The use of a microsomal in vitro assay to study phase I biotransformation of chlorobornanes (toxaphene®) in marine mammals and birds -: Possible consequences of biotransformation for bioaccumulation and genotoxicity

被引:43
作者
Boon, JP
Sleiderink, HM
Helle, MS
Dekker, M
van Schanke, A
Roex, E
Hillebrand, MTJ
Klamer, HJC
Govers, B
Pastor, D
Morse, D
Wester, PG
de Boer, J
机构
[1] Netherlands Inst Sea Res, NL-1790 AB Den Burg, Netherlands
[2] Minist Transport Publ Works & Water Management, Directorate Gen Publ Works & Water Management, Natl Inst Coastal & Marine Management, NL-9750 AE Haren, Netherlands
[3] Wageningen Univ Agr, Dept Toxicol, NL-6700 EA Wageningen, Netherlands
[4] DLO, Netherlands Inst Fisheries Invest, NL-1970 AB Ijmuiden, Netherlands
来源
COMPARATIVE BIOCHEMISTRY AND PHYSIOLOGY C-TOXICOLOGY & PHARMACOLOGY | 1998年 / 121卷 / 1-3期
关键词
in vitro biotransformation; toxaphene (R) residue patterns; genotoxicity; wildlife;
D O I
10.1016/S0742-8413(98)10058-0
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The factors determining the bioaccumulation of lipophilic compounds in wildlife are often poorly understood, partly because it is difficult to do in vivo experiments with animals such as marine mammals and birds. To evaluate the role of phase I biotransformation in the bioaccumulation process of chlorobornanes (toxaphene(R)), this was studied in in vitro assays with hepatic microsomes of animals that could be sampled shortly after death. The capacity of microsomes to metabolise a technical toxaphene mixture decreased in the order Phoca vitulina (harbour seal) much greater than lagenorhynchus albirostris (whitebeaked dolphin) congruent to Diomedea immutabilis (Laysan albatross) > Physeter macrocephalus (:sperm whale). Harbour seal microsomes metabolised the chlorobornane (CHB) congeners CHB-32 and CHB-62; whitebeaked dolphin and Laysan albatross microsomes only metabolised CHB-32. Metabolism of CHB-26 and CHB-50 was never observed. The negative chemical ionisation (NCI -) mass spectra of some of the hydroxylated metabolites were obtained. The number of peaks in the toxaphene residues of wildlife extracts decreased in the order of increasing in-vitro biotransformation capacity. Thus, the results of the in vitro assays and residue analysis were in accordance, although assays with microsomes of more individuals of the same species are required for a more general conclusion at the species level. Finally, the effect of in vitro biotransformation was evaluated in terms of the genotoxic potential using the Mutatox(R) assay. Only technical toxaphene and CHB-32 were genotoxic in the direct assay, whereas the addition of rat S9 fraction or microsomes of harbour seal and albatross decreased the genotoxic response. Thus, organisms with a low ability to metabolise chlorobornanes, such as whales, may be most affected by the carcinogenic properties of toxaphene. A hypothetical reaction which fits the experimental results is discussed. Based on these results it is concluded that in vitro assays with microsomes of wildlife animals which died a natural cause can act as a valuable tool to assess the occurrence and effects of phase I metabolism. Some precautions are discussed, that should be taken to reduce the chance of false negative results. (C) 1998 Published by Elsevier Science Inc. All rights reserved.
引用
收藏
页码:385 / 403
页数:19
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