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KMID : 1161520090130040399
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Animal Cells and Systems
2009 Volume.13 No. 4 p.399 ~ p.403
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p19ras Accelerates p73¥â?mediated apoptosis through a caspase?3 dependent pathway
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Jang Sang-Min
Kim Jung-Woong
Choi Kyung-Hee
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Abstract
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p19ras is an alternative splicing variant of the proto?oncogene c?H?ras pre?mRNA of p21ras. In contrast to p21ras, p19ras does not have a C?terminal CAAX motif that targets the plasma membrane and is localized to both the cytoplasm and nucleus. We found that p19ras activated the transcriptional activity of p73¥â through protein?protein interactions in the nucleus. p73 is known to play an important role in cellular damage responses such as apoptosis. Although p73 is a structural and functional homologue of p53, p73?mediated apoptosis has not yet been clearly elucidated. In this study, we demonstrate that the interaction between p19ras and p73¥â accelerated p73¥â?induced apoptosis through a caspase?3 dependent pathway. Treatment with DEVD?CHO, a caspase inhibitor, also strengthened p73¥â?mediated apoptosis through a caspase?3 dependent pathway. Furthermore, the enhanced transcriptional activity of endogenous p73¥â by treatment with Taxol was amplified by p19ras overexpression, which markedly increased caspase?3 dependent apoptosis in the p53?null SAOS2 cancer cell line. Our findings indicate a functional linkage between p19ras and p73 in caspase?3 mediated apoptosis of cancer cells.
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KEYWORD
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p19ras, p73¥â, caspase-3, apoptosis
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