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Genotoxicity of naturally occurring hydroxyanthraquinones.

作者信息

Westendorf J, Marquardt H, Poginsky B, Dominiak M, Schmidt J, Marquardt H

机构信息

Department of Toxicology, University of Hamburg Medical School, F.R.G.

出版信息

Mutat Res. 1990 Jan;240(1):1-12. doi: 10.1016/0165-1218(90)90002-j.

Abstract

A variety of structurally related hydroxyanthraquinones (HA) were investigated in a test battery for the evaluation of mutagenicity and cell-transforming activity. The tests were: (1) the Salmonella typhimurium mutagenicity assay, (2) the V79-HGPRT mutagenicity assay, (3) the DNA-repair induction assay in primary rat hepatocytes and (4) the in vitro transformation of C3H/M2 mouse fibroblasts. In Salmonella, most of the tested compounds were mutagenic in strain TA1537, but only a few were active in other strains. Among these were HA with a hydroxymethyl group, such as lucidin and aloe-emodin. In V79 cells, only HA with 2 hydroxy groups in the 1,3 positions (1,3-DHA, purpurin, emodin) or with a hydroxymethyl sidechain (lucidin and aloe-emodin) were mutagenic. The compounds found to be active in V79 cells were also active in the DNA-repair assay and in the C3H/M2 transformation assay. Thus, it appears that the genotoxicity of HA is dependent on certain structural requirements.

摘要

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