Am. J. Respir. Cell Mol. Biol., Vol 17, No. 6, Dec 1997, 660-671.
Analysis of cell cycle disruptions in cultures of rat pleural mesothelial cells exposed to asbestos fibers
V Levresse, A Renier, J Fleury-Feith, F Levy, S Moritz, C Vivo, Y Pilatte and MC Jaurand
INSERM U 139, Institut mondor de Medecine Moliculaire, Faculte de Medecine, Creteil, France.
The control of DNA integrity in mammalian cells is important to maintain
the cell homeostasis and prevent neoplastic transformation. Control of cell
division and cell death permits repair or elimination of damaged cells.
Since asbestos fibers can produce DNA damage, chromosome alterations and
apoptosis in several sorts of cells, including mesothelial cells, it was
interesting to investigate cell cycle disturbances in rat pleural
mesothelial cells (RPMC) treated with asbestos fibers. Cell cycle analyses
were performed in RPMC exposed to crocidolite (10 and 20 microg/cm2) and
chrysotile (5 and 10 microg/cm2) for different times (4 to 48 h). Both
fiber types entailed a G2/M accumulation in agreement with a delay in the
mitosis course. Chrysotile fibers produced a G0/G1 accumulation associated
with a time- dependent p53 and p21 expression. Crocidolite exposure
resulted in a delay in the G1/S transition paralleling a low rate of p53
expression. These results are in agreement with a DNA damaging potential of
asbestos fibers since similar results were found following RPMC exposure to
gamma rays. In asbestos-treated RPMC, a low rate of apoptosis was found
suggesting that RPMC may follow a DNA repair pathway that could contribute
to the formation of DNA lesions. In addition, the cell cycle disturbances
at the G2/M checkpoint suggest that genetically altered cells have
progressed through the cycle and support the already published findings on
the ability of asbestos fibers to impair cell division.
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Copyright © 1997 American Thoracic Society.
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