Carcinogenesis, Vol 18, 93-96, Copyright © 1997 by Oxford University Press
AJ Giurgiovich, BA Diwan, OA Olivero, LM Anderson, JM Rice and MC Poirier
Although there is evidence that the toxic effects of cis-
diamminedichloroplatinum(II) (cisplatin) include morphologically abnormal
mitochondria, direct demonstrations of mitochondrial DNA damage by this
chemotherapeutic agent have rarely been reported. Here we show that, in
rats exposed to a single dose of cisplatin during gestation, cisplatin-DNA
binding levels in both maternal and fetal liver and brain mitochondrial DNA
are higher than those observed in genomic DNA. Pregnant F344/NCr rats were
injected i.p. with either 5 or 15 mg cisplatin/kg body wt at 18 days of
gestation and killed 24 h later. Cisplatin-DNA adducts were determined by
dissociation-enhanced lanthanide fluoroimmunoassay using a cisplatin-DNA
standard modified in the same range as the biological samples. Values for
genomic cisplatin- DNA adducts in multiple maternal and fetal tissues have
been presented elsewhere. Here, genomic DNA adduct levels for liver, brain,
kidney and placenta are reported again for comparison with mitochondrial
DNA adduct levels in the same tissues. In maternal and fetal brain,
mitochondrial DNA adduct levels were approximately 7- to 50-fold higher
than genomic DNA adduct levels, and in fetal liver they were approximately
2- to 16-fold higher than genomic DNA adduct levels. These studies
demonstrate extensive cisplatin-DNA adduct formation in brain and liver
mitochondria of fetal rats exposed transplacentally and suggest that
mitochondrial DNA in some organs may be a particular target for cisplatin
genotoxicity.
ARTICLES
Elevated mitochondrial cisplatin-DNA adduct levels in rat tissues after transplacental cisplatin exposure
Laboratory of Cellular Carcinogenesis and Tumor Promotion, National Cancer Institute, NIH, Bethesda, MD 20892-4255, USA.
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