P53 Contributes to Cisplatin Induced Renal Oxidative Damage via Regulating P66shc and MnSOD

P53 Contributes to Cisplatin Induced Renal Oxidative Damage via Regulating P66shc and MnSOD

Background/Aims: Cisplatin is widely used to treat malignancies. However, its major limitation is the development of dose-dependent nephrotoxicity. The precise mechanisms of cisplatin-induced kidney damage remain unclear. Previous study demonstrated the central role of mitochondrial ROS (mtROS) in t...

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Main Authors: Yanggang Yuan, Hui Wang, Yingyi Wu, Bo Zhang, Ningning Wang, Huijuan Mao, Changying Xing
Format: Article
Language:English
Published: Cell Physiol Biochem Press GmbH & Co KG 2015-10-01
Series:Cellular Physiology and Biochemistry
Subjects:
p53
MnSOD
p66shc
Cisplatin nephrotoxicity
Online Access:http://www.karger.com/Article/FullText/430247
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spelling doaj-610e9060f2f746f8bd9b48a02520eaa82020-11-25T01:39:52ZengCell Physiol Biochem Press GmbH & Co KGCellular Physiology and Biochemistry1015-89871421-97782015-10-013741240125610.1159/000430247430247P53 Contributes to Cisplatin Induced Renal Oxidative Damage via Regulating P66shc and MnSODYanggang YuanHui WangYingyi WuBo ZhangNingning WangHuijuan MaoChangying XingBackground/Aims: Cisplatin is widely used to treat malignancies. However, its major limitation is the development of dose-dependent nephrotoxicity. The precise mechanisms of cisplatin-induced kidney damage remain unclear. Previous study demonstrated the central role of mitochondrial ROS (mtROS) in the pathogenesis of cisplatin nephrotoxicity. The purpose of this study was to explore the mechanism of mtROS regulation in cisplatin nephrotoxicity. Methods: p53, MnSOD and p66shc were detected at mRNA and protein levels by qPCR and western blot in HK2 cells. mtROS levels were determined by DCFDA and MitoSOX staining. Cell viability and cell apoptosis were accessed by CCK-8 assay, TUNEL assay and flow cytometry, respectivesly. siRNAs were used to knock down p53 and p66shc expression and subsequent changes were observed. In vivo assays using a mouse model of cisplatin-induced acute kidney injury were used to validate the in vitro results. Results: In HK2 cells, cisplatin exposure decreased the MnSOD and increased the expression of p53 and p66shc. MnTBAP, a MnSOD mimic, blocked cisplatin-induced the generation of mtROS and cell injury. P66shc and p53 siRNAs rendered renal cells resistant to cisplatin-induced mtROS production and cell death. Furthermore, knockdown of p53 restored MnSOD and inhibiting p66shc. Consistent with these results, we revealed that p53 inhibitor reduced cisplatin-induced oxidative stress and apoptosis by regulating MnSOD and p66shc in the kidney of cisplatin-treated mice. Conclusion: Our study identifies activation of p53 signalling as a potential strategy for reducing the nephrotoxicity associated with cisplatin treatments and, as a result, broadens the therapeutic window of this chemotherapeutic agent.http://www.karger.com/Article/FullText/430247p53MnSODp66shcCisplatin nephrotoxicity
collection DOAJ
language English
format Article
sources DOAJ
author Yanggang Yuan
Hui Wang
Yingyi Wu
Bo Zhang
Ningning Wang
Huijuan Mao
Changying Xing
spellingShingle Yanggang Yuan
Hui Wang
Yingyi Wu
Bo Zhang
Ningning Wang
Huijuan Mao
Changying Xing
P53 Contributes to Cisplatin Induced Renal Oxidative Damage via Regulating P66shc and MnSOD
Cellular Physiology and Biochemistry
p53
MnSOD
p66shc
Cisplatin nephrotoxicity
author_facet Yanggang Yuan
Hui Wang
Yingyi Wu
Bo Zhang
Ningning Wang
Huijuan Mao
Changying Xing
author_sort Yanggang Yuan
title P53 Contributes to Cisplatin Induced Renal Oxidative Damage via Regulating P66shc and MnSOD
title_short P53 Contributes to Cisplatin Induced Renal Oxidative Damage via Regulating P66shc and MnSOD
title_full P53 Contributes to Cisplatin Induced Renal Oxidative Damage via Regulating P66shc and MnSOD
title_fullStr P53 Contributes to Cisplatin Induced Renal Oxidative Damage via Regulating P66shc and MnSOD
title_full_unstemmed P53 Contributes to Cisplatin Induced Renal Oxidative Damage via Regulating P66shc and MnSOD
title_sort p53 contributes to cisplatin induced renal oxidative damage via regulating p66shc and mnsod
publisher Cell Physiol Biochem Press GmbH & Co KG
series Cellular Physiology and Biochemistry
issn 1015-8987
1421-9778
publishDate 2015-10-01
description Background/Aims: Cisplatin is widely used to treat malignancies. However, its major limitation is the development of dose-dependent nephrotoxicity. The precise mechanisms of cisplatin-induced kidney damage remain unclear. Previous study demonstrated the central role of mitochondrial ROS (mtROS) in the pathogenesis of cisplatin nephrotoxicity. The purpose of this study was to explore the mechanism of mtROS regulation in cisplatin nephrotoxicity. Methods: p53, MnSOD and p66shc were detected at mRNA and protein levels by qPCR and western blot in HK2 cells. mtROS levels were determined by DCFDA and MitoSOX staining. Cell viability and cell apoptosis were accessed by CCK-8 assay, TUNEL assay and flow cytometry, respectivesly. siRNAs were used to knock down p53 and p66shc expression and subsequent changes were observed. In vivo assays using a mouse model of cisplatin-induced acute kidney injury were used to validate the in vitro results. Results: In HK2 cells, cisplatin exposure decreased the MnSOD and increased the expression of p53 and p66shc. MnTBAP, a MnSOD mimic, blocked cisplatin-induced the generation of mtROS and cell injury. P66shc and p53 siRNAs rendered renal cells resistant to cisplatin-induced mtROS production and cell death. Furthermore, knockdown of p53 restored MnSOD and inhibiting p66shc. Consistent with these results, we revealed that p53 inhibitor reduced cisplatin-induced oxidative stress and apoptosis by regulating MnSOD and p66shc in the kidney of cisplatin-treated mice. Conclusion: Our study identifies activation of p53 signalling as a potential strategy for reducing the nephrotoxicity associated with cisplatin treatments and, as a result, broadens the therapeutic window of this chemotherapeutic agent.
topic p53
MnSOD
p66shc
Cisplatin nephrotoxicity
url http://www.karger.com/Article/FullText/430247
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