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CYP3A4 和 CYP3A5 多态性与氨氯地平在早期高血压性肾病的非裔美国男性和女性中对血压反应的关系。

CYP3A4 and CYP3A5 polymorphisms and blood pressure response to amlodipine among African-American men and women with early hypertensive renal disease.

机构信息

University of California-San Diego, 3350 La Jolla Village Drive, San Diego, CA 92131, USA.

出版信息

Am J Nephrol. 2010;31(2):95-103. doi: 10.1159/000258688. Epub 2009 Nov 12.

DOI:10.1159/000258688
PMID:19907160
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2853591/
Abstract

PURPOSE

To explore the association between CYP3A4 and CYP3A5 gene polymorphisms and blood pressure response to amlodipine among participants from the African-American Study of Kidney Disease and Hypertension Trial randomized to amlodipine (n = 164).

METHODS

Cox proportional hazards models were used to determine the risk of reaching a target mean arterial pressure (MAP) of < or =107 mm Hg by CYP3A4 (A-392G and T16090C) and CYP3A5 (A6986G) gene polymorphisms, stratified by MAP randomization group (low or usual) and controlling for other predictors for blood pressure response.

RESULTS

Women randomized to a usual MAP goal with an A allele at CYP3A4 A-392G were more likely to reach a target MAP of 107 mm Hg. The adjusted hazard ratio (AA/AG compared to GG) with 95% confidence interval was 3.41 (1.20-9.64; p = 0.020). Among participants randomized to a lower MAP goal, those with the C allele at CYP3A4 T16090C were more likely to reach target MAP: The adjusted hazard ratio was 2.04 (1.17-3.56; p = 0.010). After adjustment for multiple testing using a threshold significance level of p = 0.016, only the CYP3A4 T16090C SNP remained significant. CYP3A5 A6986G was not associated with blood pressure response.

CONCLUSIONS

Our findings suggest that blood pressure response to amlodipine among high-risk African-Americans appears to be determined by CYP3A4 genotypes, and sex specificity may be an important consideration. Clinical applications of CYP3A4 genotype testing for individualized treatment regimens warrant further study.

摘要

目的

探讨 CYP3A4 和 CYP3A5 基因多态性与非洲裔美国人肾脏病和高血压研究试验中接受氨氯地平治疗的参与者的血压反应之间的关系(n = 164,随机分为氨氯地平组)。

方法

使用 Cox 比例风险模型确定 CYP3A4(A-392G 和 T16090C)和 CYP3A5(A6986G)基因多态性与目标平均动脉压(MAP)<或=107mmHg 之间的相关性,根据 MAP 随机分组(低值或常规值)分层,并控制其他血压反应预测因素。

结果

随机分到常规 MAP 目标的女性中,CYP3A4 A-392G 存在 A 等位基因者更有可能达到 107mmHg 的目标 MAP。调整后的风险比(AA/AG 与 GG 相比)及其 95%置信区间为 3.41(1.20-9.64;p = 0.020)。在随机分到较低 MAP 目标的参与者中,CYP3A4 T16090C 存在 C 等位基因者更有可能达到目标 MAP:调整后的风险比为 2.04(1.17-3.56;p = 0.010)。在使用 p = 0.016 的阈值显著水平进行多次检验调整后,只有 CYP3A4 T16090C SNP 仍然具有显著意义。CYP3A5 A6986G 与血压反应无关。

结论

我们的研究结果表明,高危非洲裔美国人对氨氯地平的血压反应似乎取决于 CYP3A4 基因型,性别特异性可能是一个重要的考虑因素。进一步研究 CYP3A4 基因型检测用于个体化治疗方案的临床应用是有必要的。

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