Nanocarrier of α-Tocopheryl Succinate Based on a Copolymer Derivative of (4,7-dichloroquinolin-2-yl)methanol and Its Cytotoxicity against a Breast Cancer Cell Line

Author:

Valle Hernán12,Palao-Suay Raquel34,Aguilar María Rosa34ORCID,Lerma Tulio A.56,Palencia Manuel5ORCID,Mangalaraja Ramalinga Viswanathan7ORCID,Guzmán Leonardo8,Pérez Sotelo Dairo1,Becerra José2

Affiliation:

1. Chemistry Department, Faculty of Basic Sciences, University of Córdoba, Montería 230002, Colombia

2. Laboratory of Chemistry of Natural Products, Department of Botany, Faculty of Natural and Oceanographic Sciences, University of Concepción, Casilla 160-C, Concepción 4070386, Chile

3. Group of Biomaterials, Department of Polymeric Nanomaterials and Biomaterials, Institute of Polymer Science and Technology, Spanish National Research Council (ICTP-CSIC), 28006 Madrid, Spain

4. Networking Biomedical Research Centre in Bioengineering, Biomaterials and Nanomedicine, CIBER-BBN, 28029 Madrid, Spain

5. Research Group in Science with Technological Applications (GI-CAT), Department of Chemistry, Faculty of Natural and Exact Science, University of Valle, Cali 760042, Colombia

6. Mindtech Research Group (Mindtech-RG), Mindtech s.a.s., Barranquilla 080006, Colombia

7. Faculty of Engineering and Sciences, Adolfo Ibáñez University, Diagonal Las Torres 2640, Peñalolén, Santiago 7941169, Chile

8. Laboratory of Molecular Neurobiology, Department of Physiology, Faculty of Biological Sciences, University of Concepción, Casilla 160-C, Concepción 4070386, Chile

Abstract

In order to improve the water solubility and, therefore, bioavailability and therapeutic activity of anticancer hydrophobic drug α-tocopherol succinate (α-TOS), in this work, copolymers were synthesized via free radicals from QMES (1-[4,7-dichloroquinolin-2-ylmethyl]-4-methacryloyloxyethyl succinate) and VP (N-vinyl-2-pirrolidone) using different molar ratios, and were used to nanoencapsulate and deliver α-TOS into cancer cells MCF-7. QMES monomer was chosen because the QMES pendant group in the polymer tends to hydrolyze to form free 4,7-dichloro-2-quinolinemethanol (QOH), which also, like α-TOS, exhibit anti-proliferative effects on cancerous cells. From the QMES-VP 30:70 (QMES-30) and 40:60 (QMES-40) copolymers obtained, it was possible to prepare aqueous suspensions of empty nanoparticles (NPs) loaded with α-TOS by nanoprecipitation. The diameter and encapsulation efficiency (%EE) of the QMES-30 NPs loaded with α-TOS were 128.6 nm and 52%; while for the QMES-40 NPs loaded with α-TOS, they were 148.8 nm and 65%. The results of the AlamarBlue assay at 72 h of treatment show that empty QMES-30 NPs (without α-TOS) produced a marked cytotoxic effect on MCF-7 breast cancer cells, corresponding to an IC50 value of 0.043 mg mL−1, and importantly, they did not exhibit cytotoxicity against healthy HUVEC cells. Furthermore, NP-QMES-40 loaded with α-TOS were cytotoxic with an IC50 value of 0.076 mg mL−1, demonstrating a progressive release of α-TOS; however, the latter nanoparticles were also cytotoxic to healthy cells in the range of the assayed concentrations. These results contribute to the search for a new polymeric nanocarrier of QOH, α-TOS or other hydrophobic drugs for the treatment of cancer or others diseases treatable with these drugs.

Funder

National Agency for Research and Development of Chile

MICINN, Spain

Publisher

MDPI AG

Subject

Polymers and Plastics,General Chemistry

Reference50 articles.

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