Evaluation of the genotoxicity of cis-bis(3-aminoflavone)dichloroplatinum(II) in comparison with cis-DDP [An article from: Mut.Res.-Genetic Toxicology and Environmental Mutagenesis]

Name: Evaluation of the genotoxicity of cis-bis(3-aminoflavone)dichloroplatinum(II) in comparison with cis-DDP [An article from: Mut.Res.-Genetic Toxicology and Environmental Mutagenesis]
Author: B. Kosmider, K. Wyszynska, E. Janik-Spiechowicz, O
ISBN: 978B000RQZ2J0

Author B. Kosmider, K. Wyszynska, E. Janik-Spiechowicz, O

Publisher Elsevier

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Book Details

Author(s)B. Kosmider, K. Wyszynska, E. Janik-Spiechowicz, O

PublisherElsevier

ISBN / ASINB000RQZ2JQ

ISBN-13978B000RQZ2J0

AvailabilityAvailable for download now

Sales Rank99,999,999

MarketplaceUnited States 🇺🇸

Description ▲

This digital document is a journal article from Mut.Res.-Genetic Toxicology and Environmental Mutagenesis, published by Elsevier in 2004. The article is delivered in HTML format and is available in your Amazon.com Media Library immediately after purchase. You can view it with any web browser.

Description:
Short-term tests that detect genetic damage have provided information needed for evaluating carcinogenic risks of chemicals to man. The mutagenicity of cis-bis(3-aminoflavone)dichloroplatinum(II) (cis-[Pt(AF)"2Cl"2]) in comparison with cis-diamminedichloroplatinum(II) (cis-DDP) was evaluated in the standard plate-incorporation assay in four strains of Salmonella typhimurium: TA97a, TA98, TA100 and TA102, in experiments with and without metabolic activation. It was shown that cis-[Pt(AF)"2Cl"2] acts directly and is mutagenic for three strains of S. typhimurium: TA97a, TA98 and TA100. In comparison with cis-DDP this compound showed a weaker genotoxicity. Contrary to cis-DDP it has not shown toxic properties in the tester bacteria. The genotoxicity of both tested compounds was evaluated using chromosomal aberration, sister chromatid exchange and micronucleus assays, without and with metabolic activation, in human lymphocytes in vitro. The inhibitory effects of both compounds on mitotic activity, cell proliferation kinetics and nuclear division index were also compared. In all test systems applied, cis-[Pt(AF)"2Cl"2] was a less effective clastogen and a weaker inducer of both sister chromatid exchanges and micronuclei in comparison with cis-DDP, with and without metabolic activation. cis-[Pt(AF)"2Cl"2] has a direct mechanism of action and is less cytostatic and cytotoxic than the other compound. These results provide important data on the genotoxicity of cis-[Pt(AF)"2Cl"2] and indicate its beneficial properties as a potential anticancer drug, especially in comparison with cis-DDP.