Large-scale whole-exome sequencing association studies identify rare functional variants influencing serum urate levels

被引:0
|
作者
Adrienne Tin
Yong Li
Jennifer A. Brody
Teresa Nutile
Audrey Y. Chu
Jennifer E. Huffman
Qiong Yang
Ming-Huei Chen
Cassianne Robinson-Cohen
Aurélien Macé
Jun Liu
Ayşe Demirkan
Rossella Sorice
Sanaz Sedaghat
Melody Swen
Bing Yu
Sahar Ghasemi
Alexanda Teumer
Peter Vollenweider
Marina Ciullo
Meng Li
André G. Uitterlinden
Robert Kraaij
Najaf Amin
Jeroen van Rooij
Zoltán Kutalik
Abbas Dehghan
Barbara McKnight
Cornelia M. van Duijn
Alanna Morrison
Bruce M. Psaty
Eric Boerwinkle
Caroline S. Fox
Owen M. Woodward
Anna Köttgen
机构
[1] Johns Hopkins Bloomberg School of Public Health,Department of Epidemiology
[2] University of Freiburg,Institute of Genetic Epidemiology, Faculty of Medicine and Medical Center
[3] University of Washington,Cardiovascular Health Research Unit, DoM
[4] Institute of Genetics and Biophysics “Adriano Buzzati-Traverso” - CNR,Population Sciences Branch, Division of Intramural Research
[5] National Heart,Framingham Heart Study
[6] Lung,VA Boston Healthcare System
[7] and Blood Institute,Department of Biostatistics, School of Public Health
[8] National Heart,Department of Nephrology
[9] Lung,Department of Computational Biology
[10] and Blood Institute,Department of Epidemiology
[11] Center for Population Genomics,Department of Human Genetics
[12] Boston University,Institute for Community Medicine
[13] Vanderbilt University Medical Center,Partner site Greifswald
[14] University of Lausanne,Department of Internal Medicine
[15] Erasmus Medical Center,Department of Physiology
[16] Leiden University Medical Center,Department of Internal Medicine
[17] IRCCS Neuromed,Institute of Social and Preventive Medicine (IUMSP)
[18] UTHealth School of Public Health,Leiden Academic Centre for Drug Research
[19] University Medicine Greifswald,undefined
[20] German Center for Cardiovascular Research (DZHK),undefined
[21] Centre Hospitalier Universitaire Vaudois (CHUV),undefined
[22] University of Maryland School of Medicine,undefined
[23] Erasmus Medical Center,undefined
[24] Centre Hospitalier Universitaire Vaudois (CHUV),undefined
[25] Leiden University,undefined
来源
Nature Communications | / 9卷
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摘要
Elevated serum urate levels can cause gout, an excruciating disease with suboptimal treatment. Previous GWAS identified common variants with modest effects on serum urate. Here we report large-scale whole-exome sequencing association studies of serum urate and kidney function among ≤19,517 European ancestry and African-American individuals. We identify aggregate associations of low-frequency damaging variants in the urate transporters SLC22A12 (URAT1; p = 1.3 × 10−56) and SLC2A9 (p = 4.5 × 10−7). Gout risk in rare SLC22A12 variant carriers is halved (OR = 0.5, p = 4.9 × 10−3). Selected rare variants in SLC22A12 are validated in transport studies, confirming three as loss-of-function (R325W, R405C, and T467M) and illustrating the therapeutic potential of the new URAT1-blocker lesinurad. In SLC2A9, mapping of rare variants of large effects onto the predicted protein structure reveals new residues that may affect urate binding. These findings provide new insights into the genetic architecture of serum urate, and highlight molecular targets in SLC22A12 and SLC2A9 for lowering serum urate and preventing gout.
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