Department of Internal Medicine, Section on Nephrology, Wake Forest School of Medicine, Winston-Salem, North Carolina 27157-1053, USA.
Kidney Int. 2012 Oct;82(7):805-11. doi: 10.1038/ki.2012.217. Epub 2012 Jun 13.
Familial aggregation of non-diabetic end-stage renal disease (ESRD) is found in African Americans and variants in the apolipoprotein L1 gene (APOL1) contribute to this risk. To detect genetic associations with milder forms of nephropathy in the high-risk families, analyses were performed using generalized estimating equations to assess relationships between kidney disease phenotypes and APOL1 variants in 786 relatives of 470 families. Adjusting for familial correlations, 23.1, 46.7, and 30.2% of genotyped relatives possessed two, one, or no APOL1 risk variants, respectively. Relatives with two compared with one or no risk variants had statistically indistinguishable median systolic blood pressure, urine albumin to creatinine ratio, estimated glomerular filtration rate (GFR; MDRD equation), and serum cystatin C levels. After adjusting for age, gender, age at ESRD in families, and African ancestry, significant associations were detected between APOL1 with overt proteinuria and estimated GFR (CKD-EPI equation), with a trend toward significance for quantitative albuminuria. Thus, relatives of African Americans with non-diabetic ESRD are enriched for APOL1 risk variants. After adjustment, two APOL1 risk variants weakly predict mild forms of kidney disease. Second hits appear necessary for the initiation of APOL1-associated nephropathy.
非糖尿病终末期肾病(ESRD)在非裔美国人中存在家族聚集现象,载脂蛋白 L1 基因(APOL1)的变异与此风险有关。为了在高危家族中检测与轻度肾病相关的遗传关联,使用广义估计方程对 470 个家族的 786 名亲属的肾脏疾病表型与 APOL1 变异之间的关系进行了分析。调整家族相关性后,分别有 23.1%、46.7%和 30.2%的基因分型亲属具有两个、一个或没有 APOL1 风险变异。与一个或没有风险变异的亲属相比,具有两个风险变异的亲属的收缩压、尿白蛋白与肌酐比值、估计肾小球滤过率(MDRD 方程)和血清胱抑素 C 水平无统计学差异。在调整年龄、性别、家族中 ESRD 的年龄和非洲裔祖先后,APOL1 与显性蛋白尿和估计肾小球滤过率(CKD-EPI 方程)之间存在显著关联,与定量白蛋白尿呈显著趋势。因此,非糖尿病 ESRD 的非裔美国人亲属中富含 APOL1 风险变异。调整后,两个 APOL1 风险变异可弱预测轻度肾病。第二击似乎是 APOL1 相关肾病发生的必要条件。
