4.6 Article

Efficacy of a Covalent Microtubule Stabilizer in Taxane-Resistant Ovarian Cancer Models

Journal

MOLECULES
Volume 26, Issue 13, Pages -

Publisher

MDPI
DOI: 10.3390/molecules26134077

Keywords

microtubule stabilizers; taxanes; drug resistance; natural products; ovarian cancer; metastasis; covalent drugs; anticancer agents; murine model

Funding

  1. Voelcker Young Investigator Award
  2. Cancer Prevention & Research Institute of Texas (CPRIT) [RP 170345]

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Research has found that C-22,23-epoxytaccalonolides, a novel class of covalent microtubule stabilizers, demonstrate efficacy against taxane-resistant ovarian cancer models both in vitro and in vivo. The irreversible mechanism of microtubule stabilization of taccalonolide AF shows unique potential for intraperitoneal treatment of locally disseminated taxane-resistant disease, addressing a significant unmet clinical need in the treatment of ovarian cancer patients.
Ovarian cancer often has a poor clinical prognosis because of late detection, frequently after metastatic progression, as well as acquired resistance to taxane-based therapy. Herein, we evaluate a novel class of covalent microtubule stabilizers, the C-22,23-epoxytaccalonolides, for their efficacy against taxane-resistant ovarian cancer models in vitro and in vivo. Taccalonolide AF, which covalently binds beta-tubulin through its C-22,23-epoxide moiety, demonstrates efficacy against taxane-resistant models and shows superior persistence in clonogenic assays after drug washout due to irreversible target engagement. In vivo, intraperitoneal administration of taccalonolide AF demonstrated efficacy against the taxane-resistant NCI/ADR-RES ovarian cancer model both as a flank xenograft, as well as in a disseminated orthotopic disease model representing localized metastasis. Taccalonolide-treated animals had a significant decrease in micrometastasis of NCI/ADR-RES cells to the spleen, as detected by quantitative RT-PCR, without any evidence of systemic toxicity. Together, these findings demonstrate that taccalonolide AF retains efficacy in taxane-resistant ovarian cancer models in vitro and in vivo and that its irreversible mechanism of microtubule stabilization has the unique potential for intraperitoneal treatment of locally disseminated taxane-resistant disease, which represents a significant unmet clinical need in the treatment of ovarian cancer patients.

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