Protection against Cisplatin-Induced Toxicities by N-Acetylcysteine and Sodium Thiosulfate as Assessed at the Molecular, Cellular, and in Vivo Levels

doi:10.1124/jpet.105.087601

QUICK SEARCH:

[advanced]

	Author:		Keyword(s):
Year:		Vol:		Page:

Journal of Pharmacology And Experimental Therapeutics Fast Forward
First published on June 10, 2005; DOI: 10.1124/jpet.105.087601

0022-3565/05/3143-1052-1058$20.00
JPET 314:1052-1058, 2005

This Article

	Full Text
	Full Text (PDF)
	All Versions of this Article: jpet.105.087601v1 314/3/1052 most recent
	Submit a response
	Alert me when this article is cited
	Alert me when eLetters are posted
	Alert me if a correction is posted
	Citation Map

Services

	Similar articles in this journal
	Similar articles in PubMed
	Alert me to new issues of the journal
	Download to citation manager

Citing Articles

	Citing Articles via HighWire
	Citing Articles via Google Scholar

Google Scholar

	Articles by Dickey, D. T.
	Articles by Neuwelt, E. A.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Dickey, D. T.
	Articles by Neuwelt, E. A.

GASTROINTESTINAL, HEPATIC, PULMONARY, AND RENAL

Protection against Cisplatin-Induced Toxicities by N-Acetylcysteine and Sodium Thiosulfate as Assessed at the Molecular, Cellular, and in Vivo Levels

D. Thomas Dickey, Y. Jeffrey Wu, Leslie L. Muldoon, and Edward A. Neuwelt

Oregon Health & Science University, Department of Neurology (D.T.D., Y.J.W., L.L.M., E.A.N.); and Department of Veterans Affairs (E.A.N.), Portland, Oregon

Cisplatin (CDDP) is a common, highly toxic chemotherapeuticagent. This study investigates chemoprotective effects of N-acetylcysteine(NAC) and sodium thiosulfate (STS) on in vitro and in vivo CDDPtoxicities. For ototoxicity studies, CDDP (6 mg/kg) was administeredto rats via a retrograde carotid artery infusion. Auditory brainstemresponse thresholds at 4 to 20 kHz were tested before and 7days post-treatment. STS (8 g/m² i.v.) was administered at 4,8, or 12 h after CDDP. For nephrotoxicity studies, rats weretreated with CDDP intraperitoneally (10 mg/kg) before or afterNAC (400 mg/kg) or STS (8 g/m²), and blood urea nitrogen (BUN)and creatinine concentrations were measured after 3 days. Invitro cytotoxicity and chemoprotection in human tumor cell lineswere assessed by cell viability and immunoblotting assays. Ratstreated with STS 4 h after CDDP exhibited no hearing change.The STS 8-h group had less otoprotection, whereas 12-h ratshad ototoxicity. CDDP induced high BUN and creatinine, correspondingto renal tubule toxicities. All NAC-treated animals showed normalBUN and reduced creatinine levels compared with CDDP alone andno histopathological evidence of nephrotoxicity. Delayed STStreatment was not consistently protective against nephrotoxicity.STS administration fully protected against the in vitro cytotoxicand apoptotic effects of CDDP if added within 2 h of CDDP, butchemoprotection decreased if STS administration was 4 h, andwas minimal by 6 h, after CDDP. Thus, the chemoprotection routeand timing of administration can be manipulated to maintainCDDP antitumor efficacy while protecting against toxicities.

Received for publication April 6, 2005
Accepted June 9, 2005.

Address correspondence to: Dr. Edward A. Neuwelt, L603, 3181 SW Sam Jackson Park Rd., Portland, OR 97239. E-mail: neuwelte{at}ohsu.edu

This article has been cited by other articles:

D. R. Freyer, L. Sung, and G. H. Reaman
Prevention of Hearing Loss in Children Receiving Cisplatin Chemotherapy
J. Clin. Oncol., January 10, 2009; 27(2): 317 - 318.
[Full Text] [PDF]

A. Singh, S. Boldin-Adamsky, R. K. Thimmulappa, S. K. Rath, H. Ashush, J. Coulter, A. Blackford, S. N. Goodman, F. Bunz, W. H. Watson, et al.
RNAi-Mediated Silencing of Nuclear Factor Erythroid-2-Related Factor 2 Gene Expression in Non-Small Cell Lung Cancer Inhibits Tumor Growth and Increases Efficacy of Chemotherapy
Cancer Res., October 1, 2008; 68(19): 7975 - 7984.
[Abstract] [Full Text] [PDF]

M. Fouladi, M. Chintagumpala, D. Ashley, S. Kellie, S. Gururangan, T. Hassall, L. Gronewold, C. F. Stewart, D. Wallace, A. Broniscer, et al.
Amifostine Protects Against Cisplatin-Induced Ototoxicity in Children With Average-Risk Medulloblastoma
J. Clin. Oncol., August 1, 2008; 26(22): 3749 - 3755.
[Abstract] [Full Text] [PDF]

