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一种新型晚期糖基化终产物交联断裂剂改善动脉顺应性。

Improved arterial compliance by a novel advanced glycation end-product crosslink breaker.

作者信息

Kass D A, Shapiro E P, Kawaguchi M, Capriotti A R, Scuteri A, deGroof R C, Lakatta E G

机构信息

Division of Cardiology, The Johns Hopkins Medical Institutions, Baltimore, MD 21287, USA.

出版信息

Circulation. 2001 Sep 25;104(13):1464-70. doi: 10.1161/hc3801.097806.

Abstract

BACKGROUND

Arterial stiffening with increased pulse pressure is a leading risk factor for cardiovascular disease in the elderly. We tested whether ALT-711, a novel nonenzymatic breaker of advanced glycation end-product crosslinks, selectively improves arterial compliance and lowers pulse pressure in older individuals with vascular stiffening.

METHODS AND RESULTS

Nine US centers recruited and randomly assigned subjects with resting arterial pulse pressures >60 mm Hg and systolic pressures >140 mm Hg to once-daily ALT-711 (210 mg; n=62) or placebo (n=31) for 56 days. Preexisting antihypertensive treatment (90% of subjects) was continued during the study. Morning upright blood pressure, stroke volume, cardiac output, systemic vascular resistance, total arterial compliance, carotid-femoral pulse wave velocity, and drug tolerability were assessed. ALT-711 netted a greater decline in pulse pressures than placebo (-5.3 versus -0.6 mm Hg at day 56; P=0.034 for treatment effect by repeated-measures ANOVA). Systolic pressure declined in both groups, but diastolic pressure fell less with ALT-711 (P=0.056). Mean pressure declined similarly in both groups (-4 mm Hg; P<0.01 for each group, P=0.34 for treatment effect). Total arterial compliance rose 15% in ALT-711-treated subjects versus no change with placebo (P=0.015 versus ALT-711), an effect that did not depend on reduced mean pressure. Pulse wave velocity declined 8% with ALT-711 (P<0.05 at day 56, P=0.08 for treatment effect). Systemic arterial resistance, cardiac output, and heart rate did not significantly change in either group.

CONCLUSIONS

ALT-711 improves total arterial compliance in aged humans with vascular stiffening, and it may provide a novel therapeutic approach for this abnormality, which occurs with aging, diabetes, and isolated systolic hypertension.

摘要

背景

动脉僵硬度增加伴脉压增大是老年人心血管疾病的主要危险因素。我们测试了新型非酶促晚期糖基化终产物交联断裂剂ALT - 711是否能选择性改善血管硬化的老年人的动脉顺应性并降低脉压。

方法与结果

美国9个中心招募了静息动脉脉压>60 mmHg且收缩压>140 mmHg的受试者,并将其随机分为每日一次服用ALT - 711(210 mg;n = 62)组或安慰剂组(n = 31),为期56天。研究期间继续进行原有的抗高血压治疗(90%的受试者)。评估晨起直立位血压、每搏输出量、心输出量、全身血管阻力、总动脉顺应性、颈股脉搏波速度和药物耐受性。ALT - 711使脉压下降幅度大于安慰剂(第56天时分别为-5.3与-0.6 mmHg;重复测量方差分析得出治疗效果P = 0.034)。两组收缩压均下降,但ALT - 711组舒张压下降幅度较小(P = 0.056)。两组平均压下降幅度相似(-4 mmHg;每组P<0.01,治疗效果P = 0.34)。ALT - 711治疗的受试者总动脉顺应性升高15%,而安慰剂组无变化(与ALT - 711相比P = 0.015),该效应不依赖于平均压降低。ALT - 711使脉搏波速度下降8%(第56天时P<0.05,治疗效果P = 0.08)。两组全身动脉阻力、心输出量和心率均无显著变化。

结论

ALT - 711可改善血管硬化的老年人的总动脉顺应性,它可能为这种与衰老、糖尿病和单纯收缩期高血压相关的异常情况提供一种新的治疗方法。

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