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Indirubin-3â²-monoxime, a CDK Inhibitor Induces Growth Inhibition and Apoptosis-independent Up-regulation of Survivin in Transitional Cell Cancer
In traditional Chinese Medicine, the preparation Danggui Longhui Wan has been used for years in the treatment of chronic myelocytic leukemia. The compound indirubin has been shown to be the active constituent. A cell permeable derivative, indirubin-3â²-monoxime, is a selective and potent inhibitor...
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| Published in: | Anticancer research 2006-05, Vol.26 (3A), p.2129 |
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| Main Authors: | , , , , , , |
| Format: | Article |
| Language: | English |
| Online Access: | Get full text |
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| Summary: | In traditional Chinese Medicine, the preparation Danggui Longhui Wan has been used for years in the treatment of chronic myelocytic
leukemia. The compound indirubin has been shown to be the active constituent. A cell permeable derivative, indirubin-3â²-monoxime,
is a selective and potent inhibitor of cyclin-dependent kinases (cdk). The ability of indirubin-3â²-monoxime to induce apoptosis
and tumor cell death in transitional cell cancer cell lines was investigated here. The growth-inhibitory properties were evaluated
by EZ4U, a cytotoxic assay; apoptosis induction was determined by immunoblotting of cleaved PARP and flow cytometry of Annexin-V/PI
staining during treatment. To evaluate further the underlying molecular action of indirubin-3â²-monoxime on the cell cycle,
the levels of cdk-1 and survivin, a mitotic spindle checkpoint and apoptosis-regulating protein, respectively, were additionally
determined by flow cytometry and immunoblotting. The results indicated that indirubin-3â²-monoxime induced reversible growth
arrest in all four cell lines and an increase of apoptosis in two of them. The treatment with indirubin-3â²-monoxime increased
the expression of survivin almost four times in the RT4 cells and more than doubled it in the RT112 and T24 cells. In the
SUP cells, the expression of survivin increased more than seven-fold after 72-h incubation. No clear correlation between the
low apoptosis induction rate and extent of survivin expression was found. Cdk expression was not significantly altered by
indirubin-3â²-monoxime. In summary, indirubin-3â²-monoxime might be a promising candidate for targeted cancer therapy, however,
its molecular action remains to be further evaluated. |
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| ISSN: | 0250-7005 1791-7530 |