2026-06-07T18:58:41Zhttps://docta.ucm.es/rest/oai/request

oai:docta.ucm.es:20.500.14352/83122023-08-25T20:00:43Zcom_20.500.14352_14col_20.500.14352_15

Docta Complutense author Ovejero Paredes, Karina author Díaz García, Diana author García Almodóvar, Victoria author Lozano Chamizo, Laura author Marciello, Marzia author Díaz-Sánchez, Miguel author Prashar, Sanjiv author Gómez-Ruiz, Santiago author Filice, Marco 2023-06-17T09:10:01Z 2023-06-17T09:10:01Z 2020-01-12 2072-6694 10.3390/cancers12010187 https://hdl.handle.net/20.500.14352/8312 https://doi.org/10.3390/cancers12010187 https://www.mdpi.com/2072-6694/12/1/187 Three different multifunctional nanosystems based on the tethering onto mesoporous silica nanoparticles (MSN) of different fragments such as an organotin-based cytotoxic compound Ph3Sn{SCH2CH2CH2Si(OMe)3} (MSN-AP-Sn), a folate fragment (MSN-AP-FA-Sn), and an enzyme-responsive peptide able to release the metallodrug only inside cancer cells (MSN-AP-FA-PEP-S-Sn), have been synthesized and fully characterized by applying physico-chemical techniques. After that, an in vitro deep determination of the therapeutic potential of the achieved multifunctional nanovectors was carried out. The results showed a high cytotoxic potential of the MSN-AP-FA-PEP-S-Sn material against triple negative breast cancer cell line (MDA-MB-231). Moreover, a dose-dependent metallodrug-related inhibitory effect on the migration mechanism of MDA-MB-231 tumor cells was shown. Subsequently, the organotin-functionalized nanosystems have been further modified with the NIR imaging agent Alexa Fluor 647 to give three different theranostic silica-based nanoplatforms, namely, MSN-AP-Sn-AX (AX-1), MSN-AP-FA-Sn-AX (AX-2), and MSN-AP-FA-PEP-S-Sn-AX (AX-3). Their in vivo potential as theranostic markers was further evaluated in a xenograft mouse model of human breast adenocarcinoma. Owing to the combination of the receptor-mediated site targeting and the specific fine-tuned release mechanism of the organotin metallodrug, the nanotheranostic drug MSN-AP-FA-PEP-S-Sn-AX (AX-3) has shown targeted diagnostic ability in combination with enhanced therapeutic activity by promoting the inhibition of tumor growth with reduced hepatic and renal toxicity upon the repeated administration of the multifunctional nanodrug. eng Atribución 3.0 España Multifunctional Silica-Based Nanoparticles with Controlled Release of Organotin Metallodrug for Targeted Theranosis of Breast Cancer journal article URL https://docta.ucm.es/bitstreams/cd6292d3-0eaf-45d8-8560-3052e4ca0d5d/download File MD5 c88066fe1f5b2acb6898a210116b8759 6793057 application/pdf cancers-12-00187.pdf