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Blogger's Note: abstract does not reference ovarian cancer (note this is a preclinical study)
Abstract
Purpose: Taxanes are important
chemotherapeutic agents with proven efficacy in human cancers, but their
use is limited by
resistance development. We report here the
preclinical characteristics of cabazitaxel (XRP6258), a semisynthetic
taxane developed
to overcome taxane resistance.
Experimental Design: Cabazitaxel effects on
purified tubulin and on taxane-sensitive or chemotherapy-resistant tumor
cells
were evaluated in vitro. Antitumor activity and pharmacokinetics of intravenously administered cabazitaxel were assessed in tumor-bearing mice.
Results: In vitro, cabazitaxel stabilized
microtubules as effectively as docetaxel, but was ten-fold more potent
than docetaxel in chemotherapy-resistant
tumor cells (IC50 ranges: cabazitaxel,
0.013-0.414 μM; docetaxel, 0.17-4.01 μM). The active concentrations of
cabazitaxel in these cell lines
were achieved easily and maintained for up to 96
hours in the tumors of mice bearing MA16/C tumors treated with
cabazitaxel
at 40 mg/kg. Cabazitaxel exhibited antitumor
efficacy in a broad spectrum of murine and human tumors (melanoma B16,
colon
C51, C38, HCT 116 and HT-29, mammary MA17/A and
MA16/C, pancreas P03 and MIA PaCa2, prostate DU145, lung A549 and
NCI-H460,
gastric N87, head and neck SR475, and kidney
Caki1). Of particular note, cabazitaxel was active in tumors poorly
sensitive
or innately resistant to docetaxel (Lewis lung,
pancreas P02, colon HCT8, gastric GXF209, mammary UISO BCA1) or with
acquired
docetaxel resistance (melanoma B16/TXT).
Conclusions: Cabazitaxel is as active as docetaxel
in docetaxel-sensitive tumor models but is more potent than docetaxel in
tumor models with innate or acquired resistance to
taxanes and other chemotherapies. These studies were the basis for
subsequent
clinical evaluation.
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