环孢素诱导的间质纤维化和小动脉转化生长因子-β表达伴肾血流保留
Cyclosporine-induced interstitial fibrosis and arteriolar TGF-beta expression with preserved renal blood flow.
作者信息
Vieira J M, Noronha I L, Malheiros D M, Burdmann E A
机构信息
Department of Medicine, University of São Paulo Medical School, Brazil.
出版信息
Transplantation. 1999 Dec 15;68(11):1746-53. doi: 10.1097/00007890-199912150-00019.
BACKGROUND
Cyclosporine A (CsA)-induced chronic nephrotoxicity is characterized by interstitial fibrosis and afferent arteriole hyalinosis. CsA lesion has been linked to maintained renal vasoconstriction and narrowing of the afferent arteriole lumen diameter, leading to preglomerular ischemia. We investigated the role of renal hemodynamics in CsA-induced transforming growth factor (TGF-beta) expression and interstitial fibrosis.
METHODS
Groups of rats fed a low salt diet were given CsA 5 mg/kg/day (CsA) or the vehicle (olive oil, [VH]) s.c. and had the renal blood flow (RBF), glomerular filtration rate (GFR), mean arterial pressure, renal vascular resistance, renal histologic changes, and immunohistochemical features for macrophages and TGF-beta evaluated after 1, 2, and 8 weeks of treatment.
RESULTS
At week 1, despite normal renal hemodynamics and MAP, there was a significant macrophage interstitial influx in CsA-treated rats (70+/-16 vs. 29+/-4 cells+/0.5 mm2, in CsA vs. VH, P=0.02) that was progressive with treatment (80+/-13 vs. 32+/-8 cells+/0.5 mm2, P=0.016 and 197+/-36 vs. 23+/-3 cells+/0.5 mm2, P=0.0002, CsA vs. VH at 2 and 8 weeks, respectively). After 2 weeks of treatment, CsA animals developed a significant interstitial fibrosis, with preserved RBF, even when it was assessed 2 hr after CsA injection. There was a significant increase in the immunostaining for TGF-beta in the juxtaglomerular arterioles in CsA-treated rats (48.6+/-3.8 vs. 35.1+/-1.1%, CsA vs. VH at 2 weeks, P<0.05 and 59.0+/-3.2 vs. 37.0+/-2.1%, CsA vs. VH at 8 weeks, P=0.0001). A significant and progressive GFR decrease followed the renal structural injury of CsA treatment. Arteriolar and glomerular anatomic injury were not found throughout the study.
CONCLUSIONS
Low CsA doses might generate interstitial fibrosis without any decrease in RBF or structural arteriolar lesion evidence, possibly through early macrophage influx and increased TGF-beta expression. It clearly seems that CsA-induced ischemia and tubulointerstitial injury may occur independently, suggesting that chronic CsA nephrotoxicity may be very hard to prevent or even not be preventable at all.
背景
环孢素A(CsA)诱导的慢性肾毒性表现为间质纤维化和入球小动脉玻璃样变性。CsA损伤与肾血管持续收缩和入球小动脉管腔直径变窄有关,导致肾小球前缺血。我们研究了肾血流动力学在CsA诱导的转化生长因子(TGF-β)表达和间质纤维化中的作用。
方法
给低盐饮食的大鼠组皮下注射CsA 5mg/kg/天(CsA组)或溶剂(橄榄油,[VH组]),并在治疗1、2和8周后评估肾血流量(RBF)、肾小球滤过率(GFR)、平均动脉压、肾血管阻力、肾脏组织学变化以及巨噬细胞和TGF-β的免疫组化特征。
结果
在第1周时,尽管肾血流动力学和平均动脉压正常,但CsA处理的大鼠出现了明显的巨噬细胞间质浸润(CsA组与VH组分别为70±16对29±4个细胞/0.5mm²,P = 0.02),且随治疗进展(第2周时分别为80±13对32±8个细胞/0.5mm²,P = 0.016;第8周时分别为197±36对23±3个细胞/0.5mm²,P = 0.0002,CsA组与VH组)。治疗2周后,CsA组动物出现了明显的间质纤维化,RBF保持正常,即使在注射CsA后2小时评估时也是如此。CsA处理的大鼠肾小球旁小动脉中TGF-β的免疫染色显著增加(第2周时CsA组与VH组分别为48.6±3.8%对35.1±1.1%,P < 0.05;第8周时分别为59.0±3.2%对37.0±2.1%,P = 0.0001)。CsA治疗导致肾脏结构损伤后,GFR显著且逐渐下降。在整个研究过程中未发现小动脉和肾小球的解剖学损伤。
结论
低剂量CsA可能在不降低RBF或无小动脉结构损伤证据的情况下产生间质纤维化,可能是通过早期巨噬细胞浸润和TGF-β表达增加。显然,CsA诱导的缺血和肾小管间质损伤可能独立发生,这表明慢性CsA肾毒性可能很难预防,甚至可能根本无法预防。
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