Abstract
BackgroundAcute doses of elevated retrograde shear rate (SR) appear to be detrimental to endothelial function in resting humans. However, retrograde shear increases during moderate intensity exercise which also enhances post-exercise endothelial function. Since SR patterns differ with the modality of exercise, it is important to determine if augmented retrograde SR during exercise influences post-exercise endothelial function. This study tested the hypothesis that (1) increased doses of retrograde SR in the brachial artery during lower body supine cycle ergometer exercise would attenuate post-exercise flow-mediated dilation (FMD) in a dose-dependent manner, and (2) antioxidant vitamin C supplementation would prevent the attenuated post-exercise FMD response.MethodsTwelve men participated in four randomized exercise sessions (90 W for 20 minutes) on separate days. During three of the sessions, one arm was subjected to increased oscillatory and retrograde SR using three different forearm cuff pressures (20, 40, 60 mmHg) (contralateral arm served as the control) and subjects ingested placebo capsules prior to exercise. A fourth session with 60 mmHg cuff pressure was performed with 1 g of vitamin C ingested prior to the session.ResultsPost-exercise FMD following the placebo conditions were lower in the cuffed arm versus the control arm (arm main effect: P < 0.05) and without differences between cuff pressures (20 mmHg: 5.7 ± 2.2%; 40 mmHg: 4.7 ± 1.3%; 60 mmHg: 5.4 ± 2.4%) (P > 0.05). Following vitamin C treatment, post-exercise FMD in the cuffed and control arm increased from baseline (P < 0.05) but were not different (control: 7.1 ± 3.5% vs. cuffed: 6.6 ± 3.3%) (P > 0.05).ConclusionsThese results indicate that augmented oscillatory and retrograde SR in non-working limbs during lower body exercise attenuates post-exercise FMD without an evident dose–response in the range of cuff pressures evaluated. Vitamin C supplementation prevented the attenuation of FMD following exercise with augmented oscillatory and retrograde SR suggesting that oxidative stress contributes to the adverse effects of oscillatory and retrograde shear during exercise on FMD.
Highlights
Acute doses of elevated retrograde shear rate (SR) appear to be detrimental to endothelial function in resting humans
Oxidative stress in endothelial cells is reduced and endothelial nitric oxide synthase (eNOS) function is preserved when the antioxidant vitamin C is administered during oxidative challenges [16,17]; it is reasonable to assume that reducing oxidative stress generated by oscillatory and retrograde shear by antioxidant supplementation may preserve NO bioavailability
The primary aims of this investigation were to (1) test the hypothesis that post-exercise brachial artery flow-mediated dilation (FMD) would be attenuated in a dose-dependent manner by varying the dose of retrograde shear in the brachial artery during lower body exercise, and (2) test the hypothesis that vitamin C supplementation would prevent the attenuation of brachial artery FMD following elevated brachial artery oscillatory and retrograde shear during lower body exercise
Summary
Acute doses of elevated retrograde shear rate (SR) appear to be detrimental to endothelial function in resting humans. Data obtained from animals and humans demonstrate that exercise produces an increased superoxide dismutase expression/ activity [3], improved endothelial nitric oxide synthase (eNOS) expression and phosphorylation [4], enhanced acetylcholine-induced vasomotor function [5], and a reduction in pro-oxidant enzymes [3,6]. These beneficial effects on the endothelium may be a result of exerciseinduced shear stress, which has been postulated to directly contribute to the improved function of the endothelium following exercise [2,7]. Oxidative stress in endothelial cells is reduced and eNOS function is preserved when the antioxidant vitamin C is administered during oxidative challenges [16,17]; it is reasonable to assume that reducing oxidative stress generated by oscillatory and retrograde shear by antioxidant supplementation may preserve NO bioavailability
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