J. Luo, T. Tsuji, H. Yasuda, Y. Sun, Y. Fujigaki, and A. Hishida
The molecular mechanisms of the attenuation of cisplatin-induced acute renal failure by N-acetylcysteine in rats
Nephrol. Dial. Transplant., July 1, 2008; 23(7): 2198 - 2205.
[Abstract] [Full Text] [PDF]

T. M. Harned, O. Kalous, A. Neuwelt, J. Loera, L. Ji, P. Iovine, R. Sposto, E. A. Neuwelt, and C. P. Reynolds
Sodium Thiosulfate Administered Six Hours after Cisplatin Does Not Compromise Antineuroblastoma Activity
Clin. Cancer Res., January 15, 2008; 14(2): 533 - 540.
[Abstract] [Full Text] [PDF]

C. L. Zuur, Y. J. Simis, P. E. Lansdaal, A. A. Hart, J. H. Schornagel, W. A. Dreschler, C. R. Rasch, and A. J. Balm
Ototoxicity in a Randomized Phase III Trial of Intra-Arterial Compared With Intravenous Cisplatin Chemoradiation in Patients With Locally Advanced Head and Neck Cancer
J. Clin. Oncol., August 20, 2007; 25(24): 3759 - 3765.
[Abstract] [Full Text] [PDF]

P. Videhult, G. Laurell, I. Wallin, and H. Ehrsson
Kinetics of Cisplatin and its monohydrated complex with sulfur-containing compounds designed for local otoprotective administration.
Experimental Biology and Medicine, November 1, 2006; 231(10): 1638 - 1645.
[Abstract] [Full Text] [PDF]

J. H. Doroshow
Redox modulation of chemotherapy-induced tumor cell killing and normal tissue toxicity.
J Natl Cancer Inst, February 15, 2006; 98(4): 223 - 225.
[Full Text] [PDF]

				A. Singh, S. Boldin-Adamsky, R. K. Thimmulappa, S. K. Rath, H. Ashush, J. Coulter, A. Blackford, S. N. Goodman, F. Bunz, W. H. Watson, et al. RNAi-Mediated Silencing of Nuclear Factor Erythroid-2-Related Factor 2 Gene Expression in Non-Small Cell Lung Cancer Inhibits Tumor Growth and Increases Efficacy of Chemotherapy Cancer Res., October 1, 2008; 68(19): 7975 - 7984. [Abstract] [Full Text] [PDF]

				M. Fouladi, M. Chintagumpala, D. Ashley, S. Kellie, S. Gururangan, T. Hassall, L. Gronewold, C. F. Stewart, D. Wallace, A. Broniscer, et al. Amifostine Protects Against Cisplatin-Induced Ototoxicity in Children With Average-Risk Medulloblastoma J. Clin. Oncol., August 1, 2008; 26(22): 3749 - 3755. [Abstract] [Full Text] [PDF]

				J. Luo, T. Tsuji, H. Yasuda, Y. Sun, Y. Fujigaki, and A. Hishida The molecular mechanisms of the attenuation of cisplatin-induced acute renal failure by N-acetylcysteine in rats Nephrol. Dial. Transplant., July 1, 2008; 23(7): 2198 - 2205. [Abstract] [Full Text] [PDF]

				T. M. Harned, O. Kalous, A. Neuwelt, J. Loera, L. Ji, P. Iovine, R. Sposto, E. A. Neuwelt, and C. P. Reynolds Sodium Thiosulfate Administered Six Hours after Cisplatin Does Not Compromise Antineuroblastoma Activity Clin. Cancer Res., January 15, 2008; 14(2): 533 - 540. [Abstract] [Full Text] [PDF]

				C. L. Zuur, Y. J. Simis, P. E. Lansdaal, A. A. Hart, J. H. Schornagel, W. A. Dreschler, C. R. Rasch, and A. J. Balm Ototoxicity in a Randomized Phase III Trial of Intra-Arterial Compared With Intravenous Cisplatin Chemoradiation in Patients With Locally Advanced Head and Neck Cancer J. Clin. Oncol., August 20, 2007; 25(24): 3759 - 3765. [Abstract] [Full Text] [PDF]

				P. Videhult, G. Laurell, I. Wallin, and H. Ehrsson Kinetics of Cisplatin and its monohydrated complex with sulfur-containing compounds designed for local otoprotective administration. Experimental Biology and Medicine, November 1, 2006; 231(10): 1638 - 1645. [Abstract] [Full Text] [PDF]

				J. H. Doroshow Redox modulation of chemotherapy-induced tumor cell killing and normal tissue toxicity. J Natl Cancer Inst, February 15, 2006; 98(4): 223 - 225. [Full Text] [PDF]