Cellular uptake and fractionation/localization studies revealed that sagopilone enters cells more efficiently, associates more tightly with the cytoskeleton, and polymerizes tubulin more potently than paclitaxel. Moreover, in contrast to paclitaxel and other epothilones [such as the natural product epothilone B (patupilone) or its partially synthetic analogue ixabepilone], sagopilone is not a substrate of the P-glycoprotein efflux pumps.
Microtubule stabilization by sagopilone caused mitotic arrest, followed by transient multinucleation and activation of the mitochondrial apoptotic pathway.
Profiling of the proapoptotic signal transduction pathway induced by sagopilone with a panel of small interfering RNAs revealed that sagopilone acts similarly to paclitaxel.
In HCT 116 colon carcinoma cells, sagopilone-induced apoptosis was partly antagonized by the knockdown of proapoptotic members of the Bcl-2 family, including Bax, Bak, and Puma, whereas knockdown of Bcl-2, Bcl-X(L), or Chk1 sensitized cells to sagopilone-induced cell death.
Related to its improved subcellular pharmacokinetics, however, sagopilone is more cytotoxic than other epothilones in a large panel of human cancer cell lines in vitro and in vivo.
In particular, sagopilone is highly effective in reducing the growth of paclitaxel-resistant cancer cells.
These results underline the processes behind the therapeutic efficacy of sagopilone, which is now evaluated in a broad phase II program.
- DOI - Cancer research (DOI)
- HighWire Press - full-text online (subscription/membership/fee required)
Fecha de publicación
Cancer Res (1538-7445)
Temas de la revista
Bayer Schering Pharma AG, TRG Oncology, Müllerstrasse 72-178, G-13342 Berlin, Germany. jens.hoffmann [at] bayerhealthcare.com
Referencia de entrega
Cancer Res. 2008 Jul;68(13):5301-8
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