慢性肾脏疾病中一氧化氮的生理和病理生理。

M Noris, G Remuzzi
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引用次数: 46

摘要

一氧化氮(NO)是一种l -精氨酸衍生物,具有多种肾脏和肾外生理和病理生理作用。一氧化氮合成酶(NOS)由三种亚型产生:两种急性反应的组成型亚型,神经元NOS (nNOS)和内皮NOS (ecNOS),以及更慢、更持久的诱导型NOS (iNOS)。NO调节肾小球超滤;肾小管重吸收和肾内肾素分泌。最近的一些研究,大多数是在大鼠肾团块减少(RMR)的实验模型中,提出了一个假设,即一氧化氮合成途径受损可能在介导与肾脏疾病进展相关的复杂肾脏血流动力学和非血流动力学疾病中起关键作用。因此,RMR大鼠肾脏产生的NO比正常大鼠少,并且NO的产生与肾损伤标志物呈负相关。这种异常是由于肾脏的iNOS缺陷造成的。也有数据显示,能够增强肾NO活性的药物可能对多种实验性肾脏疾病,特别是肾小球血流动力学紊乱的肾脏疾病具有肾保护作用。对人类的研究较少,这些研究也没有得出结论性的结果。
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Physiology and pathophysiology of nitric oxide in chronic renal disease.

Nitric oxide (NO), an L-arginine derivative, exerts a variety of renal and extrarenal physiological and pathophysiological effects. NO is generated by three isoforms of nitric oxide synthases (NOS): two acutely responsive, constitutive isoforms, neuronal NOS (nNOS) and endothelial NOS (ecNOS), and the slower, more persistent, inducible NOS (iNOS). NO regulates glomerular ultrafiltration; tubular reabsorption, and intrarenal renin secretion. A number of recent studies, most of them in the experimental model of renal mass reduction (RMR) in rats, have raised the hypothesis that an impaired NO synthetic pathway could have a key role in mediating the complex renal hemodynamic and nonhemodynamic disorders associated with the progression of renal disease. Thus, kidneys from rats with RMR produce less NO than normal rats, and NO generation negatively correlates with markers of renal damage. The abnormality is due to a defect in iNOS in the kidney. Data are also available showing that drugs capable of enhancing renal NO activity may be renoprotective in a variety of experimental renal diseases, particularly those characterized by derangements of glomerular hemodynamics. Fewer studies are available in humans and these have shown less than conclusive results.

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