Abstract

Gout is an inflammatory condition caused by elevated serum urate (SU), a condition known as hyperuricemia (HU). Genetic variations, including single nucleotide polymorphisms (SNPs), can alter the function of urate transporters, leading to differential HU and gout prevalence across different populations. In the United States (U.S.), gout prevalence differentially affects certain racial groups. The objective of this proposed analysis is to compare the frequency of urate-related genetic risk alleles between Europeans (EUR) and the following major racial groups: Africans in Southwest U.S. (ASW), Han-Chinese (CHS), Japanese (JPT), and Mexican (MXL) from the 1000 Genomes Project. The Ensembl genome browser of the 1000 Genomes Project was used to conduct cross-population allele frequency comparisons of 11 SNPs across 11 genes, physiologically involved and significantly associated with SU levels and gout risk. Gene/SNP pairs included: ABCG2 (rs2231142), SLC2A9 (rs734553), SLC17A1 (rs1183201), SLC16A9 (rs1171614), GCKR (rs1260326), SLC22A11 (rs2078267), SLC22A12 (rs505802), INHBC (rs3741414), RREB1 (rs675209), PDZK1 (rs12129861), and NRXN2 (rs478607). Allele frequencies were compared to EUR using Chi-Square or Fisher’s Exact test, when appropriate. Bonferroni correction for multiple comparisons was used, with p < 0.0045 for statistical significance. Risk alleles were defined as the allele that is associated with baseline or higher HU and gout risks. The cumulative HU or gout risk allele index of the 11 SNPs was estimated for each population. The prevalence of HU and gout in U.S. and non-US populations was evaluated using published epidemiological data and literature review. Compared with EUR, the SNP frequencies of 7/11 in ASW, 9/11 in MXL, 9/11 JPT, and 11/11 CHS were significantly different. HU or gout risk allele indices were 5, 6, 9, and 11 in ASW, MXL, CHS, and JPT, respectively. Out of the 11 SNPs, the percentage of risk alleles in CHS and JPT was 100%. Compared to non-US populations, the prevalence of HU and gout appear to be higher in western world countries. Compared with EUR, CHS and JPT populations had the highest HU or gout risk allele frequencies, followed by MXL and ASW. These results suggest that individuals of Asian descent are at higher HU and gout risk, which may partly explain the nearly three-fold higher gout prevalence among Asians versus Caucasians in ambulatory care settings. Furthermore, gout remains a disease of developed countries with a marked global rising.

Highlights

  • Gout is an inflammatory arthritic condition caused by the deposition of monosodium crystals (MSU) into the distal joints and peripheral tissues

  • HU and gout prevalence in non-U.S populations. These populations included Africans living in Africa, Asians living in Asia, Europeans living in Europe, and Hispanics living in Mexico

  • Our genetic analysis identified that the CHS and JPT populations as having the highest prevalence of validated HU and gout risk alleles compared with EUR

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Summary

Introduction

Gout is an inflammatory arthritic condition caused by the deposition of monosodium crystals (MSU) into the distal joints and peripheral tissues. Developing HU could be caused by increased consumption of high fructose corn syrup, a purine-rich diet, and high alcohol intake [1] Certain medications, such as diuretics and low-dose salicylates, can decrease urate excretion, increasing SU levels, and the risk of developing HU and gout [2]. The objective of this genetic analysis is to estimate the frequency of risk alleles associated with elevated SU levels or gout in select racial groups compared to Europeans. Some of these risk alleles are of specific interest as they may play a role in personalizing diet and treatment in patients with gout. To elucidate possible genetic sources of differential response to urate-lowering therapy among the U.S populations

Genetic Data Collection
SNP Selection
Statistical Analysis
Hyperuricemia and Gout Risk Alleles Frequencies
Global Gout Epidemiology
African Populations
Asian Populations
Hispanic Populations
European Populations
Discussion
Limitations
Future Perspective
Findings
Conclusions
Full Text
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