TGF-β 介导体 NADPH 氧化酶 4 依赖性氧化应激促进黏菌素诱导的急性肾损伤。
TGF-β-mediated NADPH oxidase 4-dependent oxidative stress promotes colistin-induced acute kidney injury.
机构信息
Department of Pharmacology, College of Medicine, Konyang University, Daejeon, Korea.
Department of Veterinary Medicine, Institute of Veterinary Science, Chungnam National University, Daejeon, Korea.
出版信息
J Antimicrob Chemother. 2018 Apr 1;73(4):962-972. doi: 10.1093/jac/dkx479.
BACKGROUND
Colistin (polymyxin E) is an important constituent of the polymyxin class of cationic polypeptide antibiotics. Intrarenal oxidative stress can contribute to colistin-induced nephrotoxicity. Nicotinamide adenine dinucleotide 3-phosphate oxidases (Noxs) are important sources of reactive oxygen species. Among the various types of Noxs, Nox4 is predominantly expressed in the kidney.
OBJECTIVES
We investigated the role of Nox4 and benefit of Nox4 inhibition in colistin-induced acute kidney injury using in vivo and in vitro models.
METHODS
Human proximal tubular epithelial (HK-2) cells were treated with colistin with or without NOX4 knockdown, or GKT137831 (most specific Nox1/4 inhibitor). Effects of Nox4 inhibition on colistin-induced acute kidney injury model in Sprague-Dawley rats were examined.
RESULTS
Nox4 expression in HK-2 cells significantly increased following colistin exposure. SB4315432 (transforming growth factor-β1 receptor I inhibitor) significantly inhibited Nox4 expression in HK-2 cells. Knockdown of NOX4 transcription reduced reactive oxygen species production, lowered the levels of pro-inflammatory markers (notably mitogen-activated protein kinases) implicated in colistin-induced nephrotoxicity and attenuated apoptosis by altering Bax and caspase 3/7 activity. Pretreatment with GKT137831 replicated these effects mediated by downregulation of mitogen-activated protein kinase activities. In a rat colistin-induced acute kidney injury model, administration of GKT137831 resulted in attenuated colistin-induced acute kidney injury as indicated by attenuated impairment of glomerulus function, preserved renal structures, reduced expression of 8-hydroxyguanosine and fewer apoptotic cells.
CONCLUSIONS
Collectively, these findings identify Nox4 as a key source of reactive oxygen species responsible for kidney injury in colistin-induced nephrotoxicity and highlight a novel potential way to treat drug-related nephrotoxicity.
背景
黏菌素(多粘菌素 E)是一类阳离子多肽抗生素中的重要组成部分。肾内氧化应激可能导致黏菌素诱导的肾毒性。烟酰胺腺嘌呤二核苷酸 3-磷酸氧化酶(Noxs)是活性氧的重要来源。在各种类型的 Noxs 中,Nox4 主要在肾脏中表达。
目的
我们通过体内和体外模型研究了 Nox4 在黏菌素诱导的急性肾损伤中的作用和 Nox4 抑制的益处。
方法
用黏菌素处理人近端肾小管上皮(HK-2)细胞,并用 Nox4 敲低或 GKT137831(最特异的 Nox1/4 抑制剂)处理。在 Sprague-Dawley 大鼠中检查 Nox4 抑制对黏菌素诱导的急性肾损伤模型的影响。
结果
黏菌素暴露后 HK-2 细胞中 Nox4 的表达明显增加。SB4315432(转化生长因子-β1 受体 I 抑制剂)显著抑制 HK-2 细胞中 Nox4 的表达。NOX4 转录的敲低减少了活性氧的产生,降低了与黏菌素诱导的肾毒性有关的促炎标志物(特别是丝裂原活化蛋白激酶)的水平,并通过改变 Bax 和 caspase 3/7 活性来减轻细胞凋亡。GKT137831 的预处理复制了这些通过下调丝裂原活化蛋白激酶活性介导的作用。在大鼠黏菌素诱导的急性肾损伤模型中,GKT137831 的给药导致黏菌素诱导的急性肾损伤减弱,表现为肾小球功能损伤减轻、肾脏结构保存、8-羟基鸟嘌呤表达减少和凋亡细胞减少。
结论
总之,这些发现确定了 Nox4 作为活性氧的关键来源,负责黏菌素诱导的肾毒性中的肾损伤,并强调了一种治疗与药物相关的肾毒性的新的潜在方法。
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