection for Ear Number

Genetics ◽

10.1534/genetics.113.160655 ◽

2013 ◽

Vol 196 (3) ◽

pp. 829-840 ◽

Cited By ~ 47

Author(s):

Timothy M. Beissinger ◽

Candice N. Hirsch ◽

Brieanne Vaillancourt ◽

Shweta Deshpande ◽

Kerrie Barry ◽

...

Keyword(s):

Artificial Selection ◽

Maize Population ◽

Genome Wide ◽

A Genome ◽

Selection For ◽

Ear Number ◽

Genome Wide Scan

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Assessing linkage of monoamine oxidase B in a genome-wide scan using a univariate variance components approach

Genetic Epidemiology ◽

10.1002/gepi.1370170709 ◽

1999 ◽

Vol 17 (S1) ◽

pp. S49-S54 ◽

Cited By ~ 9

Author(s):

J.S. Barnholtz ◽

M. de Andrade ◽

G.P. Page ◽

T.M. King ◽

L.E. Peterson ◽

...

Keyword(s):

Monoamine Oxidase ◽

Variance Components ◽

Monoamine Oxidase B ◽

Genome Wide ◽

A Genome ◽

Genome Wide Scan

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Abstract P359: A Sickle Cell Variant Associates With Urine Albumin Excretion in Genome Wide Association Study of Hispanics: The HCHS/SOL Study

Circulation ◽

10.1161/circ.131.suppl_1.p359 ◽

2015 ◽

Vol 131 (suppl_1) ◽

Author(s):

Nora Franceschini ◽

Adrienne Stilp ◽

Christina L Wassel ◽

Holly J Mattix-Kramer ◽

Michael F Flessner ◽

...

Keyword(s):

Allele Frequency ◽

Sickle Cell ◽

Missense Variant ◽

Genome Wide Association ◽

European Ancestry ◽

Minority Population ◽

Genome Wide Association Studies ◽

Urine Albumin ◽

Genome Wide ◽

A Genome

Introduction: Genome wide association studies have identified genetic variants in the Cubillin gene ( CUBN ) that explain inter-individual variation in urine albumin-to-creatinine excretion (UACR) in populations. These studies have not included Hispanics/Latinos, the fast growing minority population in the U.S., who has also high prevalence of chronic kidney disease and its risk factors. Hypothesis: By leveraging on population admixture of Hispanics and using a genome wide association approach, we hypothesized that novel loci associated with UACR would be identified. Methods: We used data from 12,212 self-identified Hispanic individuals recruited in a community-based study, aged 18-74 years at screening (2008-2011), and randomly selected from households in four U.S. field centers (Chicago, IL; Miami, FL; Bronx, NY; San Diego, CA). Urine albumin (mg/dl) and creatinine (g/dl) were measured at the baseline exam. UACR was log-transformed for analysis. Individuals were excluded if reporting to have end-stage renal disease. Genotyping was performed using a custom Illumina Omni2.5M array. Imputation of variants was performed using 1000 Genome Project data from cosmopolitan HapMap samples. After quality control of imputed data, we performed mixed linear regression analyses that accounted for the sampling strategy and family relatedness, for variants with minor allele frequency (MAF) > 0.01 and imputation quality > 0.3. We used additive genetic models and adjusted for age, sex, and principal components which were estimated from the data. In a secondary analysis, we also examine the association of significant variants with kidney function using estimated glomerular filtration rate (eGFR) equations. Results: Among 12,212 participants, 41% were men, and mean age was 46 (SD =13). There was little evidence for genome wide inflation (lambda =1.024). We identified significant associations of single nucleotide polymorphisms (SNPs) with UACR at two loci: CUBN and HBB . The CUBN SNP (chr10:16966414, p=2.1x10-8) is an indel variant with MAF of 0.14, which was not in linkage disequilibrium with previously reported SNP rs1801239 (rsq=0.38, p=1.3x10-4) identified in individuals of European ancestry. The HBB SNP is a missense variant which results in an E [Glu] ⇒ A [Ala] substitution in the beta-globin chain of hemoglobin and a cause of the Mendelian disorder sickle cell anemia (rs334, T allele frequency =0.01, beta=0.44, SE=0.06, p=7.6x10-12). rs344 was not associated with eGFR in our data (p>0.05). Conclusion: This study identified a novel association of a sickle cell missense variant with UACR in Hispanics, and provided evidence for allelic heterogeneity at the CUBN locus. Our findings suggest a role for Mendelian gene variants in increased albuminuria in Hispanic populations with admixture.

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Abstract P629: Genome-Wide Association Study of Individuals of Native Hawaiian Ancestry Reveals Unique Genetic Risk Factors for Stroke and Myocardial Infarction

Stroke ◽

10.1161/str.52.suppl_1.p629 ◽

2021 ◽

Vol 52 (Suppl_1) ◽

Author(s):

Stacy C Brown ◽

Cameron Both ◽

Julian N Acosta ◽

Natalia Szejko ◽

Victor Torres ◽

...

Keyword(s):

Myocardial Infarction ◽

Ischemic Stroke ◽

Association Study ◽

Genome Wide Association Study ◽

Native Hawaiian ◽

European Ancestry ◽

Intronic Region ◽

Genome Wide ◽

A Genome ◽

Risk Locus

Background: Several genetic susceptibility risk loci for ischemic stroke have been identified. However, the relative dearth of genetic data from populations of non-European ancestry has the potential to create disparities in access to genomics-based precision medicine strategies. Individuals of Native Hawaiian ancestry represent a particularly understudied group in stroke genomics research despite facing high rates of cerebrovascular disease. Hypothesis: Genetic variants associated with stroke differ between Native Hawaiians and previously studied groups of predominantly European ancestry. Methods: We conducted a genome-wide (GW) association study of stroke and myocardial infarction (MI) in an adult population of Native Hawaiian ancestry, using data from the Multiethnic Cohort study (MEC). Genetic information was ascertained via genome-wide array genotyping using the AB OpenArray and TaqMan platforms followed by imputation to 1000 Genomes reference panels. We pursued replication of variants that were GW significant (p<5x10 -8 ) or yielded suggestive associations (p<5x10 -7 ) in the prior stroke GW association study MEGASTROKE. Results: We identified 2,104 individuals (1,089 [51.8%] female) of Native Hawaiian ancestry, including 173 cases and 1,931 controls. We identified one novel susceptibility risk locus at a narrow intronic region located at chromosome q26.2 (top associated SNP 3:169096251, OR 2.48, 95%CI 1.81-3.41; p=1.93x10 -8 ), overlying the MECOM gene. We also identified 9 other suggestive risk loci at p<5x10 -7 . When replicating in MEGASTROKE, q26.2 did not have available counterpart variants to analyze, and 3 out of 9 suggestive signals were associated with ischemic stroke subtypes at p<0.05. Conclusions: We report the first GW association study of ischemic stroke and myocardial infarction in a Native Hawaiian population. We identified one susceptibility risk locus at q26.2, located in a narrow intronic region of MECOM, a gene that codes for a histone-lysine N-methyltransferase that has transcriptional regulation and oncoprotein functions. The lack of available replication data for this locus in the large MEGASTROKE collaboration emphasizes the importance of developing genomic resources across ancestral groups.

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