- Confirmation of HIF-1α Independent Pathway in the Progression of HepG2 Cells by Hypoxic Condition
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Sang Woo Lee, Jae Uk Chong, Seon Ok Min, Kyung Sik Kim
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J Liver Cancer. 2016;16(1):31-37. Published online March 31, 2016
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DOI: https://doi.org/10.17998/jlc.16.1.31
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 Abstract
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- Background/Aim
s: When hepatocellular carcinoma (HCC) is exposed to hypoxic condition,
HIF-1α is activated and results in angiogenesis and increased tumor burden. Although
inhibition of HIF-1α may reduce tumor growth, there are some limitations to control tumor
growth completely. For a more effective therapy for HCC, we investigated HIF-1α independent
pathway related tumor growth with angiogenesis.
Methods
We cultured HepG2 cells (HCC cell line) in both normoxia and hypoxia conditions.
These cells were divided into three groups: a echinomycin treated group, a echinomycin and
quinazoline treated group and a control group without any treatments. Growth morphologies
of cells were observed with a microscope after 24 hours. Immunocytochemistry assay
was done to detect the angiogenesis during inhibition of HIF-1α and/or NF-κB in hypoxia
condition, and compared with results in normoxia condition.
Results
In normoxia, the expression of HIF-1α on tumor growth was not found. In hypoxia,
inhibition of HIF-1α reduced the tumor growth compared to the control group. But, inhibition
of both HIF-1α and NF-κB did not show apparent reduction of tumor growth as shown in HIF-
1α only group.
Conclusions
Signaling pathways related to cancer cell growth exist through a vast network.
Inhibition of one target molecule may result in over-expression of other molecules related
to the tumor growth. For an effective therapy in blocking of the tumor growth, more
comprehensive understanding of the network related to signaling pathways on tumor growth
is necessary. (J Liver Cancer 2016;16:31-37)
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