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Impact of cell cycle delay on micronucleus frequency in TK6 cells.

Environ Mol Mutagen

January 2014

Pfizer Worldwide Research and Development, Genetic Toxicology Center of Expertise, Eastern Point Road, Groton, Connecticut.

Previous studies with TK6 cells have shown that extending the recovery period after pulse treatment allows for greater micronucleus expression for some compounds. This study explores the role of cell cycle delay in micronucleus expression after pulse treatment with three model genotoxins [mitomycin C, etoposide (ETOP), vinblastine]. Cells were treated for 4 hr and allowed to recover for 36 hr with samples removed at various time points during the recovery period and analyzed for cell cycle distribution, apoptosis and micronucleus frequency.

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