Possible involvement of oxidative stress in cisplatin-induced apoptosis in LLC-PK1 cells

T. Xiao; S. Choudhary; W. Zhang; Nassem H. Ansari; A. Salahudeen

doi:10.1080/15287390306449

Possible involvement of oxidative stress in cisplatin-induced apoptosis in LLC-PK1 cells

T. Xiao, S. Choudhary, W. Zhang, Nassem H. Ansari, A. Salahudeen

General Internal Medicine

Research output: Contribution to journal › Article › peer-review

77 Scopus citations

Abstract

Use of cisplatin, a chemotherapeutic agent, is associated with toxicity as a significant number of patients develop a decline in renal function. The mechanisms by which cisplatin produces renal injury are not well understood. It has been suggested that free radical-catalyzed lipid peroxidation can induce apoptosis or necrosis leading to renal injury. This study examined whether low concentrations of cisplatin induce apoptosis in LLC-PK1 cells and whether caspases 1, 2, 3, 8, and 9 are activated during this event. Our results show a dose- and time-dependent induction of apoptosis by micromolar concentrations of cisplatin. Expression of oncogenes c-myc and p53 was induced, and except for caspase 1, all the other caspases tested were activated. Z-VAD, the broad-spectrum inhibitor of caspases, prevented caspase activation and apoptosis, but not c-myc and p53 induction. On the other hand, N-acetylcysteine prevented cisplatin-induced apoptosis as well as c-myc induction but not p53 induction. The antioxidant trolox also prevented cisplatin-induced apoptosis. The results suggest that antioxidants and caspase inhibitors may alleviate cisplatin-associated nephrotoxicity.

Original language	English (US)
Pages (from-to)	469-479
Number of pages	11
Journal	Journal of Toxicology and Environmental Health - Part A
Volume	66
Issue number	5
DOIs	https://doi.org/10.1080/15287390306449
State	Published - Mar 14 2003

ASJC Scopus subject areas

Toxicology
Health, Toxicology and Mutagenesis

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title = "Possible involvement of oxidative stress in cisplatin-induced apoptosis in LLC-PK1 cells",

abstract = "Use of cisplatin, a chemotherapeutic agent, is associated with toxicity as a significant number of patients develop a decline in renal function. The mechanisms by which cisplatin produces renal injury are not well understood. It has been suggested that free radical-catalyzed lipid peroxidation can induce apoptosis or necrosis leading to renal injury. This study examined whether low concentrations of cisplatin induce apoptosis in LLC-PK1 cells and whether caspases 1, 2, 3, 8, and 9 are activated during this event. Our results show a dose- and time-dependent induction of apoptosis by micromolar concentrations of cisplatin. Expression of oncogenes c-myc and p53 was induced, and except for caspase 1, all the other caspases tested were activated. Z-VAD, the broad-spectrum inhibitor of caspases, prevented caspase activation and apoptosis, but not c-myc and p53 induction. On the other hand, N-acetylcysteine prevented cisplatin-induced apoptosis as well as c-myc induction but not p53 induction. The antioxidant trolox also prevented cisplatin-induced apoptosis. The results suggest that antioxidants and caspase inhibitors may alleviate cisplatin-associated nephrotoxicity.",

author = "T. Xiao and S. Choudhary and W. Zhang and Ansari, {Nassem H.} and A. Salahudeen",

note = "Funding Information: Received 5 June 2002; accepted 22 July 2002. The work was supported by National Institutes of Health grant EY 13014 and a Lions Eye Bank grant awarded to N. H. Ansari. Address correspondence to Naseem H. Ansari, PhD, Department of Human Biological Chemistry and Genetics, University of Texas Medical Branch, 6.642 Basic Science Bldg., Galveston, TX 77555-0647, USA. E-mail: nansari@utmb.edu",

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AU - Xiao, T.

AU - Choudhary, S.

AU - Zhang, W.

AU - Ansari, Nassem H.

AU - Salahudeen, A.

N1 - Funding Information: Received 5 June 2002; accepted 22 July 2002. The work was supported by National Institutes of Health grant EY 13014 and a Lions Eye Bank grant awarded to N. H. Ansari. Address correspondence to Naseem H. Ansari, PhD, Department of Human Biological Chemistry and Genetics, University of Texas Medical Branch, 6.642 Basic Science Bldg., Galveston, TX 77555-0647, USA. E-mail: nansari@utmb.edu

PY - 2003/3/14

Y1 - 2003/3/14

N2 - Use of cisplatin, a chemotherapeutic agent, is associated with toxicity as a significant number of patients develop a decline in renal function. The mechanisms by which cisplatin produces renal injury are not well understood. It has been suggested that free radical-catalyzed lipid peroxidation can induce apoptosis or necrosis leading to renal injury. This study examined whether low concentrations of cisplatin induce apoptosis in LLC-PK1 cells and whether caspases 1, 2, 3, 8, and 9 are activated during this event. Our results show a dose- and time-dependent induction of apoptosis by micromolar concentrations of cisplatin. Expression of oncogenes c-myc and p53 was induced, and except for caspase 1, all the other caspases tested were activated. Z-VAD, the broad-spectrum inhibitor of caspases, prevented caspase activation and apoptosis, but not c-myc and p53 induction. On the other hand, N-acetylcysteine prevented cisplatin-induced apoptosis as well as c-myc induction but not p53 induction. The antioxidant trolox also prevented cisplatin-induced apoptosis. The results suggest that antioxidants and caspase inhibitors may alleviate cisplatin-associated nephrotoxicity.

AB - Use of cisplatin, a chemotherapeutic agent, is associated with toxicity as a significant number of patients develop a decline in renal function. The mechanisms by which cisplatin produces renal injury are not well understood. It has been suggested that free radical-catalyzed lipid peroxidation can induce apoptosis or necrosis leading to renal injury. This study examined whether low concentrations of cisplatin induce apoptosis in LLC-PK1 cells and whether caspases 1, 2, 3, 8, and 9 are activated during this event. Our results show a dose- and time-dependent induction of apoptosis by micromolar concentrations of cisplatin. Expression of oncogenes c-myc and p53 was induced, and except for caspase 1, all the other caspases tested were activated. Z-VAD, the broad-spectrum inhibitor of caspases, prevented caspase activation and apoptosis, but not c-myc and p53 induction. On the other hand, N-acetylcysteine prevented cisplatin-induced apoptosis as well as c-myc induction but not p53 induction. The antioxidant trolox also prevented cisplatin-induced apoptosis. The results suggest that antioxidants and caspase inhibitors may alleviate cisplatin-associated nephrotoxicity.

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Possible involvement of oxidative stress in cisplatin-induced apoptosis in LLC-PK1 cells

Abstract

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