Redox-Responsive Comparison of Diselenide and Disulfide Core-Cross-Linked Micelles for Drug Delivery Application

Author:

Yadav Sonyabapu1ORCID,Ramesh Kalyan2ORCID,Reddy Obireddy Sreekanth3ORCID,Karthika Viswanathan3,Kumar Parveen3ORCID,Jo Sung-Han4,Yoo Seong II5,Park Sang-Hyug4,Lim Kwon Taek13ORCID

Affiliation:

1. Department of Smart Green Technology Engineering, Pukyong National University, Busan 48513, Republic of Korea

2. R&D Center, Devens Lab, SEQENS (CDMO) Pharmaceutical Solutions, Devens, MA 01434, USA

3. Major of Display Semiconductor Engineering, Pukyong National University, Busan 48513, Republic of Korea

4. Department of Biomedical Engineering, Pukyong National University, