首页> 美国卫生研究院文献>Clinical Cardiology >Gender‐specific association between preproendothelin‐1 genotype and reduction of systolic blood pressure during antihypertensive treatment‐‐‐results from the Swedish irbesartan left ventricular hypertrophy investigation versus atenolol (SILVHIA)
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Gender‐specific association between preproendothelin‐1 genotype and reduction of systolic blood pressure during antihypertensive treatment‐‐‐results from the Swedish irbesartan left ventricular hypertrophy investigation versus atenolol (SILVHIA)

机译:降钙素原前素-1基因型与降压治疗期间收缩压降低之间的性别特异性关联-瑞典厄贝沙坦左心室肥大研究与阿替洛尔(SILVHIA)的结果

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摘要

Background: Studies suggest that endothelin‐1 contributes to the pathogenesis of hypertension. A G5665T gene polymorphism of preproendothelin‐1 has been shown to be associated with higher blood pressure in overweight patients. No study has yet determined the effect of this polymorphism on the change in blood pressure during antihypertensive treatment. Hypothesis: This study aimed to determine this effect in hypertensive patients with left ventricular (LV) hypertrophy during antihypertensive treatment with either irbesartan or atenolol. Methods: We determined the preproendothelin‐1 genotype using minisequencing in 102 patients with essential hypertension and LV hypertrophy verified by echocardiography, randomized in a double‐blind fashion to treatment with either the AT1‐receptor antagonist irbesartan or the beta1 ‐adrenoceptor antagonist atenolol. Results: The change in systolic blood pressure (SBP) after 12 weeks of treatment was related to the preproendothelin‐1 genotype in men; after adjustment for potential covariates (age, blood pressure, and LV mass index at study entry, dose of irbesartan/atenolol, and type of treatment), those carrying the T‐allele responded on average with a more than two‐fold greater reduction than those with the G/G genotype (‐21.9 mmHg [3.9] vs. ‐8.9 [2.3], p = 0.007). No significant differences in blood pressure change between G/G and carriers of the T‐allele were seen among women. Conclusions: Our finding suggests a gender‐specific relationship between the G5665T preproendothelin‐1 polymorphism and change in SBP in response to antihypertensive treatment with irbesartan or atenolol, suggesting the endothelin pathway to be a common mechanism included in the hypertensive action of the drugs.
机译:背景:研究表明内皮素-1有助于高血压的发病机理。已显示前原内皮素-1的G5665T基因多态性与超重患者的血压升高有关。尚无研究确定这种多态性对降压治疗期间血压变化的影响。假设:这项研究旨在确定在用厄贝沙坦或阿替洛尔进行降压治疗期间左心室肥大的高血压患者中的这种作用。方法:我们采用微序列测定法确定了102例原发性高血压和左室肥厚的前内皮素-1基因型,该患者经超声心动图检查证实,以双盲方式随机分配至AT1受体拮抗剂厄贝沙坦或β1肾上腺素受体拮抗剂阿替洛尔。结果:治疗12周后收缩压(SBP)的变化与男性前原内皮素-1基因型有关。在对潜在的协变量(年龄,血压和研究开始时的LV质量指数,厄贝沙坦/ atenolol的剂量以及治疗类型)进行调整后,携带T等位基因的患者的平均缓解率要高出两倍以上具有G / G基因型的患者(‐21.9 mmHg [3.9]与‐8.9 [2.3],p = 0.007)。女性之间G / G和T等位基因携带者的血压变化无显着差异。结论:我们的发现表明G5665T肾上腺素原蛋白1多态性与依贝沙坦或阿替洛尔的降压治疗引起的SBP变化之间存在性别特异性关系,这表明内皮素途径是药物高血压作用中的常见机制。

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