Rational Understanding of Loading and Release of Doxorubicin by UV-Light- and pH-Responsive Poly(NIPAM- co-SPMA) Micelle-like Aggregates

Fernando Espinola-Portilla; Fanny d'Orlyé; Laura Trapiella-Alfonso; Silvia Gutiérrez-Granados; Gonzalo Ramírez-García; Anne Varenne

doi:10.1021/acs.molpharmaceut.2c00690

Rational Understanding of Loading and Release of Doxorubicin by UV-Light- and pH-Responsive Poly(NIPAM- co-SPMA) Micelle-like Aggregates

Mol Pharm. 2023 Mar 6;20(3):1490-1499. doi: 10.1021/acs.molpharmaceut.2c00690. Epub 2022 Dec 9.

Authors

Fernando Espinola-Portilla^{1

2

3}, Fanny d'Orlyé¹, Laura Trapiella-Alfonso¹, Silvia Gutiérrez-Granados², Gonzalo Ramírez-García³, Anne Varenne¹

Affiliations

¹ Chimie ParisTech PSL, CNRS 8060, Institute of Chemistry for Life and Health (i-CLeHS), Paris 75005, France.
² Departamento de Química, Universidad de Guanajuato, Guanajuato 36050, México.
³ Biofunctional Nanomaterials Laboratory, Centro de Física Aplicada y Tecnología Avanzada, Universidad Nacional Autónoma de México, Querétaro 76230, México.

PMID: 36490379
DOI: 10.1021/acs.molpharmaceut.2c00690

Abstract

A deep understanding of the interactions between micelle-like aggregates and antineoplastic drugs is paramount to control their adequate delivery. Herein, Poly(NIPAM-co-SPMA) copolymer nanocarriers were synthesized according to our previous published methodology, and the loading and release of poorly and highly water-soluble doxorubicin forms (Dox and Dox-HCl, respectively) were evaluated upon UV light irradiation and pH-variation stimuli. Capillary electrophoresis (CE) coupled to a fluorescence detector (LIF) allowed us to specifically characterize these systems and deeply study the loading and release processes. For this purpose, varying concentrations of doxorubicin were tested, and the loading/release rates were indirectly quantified thanks to the "free" doxorubicin concentration in solution. This study highlighted that Dox loading (9.4 μg/mg) was more effective than Dox-HCl loading (5.5 μg/mg). In contrast, 68 and 74% of Dox-HCl were respectively released after 2 min upon pH variation (from 7.4 to 6.0) and combined UV + pH 6.0 stimuli, while only 27% of Dox was invariably released upon application of the same stimuli. These results are coherent with the characteristics of both DoxHCl and Dox: Electrostatic interactions between Dox-HCl and the micelle-membrane structure (NIPAM) seemed predominant, while hydrophobic interactions were expected between Dox and the SP moieties at the inner part of the micelle-like aggregate, leading to different behaviors in both loading and release of the two doxorubicin forms. For doxorubicin loading concentrations higher than 3 μM, the electrophoretic profiles presented an additional peak. Thanks to CE characterizations, this peak was attributed to the formation of a complex formed between the nonaggregated copolymer and the doxorubicin molecules. This report therefore undergoes deep characterization of the dynamic formation of different micelle/drug complexes involved in the global drug-delivery behavior and therefore contributes to the development of more effective stimuli-responsive nanocarriers.

Keywords: controlled drug delivery; micelle-like aggregates; smart polymers; spiropyran copolymer; stimuli-responsive polymers.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antineoplastic Agents*
Doxorubicin / chemistry
Drug Carriers / chemistry
Drug Delivery Systems / methods
Hydrogen-Ion Concentration
Micelles*
Polymers / chemistry
Ultraviolet Rays

Substances

Micelles
Doxorubicin
Antineoplastic Agents
Polymers
Drug Carriers