Multitargeting Pt(IV) Derivatives of Cisplatin or Oxaliplatin Inhibit Tumor Growth in Mice without Inducing Neuropathic Pain

Tomer Babu; Ram Pravin Kumar Muthuramalingam; Wei Heng Chng; Jia Ning Nicolette Yau; Sourav Acharya; Nurit Engelmayer; Rachel Feldman-Goriachnik; Shaya Lev; Giorgia Pastorin; Alexander Binshtok; Menachem Hanani; Dan Gibson

doi:10.1021/acs.jmedchem.4c02263

Multitargeting Pt(IV) Derivatives of Cisplatin or Oxaliplatin Inhibit Tumor Growth in Mice without Inducing Neuropathic Pain

Tomer Babu, Ram Pravin Kumar Muthuramalingam, Wei Heng Chng, Jia Ning Nicolette Yau, Sourav Acharya, Nurit Engelmayer, Rachel Feldman-Goriachnik, Shaya Lev, Giorgia Pastorin^*, Alexander Binshtok^*, Menachem Hanani^*, Dan Gibson^*

^*Corresponding author for this work

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

Abstract

Cisplatin and oxaliplatin are Pt(II) anticancer agents that are used to treat several cancers, usually in combination with other drugs. Their efficacy is diminished by dose-limiting peripheral neuropathy (PN) that affects ∼70% of patients. PN is caused by selective accumulation of the platinum drugs in the dorsal root ganglia (DRG), which overexpress transporters for cisplatin and oxaliplatin. To date, no drug is recommended for the prevention of PN. We report that Pt(IV) prodrugs of cisplatin or oxaliplatin do not induce neuropathic pain in mice, likely due to the lower accumulation of platinum in the DRG compared with Pt(II) drugs. Moreover, the multitargeting prodrug that combines cisplatin with paclitaxel, both strong inducers of PN, efficiently inhibited tumor growth in vivo without inducing neuropathic pain. The high antitumor efficacy of Pt(IV) prodrugs and their micellar counterparts and the low level of neuropathic pain associated with them make them ideal candidates for clinical use in cancer therapy.

Original language	English
Journal	Journal of Medicinal Chemistry
DOIs	https://doi.org/10.1021/acs.jmedchem.4c02263
State	Accepted/In press - 2025

Bibliographical note

Publisher Copyright:
© 2025 The Authors. Published by American Chemical Society.

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Babu, T., Muthuramalingam, R. P. K., Chng, W. H., Yau, J. N. N., Acharya, S., Engelmayer, N., Feldman-Goriachnik, R., Lev, S., Pastorin, G., Binshtok, A., Hanani, M., & Gibson, D. (Accepted/In press). Multitargeting Pt(IV) Derivatives of Cisplatin or Oxaliplatin Inhibit Tumor Growth in Mice without Inducing Neuropathic Pain. Journal of Medicinal Chemistry. https://doi.org/10.1021/acs.jmedchem.4c02263

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title = "Multitargeting Pt(IV) Derivatives of Cisplatin or Oxaliplatin Inhibit Tumor Growth in Mice without Inducing Neuropathic Pain",

abstract = "Cisplatin and oxaliplatin are Pt(II) anticancer agents that are used to treat several cancers, usually in combination with other drugs. Their efficacy is diminished by dose-limiting peripheral neuropathy (PN) that affects ∼70% of patients. PN is caused by selective accumulation of the platinum drugs in the dorsal root ganglia (DRG), which overexpress transporters for cisplatin and oxaliplatin. To date, no drug is recommended for the prevention of PN. We report that Pt(IV) prodrugs of cisplatin or oxaliplatin do not induce neuropathic pain in mice, likely due to the lower accumulation of platinum in the DRG compared with Pt(II) drugs. Moreover, the multitargeting prodrug that combines cisplatin with paclitaxel, both strong inducers of PN, efficiently inhibited tumor growth in vivo without inducing neuropathic pain. The high antitumor efficacy of Pt(IV) prodrugs and their micellar counterparts and the low level of neuropathic pain associated with them make them ideal candidates for clinical use in cancer therapy.",

author = "Tomer Babu and Muthuramalingam, {Ram Pravin Kumar} and Chng, {Wei Heng} and Yau, {Jia Ning Nicolette} and Sourav Acharya and Nurit Engelmayer and Rachel Feldman-Goriachnik and Shaya Lev and Giorgia Pastorin and Alexander Binshtok and Menachem Hanani and Dan Gibson",

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year = "2025",

doi = "10.1021/acs.jmedchem.4c02263",

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journal = "Journal of Medicinal Chemistry",

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T1 - Multitargeting Pt(IV) Derivatives of Cisplatin or Oxaliplatin Inhibit Tumor Growth in Mice without Inducing Neuropathic Pain

AU - Babu, Tomer

AU - Muthuramalingam, Ram Pravin Kumar

AU - Chng, Wei Heng

AU - Yau, Jia Ning Nicolette

AU - Acharya, Sourav

AU - Engelmayer, Nurit

AU - Feldman-Goriachnik, Rachel

AU - Lev, Shaya

AU - Pastorin, Giorgia

AU - Binshtok, Alexander

AU - Hanani, Menachem

AU - Gibson, Dan

PY - 2025

Y1 - 2025

N2 - Cisplatin and oxaliplatin are Pt(II) anticancer agents that are used to treat several cancers, usually in combination with other drugs. Their efficacy is diminished by dose-limiting peripheral neuropathy (PN) that affects ∼70% of patients. PN is caused by selective accumulation of the platinum drugs in the dorsal root ganglia (DRG), which overexpress transporters for cisplatin and oxaliplatin. To date, no drug is recommended for the prevention of PN. We report that Pt(IV) prodrugs of cisplatin or oxaliplatin do not induce neuropathic pain in mice, likely due to the lower accumulation of platinum in the DRG compared with Pt(II) drugs. Moreover, the multitargeting prodrug that combines cisplatin with paclitaxel, both strong inducers of PN, efficiently inhibited tumor growth in vivo without inducing neuropathic pain. The high antitumor efficacy of Pt(IV) prodrugs and their micellar counterparts and the low level of neuropathic pain associated with them make them ideal candidates for clinical use in cancer therapy.

AB - Cisplatin and oxaliplatin are Pt(II) anticancer agents that are used to treat several cancers, usually in combination with other drugs. Their efficacy is diminished by dose-limiting peripheral neuropathy (PN) that affects ∼70% of patients. PN is caused by selective accumulation of the platinum drugs in the dorsal root ganglia (DRG), which overexpress transporters for cisplatin and oxaliplatin. To date, no drug is recommended for the prevention of PN. We report that Pt(IV) prodrugs of cisplatin or oxaliplatin do not induce neuropathic pain in mice, likely due to the lower accumulation of platinum in the DRG compared with Pt(II) drugs. Moreover, the multitargeting prodrug that combines cisplatin with paclitaxel, both strong inducers of PN, efficiently inhibited tumor growth in vivo without inducing neuropathic pain. The high antitumor efficacy of Pt(IV) prodrugs and their micellar counterparts and the low level of neuropathic pain associated with them make them ideal candidates for clinical use in cancer therapy.

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Multitargeting Pt(IV) Derivatives of Cisplatin or Oxaliplatin Inhibit Tumor Growth in Mice without Inducing Neuropathic Pain

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