N-acetylcysteine suppresses colistimethate sodium-induced nephrotoxicity via activation of SOD2, eNOS, and MMP3 protein expressions

Ceylan, Bahadır; Ozansoy, Mehmet; Kılıç, Ülkan; Yozgat, Yasemin; Ercan, Çilem; Yıldız, Pelin; Aslan, Turan

doi:10.1080/0886022x.2018.1489286

Cited by 22 publications

(11 citation statements)

References 50 publications

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“…35 NAC was also able to promote overexpression of SOD2, endothelial nitric oxide synthase (eNOS) and matrix metalloproteinase 3 (MMP3) in rat kidneys. 36 In agreement with our results, previous studies also showed that tempol upregulated SOD2 activity and that this increase was accompanied by oxidative stress reduction. 37,38 Tempol can act by catalysing superoxide anion, promoting an increased hydroxyl radical (OH) level generation from hydrogen peroxide (H2O2).…”

Section: Discussionsupporting

confidence: 93%

Tempol improves redox status in mdx dystrophic diaphragm muscle

Hermes

Mizobuti

Rocha

et al. 2020

Int J Experimental Path

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Several studies have demonstrated that oxidative stress plays a critical function in the pathogenesis of Duchenne muscular dystrophy (DMD). 1-3 DMD is the most frequent and lethal muscular dystrophy, affecting 1 in 3000-6000 male children, 3 and at present, there is no efficient therapy for this dystrophy. 4 Mitochondria are one of the main sources of reactive oxygen species (ROS). Hydroxyl radical, superoxide anion, hydrogen peroxide and singlet oxygen constitute the ROS, and when produced in excess or not properly controlled, it becomes toxic. 5,6 There is feed-forward looping; the high levels of ROS produced by the mitochondrial electron transport chain damage the mitochondria and consequently lead to even greater production of ROS and mitochondrial injury. 6

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Section: Discussionsupporting

confidence: 93%

Tempol improves redox status in mdx dystrophic diaphragm muscle

Hermes

Mizobuti

Rocha

et al. 2020

Int J Experimental Path

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“…CMS for 10 days SCr, urine NAG, TOS, TAS, OSI, eNOS, SOD2, MMP, renal apoptosis (by TUNEL assay), renal histology examination Reversed colistin-induced negative effects, as determined by increased SCr, urine NAG, apoptosis index, and renal histological damage score as well as by decreased renal expression levels of eNOS, SOD2, and MMP [ 110 ] Silymarin Rats 50 mg/kg I.V silymarin twice a day 2 h before polymyxin E injection for 7 days A cumulative dose of 36.5 mg/kg I.V. polymyxin E given twice a day, 8 h apart, for 7 days Histological, ultrastructural, and morphometric changes Alleviated the degenerative changes on the rat kidney induced by polymyxin E [ 111 ] Silymarin Rats 50 mg/kg I.V silymarin twice a day 2 h before polymyxin E injection for 7 days A cumulative dose of 36.5 mg/kg I.V. polymyxin E given twice a day, 8 h apart, for 7 days SCr, serum urea, serum UA, serum Na, serum K, ameliorated the biochemical changes induced by polymyxin E in rats including elevated urinary NAG and serum levels of urea, creatinine, uric acid, sodium, and potassium.…”

Section: Methodsmentioning

confidence: 99%

“…However, no significant differences were observed between the study groups regarding the renal total antioxidant and oxidant capacity. Thus, the researchers proposed that NAC exerted its beneficial effects through the activation of SOD2 and eNOS expression levels as well as MMP3 [ 111 ].…”

Section: Methodsmentioning

confidence: 99%

Pharmacological agents for the prevention of colistin-induced nephrotoxicity

2022

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Background Colistin is a polymyxin antibiotic which has been used for treatment of Gram-negative infections, but it was withdrawn due to its nephrotoxicity. However, colistin has gained its popularity in recent years due to the reemergence of multidrug resistant Gram-negative infections and drug-induced toxicity is considered as the main obstacle for using this valuable antibiotic. Results In total, 30 articles, including 29 animal studies and one clinical trial were included in this study. These compounds, including aged black garlic extract, albumin fragments, alpha lipoic acid, astaxanthin, baicalein, chrysin, cilastatin, colchicine, curcumin, cytochrome c, dexmedetomidine, gelofusine, grape seed proanthocyanidin extract, hesperidin, luteolin, lycopene, melatonin, methionine, N-acetylcysteine, silymarin, taurine, vitamin C, and vitamin E exhibited beneficial effects in most of the published works. Conclusions In this review, the authors have attempted to review the available literature on the use of several compounds for prevention or attenuation of colistin-induced nephrotoxicity. Most of the studied compounds were potent antioxidants, and it seems that using antioxidants concomitantly can have a protective effect during the colistin exposure.

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“…Overall, the concomitant use of these agents with polymyxins has led to the reduced production of inflammatory and oxidative stress biomarkers [103,104,105,106]. Attenuation of both cellular apoptosis and histopathological changes in mice kidneys has been shown as well [103,105,107,108,109]. Nevertheless, not all studies have shown significant changes in serum creatinine values when comparing polymyxins prescribed alone or combined with anti-oxidant drugs [106,110], possibly because after a renal insult, there is a delay in the response of the serum creatinine concentration.…”

Section: Other Strategies To Reduce Nephrotoxicitymentioning

confidence: 99%

Polymyxin Acute Kidney Injury: Dosing and Other Strategies to Reduce Toxicity

et al. 2019

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Polymyxins are valuable antimicrobials for the management of multidrug-resistant Gram-negative bacteria; however, nephrotoxicity associated with these drugs is a very common side effect that occurs during treatment. This article briefly reviews nephrotoxic mechanisms and risk factors for polymyxin-associated acute kidney injury (AKI) and discusses dosing strategies that may mitigate kidney damage without compromising antimicrobial activity. Polymyxins have a very narrow therapeutic window and patients requiring treatment with these drugs are frequently severely ill and have multiple comorbidities, which increases the risk of AKI. Notably, there is a significant overlap between therapeutic and toxic plasma polymyxin concentrations that substantially complicates dose selection. Recent dosing protocols for both colistin and polymyxin B have been developed and may help fine tune dose adjustment of these antibiotics. Minimizing exposure to modifiable risk factors, such as other nephrotoxic agents, is strongly recommended. The dose should be carefully selected, particularly in high-risk patients. The administration of oxidative stress-reducing drugs is a promising strategy to ameliorate polymyxin-associated AKI, but still requires support from clinical studies.

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N-acetylcysteine suppresses colistimethate sodium-induced nephrotoxicity via activation of SOD2, eNOS, and MMP3 protein expressions

Cited by 22 publications

References 50 publications

Tempol improves redox status in mdx dystrophic diaphragm muscle

Tempol improves redox status in mdx dystrophic diaphragm muscle

Pharmacological agents for the prevention of colistin-induced nephrotoxicity

Polymyxin Acute Kidney Injury: Dosing and Other Strategies to Reduce Toxicity

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