Klahr S
Department of Medicine, Barnes-Jewish Hospital at Washington University School of Medicine, St. Louis, MO 63110-1092, USA.
Semin Nephrol. 2001 Mar;21(2):133-45. doi: 10.1053/snep.2001.20942.
Angiotensin II plays a pivotal role in the progression of renal diseases, including obstructive nephropathy. Increasing levels of angiotensin II in obstructive nephropathy upregulate the expression of several factors: transforming growth factor-beta1 (TGF-beta1), tumor necrosis factor-alpha (TNF-alpha), platelet-derived growth factor (PDGF), insulin-like growth factor (IGF-1), osteopontin, vascular cell adhesion molecule-1 (VCAM-1), nuclear factor-kappaB (NF-kappaB), monocyte chemoattractant peptide-1 (MCP-1), intercellular adhesion molecule-1 (ICAM-1), and CD14 among others. Local production of TGF-beta, by intrinsic renal cells or by macrophages invading the kidney, is a key mediator of renal fibrosis. Activation of TGF-beta stimulates endothelin production. Endothelin, in turn, is a potent stimulus for fibrogenesis. Oxidative stress, fueled in part by angiotensin II, upregulates the expression of adhesion molecules, chemoattractant compounds and cytokines. Sustained obstructive nephropathy leads to apoptosis of tubular epithelial cells. Several factors and genes involved in apoptosis have been described. Nuclear factor kappa-B is involved in the transcriptional regulation of genes present in several organs, including the kidney. NF-kappaB is activated in the setting of ureteral obstruction. Administration of angiotensin-converting enzyme (ACE) inhibitors decreased significantly the activation of NF-kappaB in the obstructed kidney. Studies in neonatal rats indicate that chronic ureteral obstruction decreases the expression of epidermal growth factor (EGF). Replacement of this factor decreased apoptosis and reduced the expression of vimentin, clusterin, and TGF-beta. The administration of IGF-1 also lessened the tubular and interstitial pathology in the setting of ureteral obstruction. A spectrum of urinary tract malformations have been described. The utility of certain markers such as fetal serum beta(2) microglobulin as a predictor of postnatal renal function in bilateral uropathies has been described. A number of pharmacologic interventions that ameliorate the increased expansion of the interstitial volume, decrease the expression of TGF-beta, and down-regulate the production of extracellular matrix and the infiltration of the interstitium by macrophages have been described. Drugs used include ACE inhibitors, administration of arginine, administration of osteogenic protein-1, Pirferidone, and so on. It is likely that in the next decade advances in genetic manipulations and new drug therapies may forestall the development of fibrosis in the setting of urinary tract obstruction.
血管紧张素II在包括梗阻性肾病在内的肾脏疾病进展中起关键作用。梗阻性肾病中血管紧张素II水平升高会上调多种因子的表达:转化生长因子-β1(TGF-β1)、肿瘤坏死因子-α(TNF-α)、血小板衍生生长因子(PDGF)、胰岛素样生长因子(IGF-1)、骨桥蛋白、血管细胞黏附分子-1(VCAM-1)、核因子-κB(NF-κB)、单核细胞趋化蛋白-1(MCP-1)、细胞间黏附分子-1(ICAM-1)以及CD14等。肾脏固有细胞或侵入肾脏的巨噬细胞局部产生的TGF-β是肾纤维化的关键介质。TGF-β的激活会刺激内皮素的产生。内皮素反过来又是纤维化形成的有力刺激因素。部分由血管紧张素II引发的氧化应激会上调黏附分子、趋化性化合物和细胞因子的表达。持续性梗阻性肾病会导致肾小管上皮细胞凋亡。已经描述了一些与凋亡相关的因子和基因。核因子κB参与包括肾脏在内的多个器官中基因的转录调控。输尿管梗阻时NF-κB被激活。给予血管紧张素转换酶(ACE)抑制剂可显著降低梗阻肾脏中NF-κB的激活。对新生大鼠的研究表明,慢性输尿管梗阻会降低表皮生长因子(EGF)的表达。补充该因子可减少凋亡并降低波形蛋白、聚集素和TGF-β的表达。给予IGF-1也可减轻输尿管梗阻时的肾小管和间质病变。已经描述了一系列泌尿系统畸形。已经描述了某些标志物如胎儿血清β2微球蛋白作为双侧尿路疾病中出生后肾功能预测指标的效用。已经描述了一些改善间质容积增加、降低TGF-β表达、下调细胞外基质产生以及减少巨噬细胞对间质浸润的药物干预措施。使用的药物包括ACE抑制剂、精氨酸给药、成骨蛋白-1给药、吡非尼酮等等。在未来十年,基因操作和新药物疗法的进展可能会预防尿路梗阻时纤维化的发展。
