Chronic Exposure to Zinc Chromate Induces Centrosome Amplification and Spindle Assembly Checkpoint Bypass in Human Lung Fibroblasts

Hexavalent chromium (Cr(VI)) compounds are known human lung carcinogens. Solubility plays an important role in its carcinogenicity with the particulate or insoluble form being the most potent. Of the particulate Cr(VI) compounds, zinc chromate appears to be the most potent carcinogen; however, very...

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Bibliographic Details
Published inChemical research in toxicology Vol. 23; no. 2; pp. 386 - 395
Main Authors Holmes, Amie L, Wise, Sandra S, Pelsue, Stephen C, Aboueissa, AbouEl-Makarim, Lingle, Wilma, Salisbury, Jeffery, Gallagher, Jamie, Wise, John Pierce
Format Journal Article
LanguageEnglish
Published United States American Chemical Society 15.02.2010
Subjects
Aneuploidy
Cell Line
Centrosome - drug effects
Chromates - toxicity
Chromosomal Instability - drug effects
Fibroblasts - drug effects
Humans
Lung - cytology
Lung - drug effects
Particle Size
Solubility
Spindle Apparatus - drug effects
Zinc Compounds - toxicity
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Summary:Hexavalent chromium (Cr(VI)) compounds are known human lung carcinogens. Solubility plays an important role in its carcinogenicity with the particulate or insoluble form being the most potent. Of the particulate Cr(VI) compounds, zinc chromate appears to be the most potent carcinogen; however, very few studies have investigated its carcinogenic mechanism. In this study, we investigated the ability of chronic exposure to zinc chromate to induce numerical chromosome instability. We found no increase in aneuploidy after a 24 h exposure to zinc chromate, but with more chronic exposures, zinc chromate induced concentration- and time-dependent increases in aneuploidy in the form of hypodiploidy, hyperdiploidy, and tetraploidy. Zinc chromate also induced centrosome amplification in a concentration- and time-dependent manner in both interphase and mitotic cells after chronic exposure, producing cells with centriolar defects. Furthermore, chronic exposure to zinc chromate induced concentration- and time-dependent increases in spindle assembly checkpoint bypass with increases in centromere spreading, premature centromere division, and premature anaphase. Last, we found that chronic exposure to zinc chromate induced a G2 arrest. All together, these data indicate that zinc chromate can induce chromosome instability after prolonged exposures.
ISSN:0893-228X
1520-5010
DOI:10.1021/tx900360w