The association of the MYH9 gene and kidney outcomes in American Indians: the Strong Heart Family Study

被引:0
|
作者
Nora Franceschini
V. Saroja Voruganti
Karin Haack
Laura Almasy
Sandy Laston
Harald H. H. Göring
Jason G. Umans
Elisa T. Lee
Lyle G. Best
Richard R. Fabsitz
Jean W. MacCluer
Barbara V. Howard
Kari E. North
Shelley A. Cole
机构
[1] University of North Carolina,Department of Epidemiology
[2] Southwest Foundation for Biomedical Research,Department of Genetics
[3] Georgetown University Medical Center,Division of Nephrology and Hypertension
[4] University of Oklahoma Health Sciences Center,Center for American Indian Health Research, College of Public Health
[5] Missouri Breaks Industries Research,Division of Cardiovascular Sciences
[6] Inc.,Center for Genome Sciences
[7] National Heart,undefined
[8] Lung,undefined
[9] and Blood Institute,undefined
[10] MedStar Research Institute,undefined
[11] University of North Carolina,undefined
来源
Human Genetics | 2010年 / 127卷
关键词
Chronic Kidney Disease; Variance Component Model; MYH9 Gene; Reduce Kidney Function; American Indian Population;
D O I
暂无
中图分类号
学科分类号
摘要
Chronic kidney disease (CKD) is an important public health problem in American Indian populations. Recent research has identified associations of polymorphisms in the myosin heavy chain type II isoform A (MYH9) gene with hypertensive CKD in African-Americans. Whether these associations are also present among American Indian individuals is unknown. To evaluate the role of genetic polymorphisms in the MYH9 gene on kidney disease in American Indians, we genotyped 25 SNPs in the MYH9 gene region in 1,119 comparatively unrelated individuals. Four SNPs failed, and one SNP was monomorphic. We inferred haplotypes using seven SNPs within the region of the previously described E haplotype using Phase v2.1. We studied the association between 20 MYH9 SNPs with kidney function (estimated glomerular filtration rate, eGFR) and CKD (eGFR < 60 ml/min/1.73 m2 or renal replacement therapy or kidney transplant) using age-, sex- and center-adjusted models and measured genotyped within the variance component models. MYH9 SNPs were not significantly associated with kidney traits in additive or recessive genetic adjusted models. MYH9 haplotypes were also not significantly associated with kidney outcomes. In conclusion, common variants in MYH9 polymorphisms may not confer an increased risk of CKD in American Indian populations. Identification of the actual functional genetic variation responsible for the associations seen in African-Americans will likely help to clarify the lack of replication of this gene in our population of American Indians.
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页码:295 / 301
页数:6
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