In Vivo Evaluation of (-)-Zampanolide Demonstrates Potent and Persistent Antitumor Efficacy When Targeted to the Tumor Site

Leila Takahashi-Ruiz; Joseph D. Morris; Phillip Crews; Tyler Johnson; April L. Risinger

doi:10.3390/molecules27134244

In Vivo Evaluation of (-)-Zampanolide Demonstrates Potent and Persistent Antitumor Efficacy When Targeted to the Tumor Site

Leila Takahashi-Ruiz
, Joseph D. Morris
, Phillip Crews
, Tyler Johnson
, April L. Risinger

Department of Natural Sciences and Mathematics

Research output: Contribution to journal › Article › peer-review

Abstract

Microtubule-stabilizing agents (MSAs) are a class of compounds used in the treatment of triple-negative breast cancer (TNBC), a subtype of breast cancer where chemotherapy remains the standard-of-care for patients. Taxanes like paclitaxel and docetaxel have demonstrated efficacy against TNBC in the clinic, however new classes of MSAs need to be identified due to the rise of taxane resistance in patients. (−)-Zampanolide is a covalent microtubule stabilizer that can circumvent taxane resistance in vitro but has not been evaluated for in vivo antitumor efficacy. Here, we determine that (−)-zampanolide has similar potency and efficacy to paclitaxel in TNBC cell lines, but is significantly more persistent due to its covalent binding. We also provide the first reported in vivo antitumor evaluation of (−)-zampanolide where we determine that it has potent and persistent antitumor efficacy when delivered intratumorally. Future work on zampanolide to further evaluate its pharmacophore and determine ways to improve its systemic therapeutic window would make this compound a potential candidate for clinical development through its ability to circumvent taxane-resistance mechanisms.

Original language	American English
Pages (from-to)	4244
Journal	Molecules
Volume	27
Issue number	13
DOIs	https://doi.org/10.3390/molecules27134244
State	Published - 2022

Funding

This work was funded by R01 CA219948 to A.L.R. the Fletcher Jones Endowment Fund of Dominican University of California (T.A.J.).

Keywords

Triple-negative Breast Cancer
Microtubule Stabilzers
Zampanolide
Paclitaxel
Covalent

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@article{4811cabbeea947af82819c1c1593508c,

title = "In Vivo Evaluation of (-)-Zampanolide Demonstrates Potent and Persistent Antitumor Efficacy When Targeted to the Tumor Site",

abstract = "Microtubule-stabilizing agents (MSAs) are a class of compounds used in the treatment of triple-negative breast cancer (TNBC), a subtype of breast cancer where chemotherapy remains the standard-of-care for patients. Taxanes like paclitaxel and docetaxel have demonstrated efficacy against TNBC in the clinic, however new classes of MSAs need to be identified due to the rise of taxane resistance in patients. (−)-Zampanolide is a covalent microtubule stabilizer that can circumvent taxane resistance in vitro but has not been evaluated for in vivo antitumor efficacy. Here, we determine that (−)-zampanolide has similar potency and efficacy to paclitaxel in TNBC cell lines, but is significantly more persistent due to its covalent binding. We also provide the first reported in vivo antitumor evaluation of (−)-zampanolide where we determine that it has potent and persistent antitumor efficacy when delivered intratumorally. Future work on zampanolide to further evaluate its pharmacophore and determine ways to improve its systemic therapeutic window would make this compound a potential candidate for clinical development through its ability to circumvent taxane-resistance mechanisms.",

keywords = "Triple-negative Breast Cancer, Microtubule Stabilzers, Zampanolide, Paclitaxel, Covalent",

author = "Leila Takahashi-Ruiz and Morris, \{Joseph D.\} and Phillip Crews and Tyler Johnson and Risinger, \{April L.\}",

note = "L.T.-R. and A.L.R. conceptualized the project, performed biological experiments, data analysis, writing, and visualization of data. J.D.M. partitioned the DMM extracts, scaled up the purification of zampanolide, performed NMR experiments, assigned NMR spectra, and assisted with writing the manuscript. T.A.J. designed purification schemes, confirmed the chemical structure, and assisted with writing the manuscript. P.C. provided the repository extract of C. mycofijiensis. All authors have read and agreed to the published version of the manuscript.",

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T1 - In Vivo Evaluation of (-)-Zampanolide Demonstrates Potent and Persistent Antitumor Efficacy When Targeted to the Tumor Site

AU - Takahashi-Ruiz, Leila

AU - Morris, Joseph D.

AU - Crews, Phillip

AU - Johnson, Tyler

AU - Risinger, April L.

N1 - L.T.-R. and A.L.R. conceptualized the project, performed biological experiments, data analysis, writing, and visualization of data. J.D.M. partitioned the DMM extracts, scaled up the purification of zampanolide, performed NMR experiments, assigned NMR spectra, and assisted with writing the manuscript. T.A.J. designed purification schemes, confirmed the chemical structure, and assisted with writing the manuscript. P.C. provided the repository extract of C. mycofijiensis. All authors have read and agreed to the published version of the manuscript.

PY - 2022

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N2 - Microtubule-stabilizing agents (MSAs) are a class of compounds used in the treatment of triple-negative breast cancer (TNBC), a subtype of breast cancer where chemotherapy remains the standard-of-care for patients. Taxanes like paclitaxel and docetaxel have demonstrated efficacy against TNBC in the clinic, however new classes of MSAs need to be identified due to the rise of taxane resistance in patients. (−)-Zampanolide is a covalent microtubule stabilizer that can circumvent taxane resistance in vitro but has not been evaluated for in vivo antitumor efficacy. Here, we determine that (−)-zampanolide has similar potency and efficacy to paclitaxel in TNBC cell lines, but is significantly more persistent due to its covalent binding. We also provide the first reported in vivo antitumor evaluation of (−)-zampanolide where we determine that it has potent and persistent antitumor efficacy when delivered intratumorally. Future work on zampanolide to further evaluate its pharmacophore and determine ways to improve its systemic therapeutic window would make this compound a potential candidate for clinical development through its ability to circumvent taxane-resistance mechanisms.

AB - Microtubule-stabilizing agents (MSAs) are a class of compounds used in the treatment of triple-negative breast cancer (TNBC), a subtype of breast cancer where chemotherapy remains the standard-of-care for patients. Taxanes like paclitaxel and docetaxel have demonstrated efficacy against TNBC in the clinic, however new classes of MSAs need to be identified due to the rise of taxane resistance in patients. (−)-Zampanolide is a covalent microtubule stabilizer that can circumvent taxane resistance in vitro but has not been evaluated for in vivo antitumor efficacy. Here, we determine that (−)-zampanolide has similar potency and efficacy to paclitaxel in TNBC cell lines, but is significantly more persistent due to its covalent binding. We also provide the first reported in vivo antitumor evaluation of (−)-zampanolide where we determine that it has potent and persistent antitumor efficacy when delivered intratumorally. Future work on zampanolide to further evaluate its pharmacophore and determine ways to improve its systemic therapeutic window would make this compound a potential candidate for clinical development through its ability to circumvent taxane-resistance mechanisms.

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