Water-soluble coenzyme Q(10) provides better protection than lipid-soluble coenzyme Q(10) in a rat model of chronic tacrolimus nephropathy

Authors
Cui, ShengLuo, KangQuan, YiLim, Sun WooShin, Yoo JinLee, Kyung EunKim, Hong LimKo, Eun JeongKim, Ju HwanChung, Sang J.Bae, Soo KyungHa Chung, ByungYang, Chul Woo
Issue Date
2021-07
Publisher
KOREAN ASSOC INTERNAL MEDICINE
Citation
KOREAN JOURNAL OF INTERNAL MEDICINE, v.36, no.4, pp.949 - 961
Abstract
Background/Aims: Coenzyme Q(10 )(CoQ(10)), is a promising antioxidant; however, low bioavailability owing to lipid-solubility is a limiting factor. We developed water-soluble COQ(10) (CoQ(10)-W) and compared its effects with conventional lipid-soluble CoQ(10) (CoQ(10) -L) in an experimental model of chronic tacrolimus (Tac) nephropathy. Methods: CoQ(10) -W was developed from a glycyrrhizic-carnitine mixed layer CoQ(10) micelle based on acyltransferases. Chronic nephropathy was induced in rats with 28-day Tac treatment; they were concomitantly treated with CoQ(10) -L or CoQ(10) -W. CoQ(10) level in plasma and kidney were measured using liquid chromatography-mass spectrometry. CoQ(10) -W and CoQ(10) -L effects on Tac-induced nephropathy were assessed in terms of renal function, histopathology, oxidative stress, and apoptotic cell death. Their effects on cell viability and reactive oxygen species (ROS) production were assessed in cultured proximal tubular cells, human kidney 2 (HK-2) cells. Results: The plasma CoQ(10) level was significantly higher in the CoQ(10) -W group than in the CoQ(10)-L group. Tac treatment caused renal dysfunction, typical pathologic lesions, and oxidative stress markers. Serum creatinine was restored in the Tac + CoQ(10) -L or CoQ(10) -W groups compared with that in the Tac group. CoQ(10) -W administration reduced oxidative stress and apoptosis markers. Mitochondrial ultrastructure assessment revealed that the addition of CoQ(10) -L or CoQ(10)-W with Tac increased mitochondrial size and number than Tac treatment alone. In vitro investigations revealed that both CoQ(10) -L and CoQ(10)-W improved cell viability and reduced ROS production in the Tac-induced HK-2 cell injury. Conclusions: CoQ(10) -W has a better therapeutic effect in Tac-induced renal injury than conventional CoQ(10) -L, possibly associated with improved CoQ(10) bioavailability.
Keywords
CHRONIC CYCLOSPORINE NEPHROPATHY; EXPRESSION; KLOTHO; CHRONIC CYCLOSPORINE NEPHROPATHY; EXPRESSION; KLOTHO; Tacrolimus; Coenzyme Q(10); Water-soluble coenzyme Q(10); Kidney; Oxidative stress
ISSN
1226-3303
URI
https://pubs.kist.re.kr/handle/201004/116714
DOI
10.3904/kjim.2020.211
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KIST Article > 2021
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