Item Type: | Article |
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Title: | The antiangiogenic and antitumoral activity of titanocene Y* in vivo |
Creators Name: | Fichtner, I., Behrens, D., Claffey, J., Deally, A., Gleeson, B., Patil, S., Weber, H. and Tacke, M. |
Abstract: | The 4-diethylaminomethylbenzyl-substituted titanocene dichloride (Titanocene Y*), which is completely water- soluble and showed nanomolar activity against the human renal cancer cells CAKI-1, was tested in vitro in an antiangiogenesis assay against human umbilical vein endothelial cells, HUVEC, delivering an IC50 value of 23 +/- 17 {Mu}M. Titanocene Y* was then given at 25, 50 and 75 mg/kg/d, on five consecutive days per week for up to three weeks to one cohort of six CAKI-1 tumor-bearing female NMRI:nu/nu mice, while a further cohort was treated with solvent only. At the two higher dosages Titanocene Y* showed high toxicity leading to mortality, while the titanocene-treated mouse cohort treated with the lowest dosage showed a moderate but statistically significant tumor growth reduction with respect to the solvent-treated control group, with an optimal T/C value of 76% at the end of the experiment. Immunohistological analysis revealed that the expression of the proliferation marker Ki-67 was reduced by 21%. Furthermore, anti-angiogenic activity was identified by CD31 staining; the number of micro vessels in a defined tumor area decreased by 23% due to Titanocene Y* treatment. The substance caused dose-dependent body weight loss but did not reduce the number of white blood cells at doses of 25 and 50 mg/kg/d. |
Keywords: | Anticancer Drug, Anti-Angiogenic Drug, Titanocene, Renal Cell Cancer, Xenograft, HUVEC, Malignant Disease, Adult Kidney, Adult Malignancies, Adenocarcinoma, Sunitinib, Sorafenib, Temsirolimus, Bevacizumab, Dichloride, Tumor Area |
Source: | Letters in Drug Design & Discovery |
ISSN: | 1570-1808 |
Publisher: | Bentham |
Volume: | 8 |
Number: | 4 |
Page Range: | 302-307 |
Date: | May 2011 |
Official Publication: | https://doi.org/10.2174/157018011794839367 |
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