AI Article Synopsis
- Arsenic trioxide shows promise in treating various cancers by slowing cell growth, blocking blood vessel formation, and promoting programmed cell death, largely influenced by transcription factors known as Sp proteins.
- By analyzing bladder cancer cell lines, researchers found that arsenic trioxide effectively reduced levels of Sp proteins and other related genes, leading to decreased tumor activity in responsive cells (KU7), while non-responsive cells (253JB-V) showed minimal changes.
- The study also revealed that oxidative stress plays a significant role in how these cancer cells respond to arsenic trioxide, with certain antioxidants protecting resistant cells from its effects, suggesting potential strategies for improving treatment outcomes.
Article Abstract
Arsenic trioxide exhibits antiproliferative, antiangiogenic and proapoptotic activity in cancer cells, and many genes associated with these responses are regulated by specificity protein (Sp) transcription factors. Treatment of cancer cells derived from urologic (bladder and prostate) and gastrointestinal (pancreas and colon) tumors with arsenic trioxide demonstrated that these cells exhibited differential responsiveness to the antiproliferative effects of this agent and this paralleled their differential repression of Sp1, Sp3 and Sp4 proteins in the same cell lines. Using arsenic trioxide-responsive KU7 and non-responsive 253JB-V bladder cancer cells as models, we show that in KU7 cells, < or =5 microM arsenic trioxide decreased Sp1, Sp3 and Sp4 and several Sp-dependent genes and responses including cyclin D1, epidermal growth factor receptor, bcl-2, survivin and vascular endothelial growth factor, whereas at concentrations up to 15 microM, minimal effects were observed in 253JB-V cells. Arsenic trioxide also inhibited tumor growth in athymic mice bearing KU7 cells as xenografts, and expression of Sp1, Sp3 and Sp4 was significantly decreased. Inhibitors of oxidative stress such as glutathione or dithiothreitol protected KU7 cells from arsenic trioxide-induced antiproliferative activity and Sp repression, whereas glutathione depletion sensitized 253JB-V cells to arsenic trioxide. Mechanistic studies suggested that arsenic trioxide-dependent downregulation of Sp and Sp-dependent genes was due to decreased mitochondrial membrane potential and induction of reactive oxygen species, and the role of peroxides in mediating these responses was confirmed using hydrogen peroxide.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2900380 | PMC |
| http://dx.doi.org/10.1016/j.yexcr.2010.04.027 | DOI Listing |
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