Literature DB >> 10591510

L- and D- methionine provide equivalent long term protection against CDDP-induced ototoxicity in vivo, with partial in vitro and in vivo retention of antineoplastic activity.

D Reser1, M Rho, D Dewan, L Herbst, G Li, H Stupak, K Zur, J Romaine, D Frenz, L Goldbloom, R Kopke, J Arezzo, T Van De Water.   

Abstract

Treatment of metastatic tumors with ionic platinum compounds is hampered by the potent nephrotoxic, ototoxic and neurotoxic properties of these drugs. Recent studies have shown that sulfur-containing antioxidants relieve the dose limiting side effects of cis-diamminedichloroplatinum (CDDP), the most commonly used ionic platinum therapy. Here we report that both isomers of the sulfur-containing antioxidant methionine (MET) completely block the in vivo ototoxic and nephrotoxic effects of CDDP, and the duration of MET otoprotection is longer than has been previously reported. Rats treated with either L- or D-MET in addition to CDDP exhibited no signs of auditory system damage after 7 days, as evaluated by the auditory brainstem response and scanning electron microscopic examination of the organ of Corti, while CDDP-treated rats exhibited pronounced evidence of ototoxic damage after only 3 days. Microscopic examination of kidney tissue revealed moderate to severe nephrotoxic damage to CDDP-treated rats after 5 days, while rats co-treated with either MET isomer showed no evidence of kidney damage. Mortality among CDDP-treated subjects increased steadily over the period of the study, while all of the MET-protected rats survived. Finally, the efficacy of CDDP in the presence of L- or D-MET was evaluated in vitro using cultures of MTLN-3 breast tumor cell lines, and in vivo using implanted MTLN-3 tumors. Both L- and D-MET reduced the ability of CDDP to kill tumor cells in vitro and in vivo, however, our data suggest that a higher proportion of the antineoplastic activity of CDDP is retained in the presence of L- MET.

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Year:  1999        PMID: 10591510

Source DB:  PubMed          Journal:  Neurotoxicology        ISSN: 0161-813X            Impact factor:   4.294


  9 in total

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3.  d-Methionine reduces tobramycin-induced ototoxicity without antimicrobial interference in animal models.

Authors:  Daniel J Fox; Morris D Cooper; Cristian A Speil; Melissa H Roberts; Susan C Yanik; Robert P Meech; Tim L Hargrove; Steven J Verhulst; Leonard P Rybak; Kathleen C M Campbell
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4.  The protective effect of aspirin-induced temporary threshold shift in an animal model of cisplatin-related ototoxicity.

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5.  Protection against cisplatin ototoxicity in a Sprague-Dawley rat animal model.

Authors:  P Giordano; G Lorito; A Ciorba; A Martini; S Hatzopoulos
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6.  Cisplatin-induced hair cell death requires STAT1 and is attenuated by epigallocatechin gallate.

Authors:  Nicole C Schmitt; Edwin W Rubel; Neil M Nathanson
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7.  Dose-dependent protection on cisplatin-induced ototoxicity - an electrophysiological study on the effect of three antioxidants in the Sprague-Dawley rat animal model.

Authors:  Guiscardo Lorito; Stavros Hatzopoulos; Göran Laurell; Kathleen C M Campbell; Joseph Petruccelli; Pietro Giordano; Krzysztof Kochanek; Lech Sliwa; Alessandro Martini; Henryk Skarzynski
Journal:  Med Sci Monit       Date:  2011-08

8.  Attenuation of progressive hearing loss in DBA/2J mice by reagents that affect epigenetic modifications is associated with up-regulation of the zinc importer Zip4.

Authors:  Hideki Mutai; Fuyuki Miya; Masato Fujii; Tatsuhiko Tsunoda; Tatsuo Matsunaga
Journal:  PLoS One       Date:  2015-04-14       Impact factor: 3.240

Review 9.  Progress in the Development of Preventative Drugs for Cisplatin-Induced Hearing Loss.

Authors:  Robert A Hazlitt; Jaeki Min; Jian Zuo
Journal:  J Med Chem       Date:  2018-02-01       Impact factor: 7.446

  9 in total

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