Biochemical modulation of cisplatin toxicity Journal Article


Authors: Borch, R. F.; Markman, M.
Article Title: Biochemical modulation of cisplatin toxicity
Abstract: The biochemical modulation of cisplatin toxicity has contributed substantially to the safe effective administration of cisplatin in the clinic. In most cases, however, the demonstration of clinical efficacy has preceded the understanding of mechanisms by which these agents provide protection to normal tissues. A number of protocols are now available to ameliorate cisplatin-induced nephrotoxicity; these approaches have been so successful that renal toxicity is rarely of clinical significance today. However, the dramatic escalation in cisplatin dose engendered by the use of modulators has resulted in new dose-limiting toxicities involving the nervous system and the bone marrow. Although preliminary data suggests that certain modulators may reduce these toxicities, extensive clinical trials will also be necessary to determined the optimum scheduling for the newer agents and to provide convincing evidence of efficacy in man. Finally, modulator combinations (i.e. DDTC and hypertonic saline) have the potential to provide the broadest coverage of normal tissue protection and appear to merti more extensive clinical investigation. Cisplatin has demonstrated remarkable clinical efficacy at currently tolerated doses; further advances in the biochemical modulation of cisplatin toxicity should provide significant therapeutic gains for this important drug in the future. © 1989.
Keywords: clinical article; review; cisplatin; animal; nephrotoxicity; rats; drug toxicity; mesna; drug interactions; amifostine; glutathione; intravenous drug administration; bone marrow toxicity; probenecid; sodium thiosulfate; human; priority journal; central nervous system toxicity; diethyldithiocarbamic acid
Journal Title: Pharmacology & Therapeutics
Volume: 41
Issue: 1-2
ISSN: 0163-7258
Publisher: Elsevier Inc.  
Date Published: 1989-01-01
Start Page: 371
End Page: 380
Language: English
DOI: 10.1016/0163-7258(89)90114-9
PUBMED: 2652155
PROVIDER: scopus
DOI/URL:
Notes: Article -- Export Date: 14 April 2020 -- Source: Scopus
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  1. Maurie Markman
    124 Markman