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Oxidative stress and cardiovascular complications in diabetes: isoprostanes as new markers on an old paradigm

机译:糖尿病中的氧化应激和心血管并发症:异前列腺素作为旧范式上的新标志物

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AbstractLong-term vascular complications still represent the main cause of morbidity and mortality in diabetic patients. Although randomized long-term clinical studies comparing the effects of conventional and intensive therapy have demonstrated a clear link between hyperglycemia and the development of complications of diabetes, they have not defined the mechanism through which excess glucose results in tissue damage. Evidence has accumulated indicating that oxidative stress may play a key role in the etiology of diabetic complications. Isoprostanes are emerging as a new class of biologically active products of arachidonic acid metabolism of potential relevance to human vascular disease. Their formation in vivo seems to reflect primarily, if not exclusively, a nonenzymatic process of lipid peroxidation. Enhanced urinary excretion of 8-iso-PGF2αhas been described in association with both type 1 and type 2 diabetes mellitus, and correlates with impaired glycemic control. Besides providing a likely noninvasive index of lipid peroxidation in this setting, measurements of specific F2isoprostanes in urine may provide a sensitive biochemical end point for dose-finding studies of natural and synthetic inhibitors of lipid peroxidation. Although the biological effects of 8-iso-PGF2αin vitro suggest that it and other isoeicosanoids may modulate the functional consequences of lipid peroxidation in diabetes, evidence that this is likely in vivo remains inadequate at this tim
机译:摘要长期血管并发症仍是糖尿病患者发病和死亡的主要原因。尽管比较常规和强化治疗效果的随机长期临床研究表明,高血糖与糖尿病并发症的发展之间存在明显的联系,但它们尚未确定过量葡萄糖导致组织损伤的机制。越来越多的证据表明,氧化应激可能在糖尿病并发症的病因中起关键作用。异前列腺素正在成为花生四烯酸代谢的一类新型生物活性产物,与人类血管疾病有潜在相关性。它们在体内的形成似乎主要反映了脂质过氧化的非酶促过程,如果不是完全的话。据报道,8-异PGF2α的尿排泄增强与1型和2型糖尿病有关,并与血糖控制受损有关。在这种情况下,除了提供可能的脂质过氧化非侵入性指标外,尿液中特定 F2 异前列腺素的测量还可以为脂质过氧化的天然和合成抑制剂的剂量探索研究提供灵敏的生化终点。尽管 8-iso-PGF2α 的体外生物学效应表明它和其他异二十烷酸类化合物可能调节糖尿病中脂质过氧化的功能后果,但目前可能存在体内的证据仍然不足

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