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The effect of an advanced glycation end-product crosslink breaker and exercise training on vascular function in older individuals: a randomized factorial design trial

机译:先进的糖化终产物交联剂和运动训练对老年人血管功能的影响:一项随机因子设计试验

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摘要

Aging leads to accumulation of irreversible advanced glycation end-products (AGEs), contributing to vascular stiffening and endothelial dysfunction. When combined with the AGE-crosslink breaker Alagebrium, exercise training reverses cardiovascular aging in experimental animals. This study is the first to examine the effect of Alagebrium, with and without exercise training, on endothelial function, arterial stiffness and cardiovascular risk in older individuals. Forty-eight non-exercising individuals (mean age 70±4 years) without manifest diseases or use of medication were allocated into 4 groups for a 1-year intervention: Exercise training & Alagebrium (200mg/day); Exercise training & placebo; No exercise training & Alagebrium (200mg/day); No exercise training & placebo. We performed a maximal exercise test (VO2max) and measured endothelial function using venous occlusion plethysmography and intra-arterial infusion of acetylcholine, sodium nitroprusside and NG-monomethyl-L-arginine. Arterial stiffness was measured using pulse wave velocity. Cardiovascular risk was calculated using the Lifetime Risk Score (LRS). In the exercise training groups, LRS and VO2max improved significantly (23.9±4.5 to 27.2±4.6mlO2/min/kg, p<0.001). Endothelial response to the vasoactive substances did not change, nor did arterial stiffness in any of the four groups. In conclusion, one year of exercise training significantly improved physical fitness and lifetime risk for cardiovascular disease without affecting endothelial function or arterial stiffness. The use of the AGE-crosslink breaker Alagebrium had no independent effect on vascular function, nor did it potentiate the effect of exercise training. Despite the clinical benefits of exercise training for older individuals, neither exercise training nor Alagebrium (alone or in combination) was able to reverse the vascular effects of decades of sedentary aging.
机译:衰老导致不可逆的晚期糖基化终产物(AGEs)积聚,导致血管僵硬和内皮功能障碍。与AGE-交联破坏剂Alagebrium结合使用时,运动训练可逆转实验动物的心血管衰老。这项研究是第一个检验Alagebrium在有和没有运动训练的情况下对老年人内皮功能,动脉僵硬度和心血管风险的影响的研究。将48名无明显疾病或未使用药物的非运动者(平均年龄70±4岁)分为4组,进行为期1年的干预:运动训练和Alagebrium(200mg /天);运动训练和安慰剂;没有运动训练和Alagebrium(200mg /天);没有运动训练和安慰剂。我们进行了最大运动测试(VO2max),并使用静脉闭塞体积描记法和动脉内灌注乙酰胆碱,硝普钠和N G -单甲基-L-精氨酸对动脉内皮功能进行了测量。使用脉搏波速度测量动脉僵硬度。使用终生风险评分(LRS)计算心血管风险。在运动训练组中,LRS和VO2max显着改善(23.9±4.5至27.2±4.6mlO2 / min / kg,p <0.001)。血管活性物质的内皮反应没有改变,四组中的任何一组都没有改变。总而言之,一年的运动训练在不影响内皮功能或动脉僵硬的情况下,显着改善了身体健康和心血管疾病的终生风险。 AGE交联破坏剂Alagebrium的使用对血管功能没有独立影响,也没有增强运动训练的效果。尽管运动训练对老年个体具有临床益处,但是运动训练和Alagebrium(单独或组合使用)都无法逆转数十年来久坐衰老对血管的影响。

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