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首页> 外文期刊>American Journal of Physiology >NAD(P)H oxidase and uncoupled nitric oxide synthase are major sources of glomerular superoxide in rats with experimental diabetic nephropathy.
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NAD(P)H oxidase and uncoupled nitric oxide synthase are major sources of glomerular superoxide in rats with experimental diabetic nephropathy.

机译:NAD(P)H氧化酶和未偶联的一氧化氮合酶是实验性糖尿病肾病大鼠肾小球超氧化物的主要来源。

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Increased production of reactive oxygen species (ROS) in diabetes may be a common pathway linking diverse pathogenic mechanisms of diabetic vascular complications, including nephropathy. Assessment of the oxidative stress production pathway is therefore important for the prediction and prevention of diabetic complications. However, ROS production mechanisms remain unclear in diabetic glomeruli. To identify the source and determine the mechanisms of ROS production in the diabetic kidney, diabetes was induced with streptozotocin in rats. After 6 wk, glomerular ROS production had increased in the streptozotocin rat kidney, as assessed by dihydroethidium-derived chemiluminescence. ROS production was increased by the addition of NADH or L-arginine and was partially reduced by the addition of diphenylene iodonium or N(G)-nitro-L-arginine methyl ester, identifying NAD(P)H oxidase and nitric oxide (NO) synthase (NOS) as ROS sources. The mRNA and protein expression of endothelial NOS (eNOS), as measured by real-time RT-PCR and Western blotting, increased significantly (mRNA level, 1.3-fold; protein level, 1.8-fold). However, the dimeric form of eNOS was decreased in diabetic glomeruli, as measured by low-temperature SDS-PAGE. Production of renal ROS and NO by uncoupled NOS was imaged by confocal laser microscopy after renal perfusion of 2',7'-dichlorofluorescein diacetate (a ROS marker) and diaminorhodamine-4M AM (a NO marker) with L-arginine. Accelerated ROS production and diminished bioavailable NO caused by NOS uncoupling were noted in the diabetic kidney. Administration of tetrahydrobiopterin (BH4), a cofactor for eNOS, reversed the decreased dimeric form of eNOS and glomerular NO production. Our results indicate that NAD(P)H oxidase and uncoupling of eNOS contribute to glomerular ROS production, mediated by the loss of BH4 availability. These mechanisms are potential key targets for therapeutic interventions.
机译:糖尿病患者体内活性氧(ROS)的增加可能是连接糖尿病性血管并发症(包括肾病)的多种致病机制的常见途径。因此,氧化应激产生途径的评估对于预测和预防糖尿病并发症很重要。但是,在糖尿病肾小球中ROS的产生机制仍不清楚。为了鉴定糖尿病肾脏中ROS的来源并确定ROS产生的机制,在大鼠中用链脲佐菌素诱导了糖尿病。 6周后,链脲佐菌素大鼠肾脏中肾小球ROS的产生增加,这是通过二氢乙啶衍生的化学发光评估的。 ROS的产生通过添加NADH或L-精氨酸而增加,并通过添加联苯碘鎓或N(G)-硝基-L-精氨酸甲酯而部分降低,从而确定了NAD(P)H氧化酶和一氧化氮(NO)合酶(NOS)作为ROS来源。通过实时RT-PCR和Western印迹检测,内皮NOS(eNOS)的mRNA和蛋白质表达显着增加(mRNA水平为1.3倍;蛋白质水平为1.8倍)。然而,如通过低温SDS-PAGE测量的,在糖尿病肾小球中eNOS的二聚体形式减少。肾灌注2',7'-二氯荧光素二乙酸盐(ROS标记)和二氨基若丹明-4M AM(NO标记)与L-精氨酸,通过共聚焦激光显微镜对未偶联NOS产生的肾脏ROS和NO进行成像。在糖尿病肾中注意到由NOS解偶联引起的ROS产生加速和NO的生物利用度降低。给予eNOS的辅助因子四氢生物蝶呤(BH4)可逆转eNOS减少的二聚体形式和肾小球NO生成。我们的结果表明NAD(P)H氧化酶和eNOS的解偶联有助于肾小球ROS的产生,其介导的BH4可用性下降。这些机制是治疗干预的潜在关键目标。

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