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首页> 外文期刊>Clinical and experimental pharmacology & physiology >The glucagon‐like peptide‐1 receptor agonist Exendin‐4, ameliorates contrast‐induced nephropathy through suppression of oxidative stress, vascular dysfunction and apoptosis independent of glycaemia
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The glucagon‐like peptide‐1 receptor agonist Exendin‐4, ameliorates contrast‐induced nephropathy through suppression of oxidative stress, vascular dysfunction and apoptosis independent of glycaemia

机译:胰高血糖素状的肽-1受体激动剂exendin-4,通过抑制氧化应激,血管功能障碍和凋亡独立于糖类症,改善了对比引起的肾病

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摘要

Summary Contrast‐induced nephropathy ( CIN ) is a leading cause of hospital‐acquired acute kidney injury, particularly in diabetic patients. Previous studies have shown renoprotective effects of glucagon‐like peptide‐1 ( GLP ‐1) signalling; however, its role in CIN remains unexplored. This study investigates the prophylactic effect of exendin‐4, a GLP ‐1R agonist, against CIN in a rat model mimicking both healthy and diabetic conditions. Animals were randomly divided into 7 groups: a control sham group (n?=?8), and 2 identical sets of 3 disease groups, one received exendin‐4 before exposure to contrast medium ( CM ), while the other served as untreated control. The 3 disease groups represented diabetes (n?=?8), CIN (n?=?8), or diabetes and CIN combined (n?=?8). Untreated groups showed deteriorating renal function as indicated by significantly higher levels of serum creatinine and blood urea nitrogen, malondialdehyde, and endothelin‐1 and caspase‐3 expression compared to the sham control group. This was accompanied by a significant decrease in tissue reserves of reduced glutathione, superoxide dismutase, nitrate and endothelin nitric oxide synthase as well as deteriorating renal histology. The CM ‐induced changes in diabetic rats indicate impaired renal function, oxidative stress, vascular dysfunction, and apoptosis, and were significance higher in intensity compared to non‐diabetic rats. Pretreatment with exendin‐4 ameliorated all the aforementioned CM ‐induced nephropathic effects independent of the glycemic state. To our knowledge, this is the first study describing the prophylactic renoprotective effects of exendin‐4 against CIN . With the current pharmaceutical use of exendin‐4 as a hypoglycaemic agent, the GLP ‐1R agonist becomes an interesting candidate for human clinical trials on CIN prevention.
机译:发明内容对比诱导的肾病(CIN)是医院获得的急性肾损伤的主要原因,特别是在糖尿病患者中。以前的研究表明了胰高血糖素样肽-1(GLP -1)信号传导的重新检查。但是,它在CIN中的作用仍然是未开发的。本研究研究了exendin-4,GLP-1R激动剂的预防效果,在模拟健康和糖尿病条件的大鼠模型中对CIN的CIN。将动物随机分为7组:控制假小组(n?=Δ8)和2组相同的3组,在暴露于造影剂(cm)之前接受Exendin-4,而另一个是未处理的对照。 3疾病组代表糖尿病(N?=?8),CIN(n?=?8),或糖尿病和CIN组合(n?=?8)。未处理的基团显示肾功能劣化,如与假对照组相比明显更高水平的血清肌酐和血尿尿素氮,丙二醛和内皮素-1和Caspase-3表达。这伴随着减少谷胱甘肽,超氧化物歧化酶,硝酸盐和内皮素一氧化氮合酶以及肾组织学的恶化的显着降低。 CM-诱导的糖尿病大鼠的变化表明肾功能受损,氧化应激,血管功能障碍和凋亡,与非糖尿病大鼠相比,强度较高。用exendin-4预处理改善了所有上述CM-诱导的肾病作用,而不依赖于血糖状态。为了我们的知识,这是第一项描述Exendin-4对CIN的预防性再试反对的研究。随着exendin-4作为低血糖药物的目前的药物用途,GLP -1R激动剂成为人类临床试验的有趣候选者对CIN预防的临床试验。

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