Magnetically modified-mitoxantrone mesoporous organosilica drugs: an emergent multimodal nanochemotherapy for breast cancer

dc.contributor.authorRomaní Cubells , Eva
dc.contributor.authorMartínez Erro, Samuel
dc.contributor.authorMorales, Victoria
dc.contributor.authorChocarro Calvo, Ana
dc.contributor.authorGarcía Martinez, Jose M.
dc.contributor.authorSanz, Raúl
dc.contributor.authorGarcía Jimenez, Custodia
dc.contributor.authorGarcía Muñoz, Rafael
dc.date.accessioned2025-01-14T09:10:59Z
dc.date.available2025-01-14T09:10:59Z
dc.date.issued2024-04-14
dc.descriptionThis work was supported by the Agencia Estatal de Investigación of the Spanish Government for Science, Innovation and Universities [Grant Nos. CTQ2017-88642-R, PID2021-1252160B-100, PID2022-136729OB-I00, PID2019- 104867RB-I00/AEI/https://doi.org/10.13039/501100011033] and Comunidad de Madrid [PRECICOLON-CM: P2022/BMD7212].
dc.description.abstractBackground Chemotherapy, the mainstay treatment for metastatic cancer, presents serious side effects due to off-target exposure. In addition to the negative impact on patients’ quality of life, side effects limit the dose that can be administered and thus the efficacy of the drug. Encapsulation of chemotherapeutic drugs in nanocarriers is a promising strategy to mitigate these issues. However, avoiding premature drug release from the nanocarriers and selectively targeting the tumour remains a challenge. Results In this study, we present a pioneering method for drug integration into nanoparticles known as mesoporous organosilica drugs (MODs), a distinctive variant of periodic mesoporous organosilica nanoparticles (PMOs) in which the drug is an inherent component of the silica nanoparticle structure. This groundbreaking approach involves the chemical modification of drugs to produce bis-organosilane prodrugs, which act as silica precursors for MOD synthesis. Mitoxantrone (MTO), a drug used to treat metastatic breast cancer, was selected for the development of MTO@MOD nanomedicines, which demonstrated a significant reduction in breast cancer cell viability. Several MODs with different amounts of MTO were synthesised and found to be efficient nanoplatforms for the sustained delivery of MTO after biodegradation. In addition, Fe3O4 NPs were incorporated into the MODs to generate magnetic MODs to actively target the tumour and further enhance drug efficacy. Importantly, magnetic MTO@MODs underwent a Fenton reaction, which increased cancer cell death twofold compared to non-magnetic MODs. Conclusions A new PMO-based material, MOD nanomedicines, was synthesised using the chemotherapeutic drug MTO as a silica precursor. MTO@MOD nanomedicines demonstrated their efficacy in significantly reducing the viability of breast cancer cells. In addition, we incorporated Fe3O4 into MODs to generate magnetic MODs for active tumour targeting and enhanced drug efficacy by ROS generation. These findings pave the way for the designing of silica-based multitherapeutic nanomedicines for cancer treatment with improved drug delivery, reduced side effects and enhanced efficacy.
dc.identifier.citationRomaní -Cubells, E., Martínez-Erro, S., Morales, V. et al. Magnetically modified-mitoxantrone mesoporous organosilica drugs: an emergent multimodal nanochemotherapy for breast cancer. J Nanobiotechnol 22, 249 (2024). https://doi.org/10.1186/s12951-024-02522-4
dc.identifier.doihttps://doi.org/10.1186/s12951-024-02522-4
dc.identifier.issn1477-3155
dc.identifier.urihttps://hdl.handle.net/10115/55678
dc.language.isoen
dc.publisherSpringer Nature
dc.rightsAttribution 4.0 Internationalen
dc.rights.accessRightsinfo:eu-repo/semantics/openAccess
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/
dc.subjectPeriodic mesoporous organosilica (PMO)
dc.subjectMagnetic mesoporous organosilica drugs (MOD)
dc.subjectDrug delivery systems
dc.subjectMitoxantrone
dc.subjectBreast cancer treatment
dc.subjectMagnetic nanomedicine
dc.titleMagnetically modified-mitoxantrone mesoporous organosilica drugs: an emergent multimodal nanochemotherapy for breast cancer
dc.typeArticle

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