Joanne Wan scite author profile

It is becoming more evident that not only can drugs and environmental chemicals interfere with normal fetal development by causing structural malformations, such as limb defects, but that xenobiotic exposure during development can also cause biochemical and functional abnormalities that may ultimately lead to cancer later on in life. Fetal toxicity may be partly mediated by the embryonic bioactivation of xenobiotics to free radical intermediates that can lead to oxidative stress and potentially lead, in some cases, to carcinogenesis. Using a number of examples, this review will focus on the role of reactive oxygen species (ROS) in the mechanisms pertaining to in utero initiated cancers.

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The role of c-MYB in benzene-initiated toxicity

Wan

Badham

Winn

2005

Chemico-Biological Interactions

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The effects of benzene and the metabolites phenol and catechol on c-Myb and Pim-1 signaling in HD3 cells

Wan

Winn

2004

Toxicology and Applied Pharmacology

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Joanne Wan

Benzene-initiated oxidative stress: Effects on embryonic signaling pathways

Benzene’s metabolites alter c-MYB activity via reactive oxygen species in HD3 cells☆

In utero–initiated cancer: The role of reactive oxygen species

The role of c-MYB in benzene-initiated toxicity

The effects of benzene and the metabolites phenol and catechol on c-Myb and Pim-1 signaling in HD3 cells

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