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Genotoxic effects of heavy metals in rat hepatocytes

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Abstract

The genotoxic interaction of metals, which are common environmental contaminants, was studied in cultured hepatocytes. Freshly isolated rat hepatocytes were exposed to concentrations of cadmium, copper, silver and lead salts ranging from non-cytotoxic to moderately cytotoxic (as determined by LDH release), and the incorporation of [3H]thymidine into the DNA, as a measure of repair synthesis, was followed. In addition, the uptake of metals by the nuclear fraction was determined using Inductively Coupled Plasma/Mass Spectrometry or atomic absorption spectrophotometry. The evaluation of binding of 109Cd to the DNA in situ was also attempted. It was observed that after a 20 h exposure period, all the metals investigated were found in the nuclear fraction of hepatocytes, with Ag apparently being accumulated less efficiently. In parallel, Cd (0.18 to 1.8 µM) and Cu (7.9 to 78.5 µM) consistently produced a statistically significant stimulation of [3H]thymidine incorporation into the DNA, in the presence or absence of hydroxyurea while Ag was active only at the highest concentration tested (18.5 µM). In contrast, Pb failed to induce a UDS response at the levels used. Moreover, exposure of hepatocytes to 1.8 µM 109CdCl2 for 20 h led to a DNA binding ratio of 0.98 ± 0.23 ng Cd/ µg DNA. The present results support the view that the nucleus may be an important target organelle for metal toxicity.

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Abbreviations

2-AAF:

2-acetylaminofluorene

Cd:

cadmium

HU:

hydroxyurea

lCP/MS:

inductively coupled plasma/mass spectrometry

Hg:

mercury

Ni:

nickel

UDS:

unscheduled DNA synthesis

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Denizeau, F., Marion, M. Genotoxic effects of heavy metals in rat hepatocytes. Cell Biol Toxicol 5, 15–25 (1989). https://doi.org/10.1007/BF00141061

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