Cole S Hudson, Anirban Roy, Qingtian Li, Aniket S Joshi, Taijun Yin, Ashok Kumar, David Sheikh-Hamad, Vincent H Tam
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A megalin knockout cell line was used as an uptake inhibition control. Methionine was included in selected experiments as an antioxidant control. A polymyxin B concentration-dependent reduction in cell viability was observed. Increased viability was observed in megalin knockout cells following comparable polymyxin B exposures. Compared with polymyxin B exposure alone, concomitant gelofusine significantly increased cell viability as well as reduced LDH release, polymyxin B uptake, mitochondrial superoxide, and apoptosis. Gelofusine and methionine were more effective at reducing renal cell injury in combination than either agent alone. In conclusion, the mechanisms of renal protection by gelofusine involve decreasing cellular drug uptake, reducing subsequent oxidative stress and apoptosis activation. 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引用次数: 0
摘要
导言:多粘菌素是治疗耐多药革兰氏阴性菌感染的最后选择,但它与肾毒性有关。之前有研究表明,在动物模型中,Gelofusine 可减轻多粘菌素相关的肾损伤。然而,肾脏保护机制尚未完全阐明。在此,我们报告了利用细胞培养模型深入了解肾脏保护机制的情况:细胞存活率、多粘菌素 B 吸收、线粒体超氧化物产生、核形态和细胞凋亡活化均在同时使用或不使用凝胶磷脂的情况下进行评估。用巨球蛋白剔除细胞系作为摄取抑制对照。在选定的实验中加入蛋氨酸作为抗氧化剂对照:结果:观察到多粘菌素 B 浓度依赖性降低细胞活力。在暴露于类似的多粘菌素 B 后,观察到megalin 基因剔除细胞的活力增加。与单独暴露于多粘菌素 B 相比,同时暴露于凝胶磷脂和蛋氨酸可显著提高细胞活力,减少线粒体超氧化物的产生,并改善细胞核形态。凝胶磷脂(而非蛋氨酸)能明显减少多粘菌素 B 的吸收和 Bax/Bcl-2 蛋白的比率(内在凋亡的生物标志物)。与单独使用两种药物相比,明胶和蛋氨酸联合使用能更有效地减轻肾细胞损伤:结论:格列福辛对肾脏的保护机制包括降低细胞对药物的吸收、减少随后的氧化应激和细胞凋亡激活。这些发现对于将研究成果转化为减轻药物相关急性肾损伤的临床策略很有价值。
Mechanisms of gelofusine protection in an in vitro model of polymyxin B-associated renal injury.
Polymyxins are a last-resort treatment option for multidrug-resistant gram-negative bacterial infections, but they are associated with nephrotoxicity. Gelofusine was previously shown to reduce polymyxin-associated kidney injury in an animal model. However, the mechanism(s) of renal protection has not been fully elucidated. Here, we report the use of a cell culture model to provide insights into the mechanisms of renal protection. Murine epithelial proximal tubular cells were exposed to polymyxin B. Cell viability, lactate dehydrogenase (LDH) release, polymyxin B uptake, mitochondrial superoxide production, nuclear morphology, and apoptosis activation were evaluated with or without concomitant gelofusine. A megalin knockout cell line was used as an uptake inhibition control. Methionine was included in selected experiments as an antioxidant control. A polymyxin B concentration-dependent reduction in cell viability was observed. Increased viability was observed in megalin knockout cells following comparable polymyxin B exposures. Compared with polymyxin B exposure alone, concomitant gelofusine significantly increased cell viability as well as reduced LDH release, polymyxin B uptake, mitochondrial superoxide, and apoptosis. Gelofusine and methionine were more effective at reducing renal cell injury in combination than either agent alone. In conclusion, the mechanisms of renal protection by gelofusine involve decreasing cellular drug uptake, reducing subsequent oxidative stress and apoptosis activation. These findings would be valuable for translational research into clinical strategies to attenuate drug-associated acute kidney injury.NEW & NOTEWORTHY Gelofusine is a gelatinous saline solution with the potential to attenuate polymyxin-associated nephrotoxicity. We demonstrated that the mechanisms of gelofusine renal protection involve reducing polymyxin B uptake by proximal tubule cells, limiting subsequent oxidative stress and apoptosis activation. In addition, gelofusine was more effective at reducing cellular injury than a known antioxidant control, methionine, and a megalin knockout cell line, indicating that gelofusine likely has additional pharmacological properties besides only megalin inhibition.
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