Segregation Analysis of Serum Uric Acid in the NHLBI Family Heart Study

Overview

Journal Hum Genet

Specialty Genetics

Date 2000 May 8

PMID 10798367

Citations 44

Authors

J B Wilk

L Djousse

I Borecki

L D Atwood

S C Hunt

S S Rich

J H Eckfeldt

D K Arnett

D C Rao

R H Myers

Affiliations

Soon will be listed here.

Abstract

Segregation analysis was performed on the serum uric acid measurements from 523 randomly ascertained Caucasian families from the NHLBI Family Heart Study. Gender-specific standardized residuals were used as the phenotypic variable in both familial correlation and segregation analysis. Uric acid residuals were adjusted for age, age2, age3, body mass index (kg/m2), creatinine level, aspirin use (yes/no), total drinks (per week), HOMA insulin resistance index [(glucose * insulin)/22.5], diuretic use (yes/no), and triglyceride level. Sibling correlations (r=0.193) and parent-offspring correlations (r=0.217) were significantly different from zero, but these two familial correlations were not significantly different from one another. After adjustment for covariates, the heritability estimate for serum uric acid was 0.399. Segregation analysis rejected the "no major gene" model but was unable to discriminate between an "environmental" and a "Mendelian major gene" model. These results support the hypothesis that uric acid is a multifactorial trait possibly influenced by more than one major gene, modifying genes, and environmental factors.

Citing Articles

A phenome-wide association and factorial Mendelian randomization study on the repurposing of uric acid-lowering drugs for cardiovascular outcomes.

Wang L, Mesa-Eguiagaray I, Campbell H, Wilson J, Vitart V, Li X Eur J Epidemiol. 2024; 39(8):869-880.

PMID: 38992218 PMC: 11410910. DOI: 10.1007/s10654-024-01138-0.

Effect of serum uric acid on the risk of aortic aneurysm and dissection: A mendelian randomization analysis.

Lin Z, He H, Aierken Y, Wu Y, Liu Y Biochem Biophys Rep. 2024; 38:101743.

PMID: 38873223 PMC: 11170348. DOI: 10.1016/j.bbrep.2024.101743.

Polymorphism rs3733591 of the gene and metabolic syndrome affect gout risk in Taiwan Biobank subjects.

Lin C, Ho C, Hsieh P, Hsiao C, Nfor O, Liaw Y Front Genet. 2024; 15:1374405.

PMID: 38689651 PMC: 11058208. DOI: 10.3389/fgene.2024.1374405.

Enrichment analysis and chromosomal distribution of gout susceptible loci identified by genome-wide association studies.

Saadat M EXCLI J. 2024; 22:1146-1154.

PMID: 38204969 PMC: 10776878. DOI: 10.17179/excli2023-6481.

Risk of gout in Taiwan Biobank participants pertaining to their sex and family history of gout among first-degree relatives.

Tsai H, Tantoh D, Hsiao C, Zhong J, Chen C, Liaw Y Clin Exp Med. 2023; 23(8):5315-5325.

PMID: 37668883 DOI: 10.1007/s10238-023-01167-1.