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Lack of experimental vesicant activity for the anticancer agents cisplatin,melphalan, and mitoxantrone
Authors:Robert T. Dorr  David S. Alberts  Michelle Soble
Affiliation:(1) Arizona Cancer Center, The University of Arizona, Tucson, AZ, USA;(2) Internal Medicine, The University of Arizona, Tucson, AZ, USA
Abstract:
Summary Cisplatin and L-PAM are DNA-crosslinking anticancer agents which have not been systematically studied for vesicant potential. Mitoxantrone is a new active anthracene-based, DNA intercalator which is undergoing widespread clinical testing for antitumor efficacy in man. These three agents were tested for vesicant activity in dehaired BALB/c mice given ID injections equivalent to human clinical doses. Neither cisplatin (up to 150 mg/m2) nor L-PAM (up to 71 mg/m2) produced any skin necrosis in the mice. The L-PAM solvent (acid/alcohol in propylene glycol) was ulcerogenic if injected undiluted. Mitoxantrone (up to 14 mg/m2) was not ulcerogenic in the mice, although the skin site retained a blue drug discoloration for several weeks. It is concluded that in clinically relevant doses, cisplatin, L-PAM, and mitoxantrone are not vesicants.Supported in part by Public Health Service grants CA-23074, CA-31078 and CA-17094 from the National Cancer Institute, Department of Health and Human Services, Bethesda, MD
Keywords:
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