中国高血压患者中α1A-肾上腺素能受体Arg347Cys多态性及血浆厄贝沙坦浓度与血压治疗反应的个体及联合关联
Individual and joint association of alpha1A-adrenergic receptor Arg347Cys polymorphism and plasma irbesartan concentration with blood pressure therapeutic response in Chinese hypertensive subjects.
作者信息
Jiang Shanqun, Mao Guangyun, Zhang Shanchun, Hong Xiumei, Tang Genfu, Li Zhiping, Liu Xue, Zhang Yan, Wang Binyan, Xu Xiping, Wang Xiaobin
机构信息
School of Life Sciences, University of Science and Technology of China, Anhui, Hefei, People's Republic of China.
出版信息
Clin Pharmacol Ther. 2005 Sep;78(3):239-48. doi: 10.1016/j.clpt.2005.06.003.
BACKGROUND
Individual variability in the therapeutic response to an antihypertensive drug could have a genetic basis. We investigated whether the alpha1A-adrenergic receptor (alpha1A-AR) Arg347Cys polymorphism is associated with the blood pressure (BP) therapeutic response to irbesartan and whether the association could be altered by the plasma irbesartan level.
METHODS
A total of 696 hypertensive subjects were treated with a daily oral dose of 150 mg irbesartan. Baseline BP was measured before the first dose. On the 28th day, after 27 consecutive days of treatment and an overnight fast, BPs and blood samples were obtained before the morning dose (0 hours) and 6 hours after the morning dose was taken. Plasma irbesartan concentrations were measured by use of HPLC-fluorescence.
RESULTS
BP therapeutic response was defined as baseline BP minus BP on the 28th day of irbesartan treatment. Relative to noncarriers, alpha1A-AR Cys347 allelic carriers had a significantly greater diastolic blood pressure (DBP) response at 0 hours (mean +/- SD, 7.5 +/- 8.4 mm Hg versus 5.5 +/- 8.4 mm Hg; P = .016) and at 6 hours (16.2 +/- 9.1 mm Hg versus 14.2 +/- 8.9 mm Hg, P = .025). Although the pattern was similar to the DBP response, alpha(1A)-AR Cys347 allelic carriers had only a moderately increased systolic blood pressure (SBP) response at the 2 time points. When subjects were stratified into subgroups with high or low plasma irbesartan concentrations (with the median value used as the cutoff point), Cys347 allelic carriers in the high-concentration group, relative to noncarriers, had a more pronounced DBP response at 0 hours (adjusted beta [+/- SE], 3.0 +/- 1.0 mm Hg; P = .004) and at 6 hours (adjusted beta, 3.0 +/- 1.2 mm Hg; P = .014), and the same was true for the SBP response at 0 hours (adjusted beta, 5.6 +/- 2.1 mm Hg; P = .006) and at 6 hours (adjusted beta, 4.7 +/- 2.0 mm Hg; P = .021). In contrast, in the low-concentration group, there was no significant association between DBP or SBP responses and Arg347Cys genotypes at 0 hours and 6 hours.
CONCLUSION
Our data suggest that the alpha1A-AR Arg347Cys polymorphism is associated with BP response (particularly DBP) to short-term irbesartan treatment. Our data also showed evidence of an interaction between the alpha1A-AR Arg347Cys polymorphism and the plasma level of irbesartan in relation to BP therapeutic response. The association of the Arg347Cys polymorphism with the BP therapeutic response was more pronounced in those patients with higher plasma concentrations of irbesartan.
背景
抗高血压药物治疗反应的个体差异可能具有遗传基础。我们研究了α1A - 肾上腺素能受体(α1A - AR)的Arg347Cys多态性是否与厄贝沙坦的血压(BP)治疗反应相关,以及这种关联是否会因血浆厄贝沙坦水平而改变。
方法
共有696名高血压患者每日口服150 mg厄贝沙坦进行治疗。在首次给药前测量基线血压。在第28天,连续治疗27天且禁食过夜后,于晨服药物前(0小时)和服药后6小时采集血压和血样。采用高效液相色谱 - 荧光法测定血浆厄贝沙坦浓度。
结果
BP治疗反应定义为厄贝沙坦治疗第28天的血压减去基线血压。与非携带者相比,α1A - AR Cys347等位基因携带者在0小时(平均±标准差,7.5±8.4 mmHg对5.5±8.4 mmHg;P = 0.016)和6小时(16.2±9.1 mmHg对14.2±8.9 mmHg,P = 0.025)时舒张压(DBP)反应显著更大。虽然收缩压(SBP)反应模式与DBP反应相似,但α1A - AR Cys347等位基因携带者在这两个时间点的SBP反应仅适度增加。当受试者按血浆厄贝沙坦浓度高或低分层(以中位数作为分界点)时,高浓度组中Cys347等位基因携带者与非携带者相比,在0小时(调整后β[±标准误],3.0±1.0 mmHg;P = 0.004)和6小时(调整后β,3.0±1.2 mmHg;P = 0.014)时DBP反应更明显,0小时(调整后β,5.6±2.1 mmHg;P = 0.006)和6小时(调整后β,4.7±即2.0 mmHg;P = 0.021)时SBP反应也是如此。相比之下,在低浓度组中,0小时和6小时时DBP或SBP反应与Arg347Cys基因型之间无显著关联。
结论
我们的数据表明,α1A - AR Arg347Cys多态性与短期厄贝沙坦治疗的BP反应(特别是DBP)相关。我们的数据还显示了α1A - AR Arg347Cys多态性与厄贝沙坦血浆水平在BP治疗反应方面存在相互作用的证据。Arg347Cys多态性与BP治疗反应的关联在血浆厄贝沙坦浓度较高的患者中更为明显。
Zotero 插件