Rare independent mutations in renal salt handling genes contribute to blood pressure variation

被引:0
|
作者
Weizhen Ji
Jia Nee Foo
Brian J O'Roak
Hongyu Zhao
Martin G Larson
David B Simon
Christopher Newton-Cheh
Matthew W State
Daniel Levy
Richard P Lifton
机构
[1] Yale University School of Medicine,Department of Genetics
[2] Howard Hughes Medical Institute,Department of Epidemiology and Public Health
[3] Yale University School of Medicine,Department of Mathematics and Statistics
[4] Yale University School of Medicine,undefined
[5] National Heart,undefined
[6] Lung,undefined
[7] and Blood Institute's Framingham Heart Study,undefined
[8] Boston University,undefined
[9] Child Study Center,undefined
[10] Yale University School of Medicine,undefined
[11] National Heart,undefined
[12] Lung and Blood Institute,undefined
来源
Nature Genetics | 2008年 / 40卷
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摘要
The effects of alleles in many genes are believed to contribute to common complex diseases such as hypertension. Whether risk alleles comprise a small number of common variants or many rare independent mutations at trait loci is largely unknown. We screened members of the Framingham Heart Study (FHS) for variation in three genes—SLC12A3 (NCCT), SLC12A1 (NKCC2) and KCNJ1 (ROMK)—causing rare recessive diseases featuring large reductions in blood pressure. Using comparative genomics, genetics and biochemistry, we identified subjects with mutations proven or inferred to be functional. These mutations, all heterozygous and rare, produce clinically significant blood pressure reduction and protect from development of hypertension. Our findings implicate many rare alleles that alter renal salt handling in blood pressure variation in the general population, and identify alleles with health benefit that are nonetheless under purifying selection. These findings have implications for the genetic architecture of hypertension and other common complex traits.
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页码:592 / 599
页数:7
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