Camptothecin
Efficacy to Poison Top1 Is Altered by
Bisphenol A in Mouse Embryonic Fibroblasts
Posted on 2018-05-25 - 00:00
Bisphenol A (BPA)
is used heavily in the production of polycarbonate
plastics, thermal receipt paper, and epoxies. Ubiquitous exposure
to BPA has been linked to obesity, diabetes, and breast and reproductive
system cancers. Resistance to chemotherapeutic agents has also been
shown in cancer cell models. Here, we investigated BPA’s ability
to confer resistance to camptothecin (CPT) in mouse embryonic fibroblasts
(MEFs). MEFs are sensitive to CPT; however, co-exposure of BPA with
CPT improved cell survival. Co-exposure significantly reduced Top1-DNA
adducts, decreasing chromosomal aberrations and DNA strand break formation.
This decrease occurs despite BPA treatment increasing the protein
levels of Top1. By examining chromatin structure after BPA exposure,
we determined that widespread compaction and loss of nuclear volume
occurs. Therefore, BPA reduced CPT activity by reducing the accessibility
of DNA to Top1, inhibiting DNA adduct formation, the generation of
toxic DNA strand breaks, and improving cell survival.
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Sonavane, Manoj; Sykora, Peter; Andrews, Joel F.; Sobol, Robert W.; Gassman, Natalie R. (2018). Camptothecin
Efficacy to Poison Top1 Is Altered by
Bisphenol A in Mouse Embryonic Fibroblasts. ACS Publications. Collection. https://doi.org/10.1021/acs.chemrestox.8b00050