首页> 外文期刊>Thrombosis and Haemostasis: Journal of the International Society on Thrombosis and Haemostasis >Effects of high-amount-high-intensity exercise on in vivo platelet activation: Modulation by lipid peroxidation and AGE/RAGE axis
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Effects of high-amount-high-intensity exercise on in vivo platelet activation: Modulation by lipid peroxidation and AGE/RAGE axis

机译:高强度高强度运动对体内血小板活化的影响:脂质过氧化和AGE / RAGE轴的调节

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Physical activity is associated with cardiovascular risk reduction, but the effects of exercise on platelet activation remain controversial. We investigated the effects of regular high-amount, high intensity aerobic exercise on in vivo thromboxane (TX)-dependent platelet activation and plasma levels of platelet-derived proteins, CD40L and P-selectin, and whether platelet variables changes may be related to changes in high-density lipoprotein (HDL) and in the extent of oxidative stress and oxidative stress-related inflammation, as reflected by urinary isoprostane excretion and endogenous soluble receptor for advanced glycation end-products (esRAGE), respectively. Urinary excretion of 11-dehydro-TXB2 and 8-iso-prostaglandin (PG)F2α and plasma levels of P-selectin, CD40L and esRAGE were measured before and after a eight-week standardised aerobic high-amount-high-intensity training program in 22 sedentary subjects with low-to-intermediate risk. Exercise training had a clear beneficial effect on HDL cholesterol (+10%, p=0.027) and triglyceride (-27%, p=0.008) concentration. In addition, a significant (p0.0001) decrease in urinary 11-dehydro-TXB2 (26%), 8-iso-PGF2α (21%), plasma P-selectin (27%), CD40L (35%) and a 61% increase in esRAGE were observed. Multiple regression analysis revealed that urinary 8-iso-PGF2α [beta=0.33, SEM=0.116, p=0.027] and esRAGE (beta=-0.30, SEM=31.3, p=0.046) were the only significant predictors of urinary 11-dehydro-TXB2 excretion rate over the training period. In conclusion, regular high-amount-high-intensity exercise training has broad beneficial effects on platelet activation markers, paralleled and possibly associated with changes in the lipoprotein profile and in markers of lipid peroxidation and AGE/RAGE axis. Our findings may help explaining why a similar amount of exercise exerts significant benefits in preventing cardiovascular events.
机译:体育锻炼与降低心血管疾病风险有关,但运动对血小板活化的影响仍存在争议。我们研究了定期进行大量高强度有氧运动对体内血栓烷(TX)依赖性血小板活化和血小板衍生蛋白,CD40L和P-选择素血浆水平的影响,以及血小板变量的变化是否可能与变化有关在高密度脂蛋白(HDL)中以及在氧化应激和氧化应激相关炎症的范围内,分别反映为尿异前列腺素排泄和晚期糖基化终产物(esRAGE)的内源性可溶性受体。在进行为期8周的有氧高强度高强度标准训练计划之前和之后,测量11-脱氢-TXB2和8-异前列腺素(PG)F2α的尿排泄以及P-选择素,CD40L和esRAGE的血浆水平22个久坐的中低风险受试者。运动训练对HDL胆固醇(+ 10%,p = 0.027)和甘油三酸酯(-27%,p = 0.008)浓度具有明显的有益作用。此外,尿中11-脱氢-TXB2(26%),8-异-PGF2α(21%),血浆P-选择素(27%),CD40L(35%)和61尿显着降低(p <0.0001)。观察到esRAGE的%增加。多元回归分析显示,尿中的8-iso-PGF2α[β= 0.33,SEM = 0.116,p = 0.027]和esRAGE(β= -0.30,SEM = 31.3,p = 0.046)是尿中11-脱氢的唯一重要预测因子在训练期间-TXB2的排泄率。总之,定期的高强度高强度运动训练对血小板活化标志物具有广泛的有益作用,与脂蛋白谱以及脂质过氧化和AGE / RAGE轴标志物的变化平行且可能相关。我们的发现可能有助于解释为什么进行相似量的运动对预防心血管事件具有重要意义。

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