BACKGROUND AND OBJECTIVES:We tested the hypothesis that single nucleotide polymorphisms (SNPs) in the calcium-sensing receptor (CASR) alter the response to the calcimimetic cinacalcet. DESIGN, SETTING, PARTICIPANTS, & MEASUREMENTS:We analyzed DNA samples in the Evaluation of Cinacalcet HCl Therapy to Lower Cardiovascular Events (EVOLVE) trial, a randomized trial comparing cinacalcet to placebo on a background of usual care. Of the 3883 patients randomized, 1919 (49%) consented to DNA collection, and samples from 1852 participants were genotyped for 18 CASR polymorphisms. The European ancestry (EA; n=1067) and African ancestry (AfAn; n=405) groups were assessed separately. SNPs in CASR were tested for their association with biochemical measures of mineral metabolism at baseline, percent change from baseline to 20 weeks, and risk of clinical fracture as dependent variables. RESULTS:There were modest associations of CASR SNPs with increased baseline serum parathyroid hormone and bone alkaline phosphatase primarily with the minor allele in the EA group (all P≤0.03), but not in the AfAn sample. In contrast, there was a modest association of decreased baseline serum calcium and FGF23 with CASR SNPs (P=0.04) primarily with the minor allele in the AfAn but not in the EA sample. The minor allele of two SNPs was associated with decreased percent reduction in parathyroid hormone from baseline to 20 weeks in the EA population (P<0.04) and this was not altered with cinacalcet. In both EA and AfAn, the same SNP (rs9740) was associated with decreased calcium with cinacalcet treatment (EA and AfAn P≤0.03). Three SNPs in high linkage disequilibrium were associated with a higher risk of clinical fracture that was attenuated by cinacalcet treatment in the EA sample (P<0.04). CONCLUSIONS:These modest associations, if validated, may provide explanations for differences in CKD-mineral bone disorder observed in EA and AfAn populations, and for differential biochemical responses to calcimimetics.

译文

背景与目的:我们检验了钙敏感受体(CASR)中的单核苷酸多态性(SNP)改变对拟钙剂西那卡塞的反应的假说。
设计,地点,参与者和测量:我们在Cinacalcet HCl降低心血管事件治疗评估(EVOLVE)试验中分析了DNA样品,该试验是在常规护理的背景下将cinacalcet与安慰剂进行比较的随机试验。在3883名随机分组的患者中,有1919名(49%)同意收集DNA,并对来自1852名参与者的样本进行了18种CASR多态性的基因分型。欧洲血统(EA; n = 1067)和非洲血统(AfAn; n = 405)分别进行了评估。测试了CASR中的SNP与基线时矿物质代谢的生化指标,从基线到20周的变化百分数以及临床骨折风险为因变量的相关性。
结果:在EA组中,CASR单核苷酸多态性与基线血清甲状旁腺激素和骨碱性磷酸酶升高之间存在适度的关联,主要与次要等位基因相关(均P≤0.03),而在AfAn样品中则无此关联。相反,基线血清钙和FGF23降低与CASR SNPs(P = 0.04)之间存在适度的联系,主要与AfAn中的次要等位基因有关,而与EA样品中无关。在EA人群中,两个SNP的次要等位基因与甲状旁腺激素从基线降低到20周的百分比降低相关(P <0.04),而西那卡塞未改变。在EA和AfAn中,相同的SNP(rs9740)与西那卡塞治疗引起的钙降低有关(EA和AfAnP≤0.03)。高连锁不平衡中的三个SNP与EA样品中的西那卡塞特治疗减弱的临床骨折风险较高相关(P <0.04)。
结论:这些适度的关联性如果得到验证,则可以解释EA和AfAn人群中CKD矿物骨骼疾病的差异,以及对拟钙剂的不同生化反应。

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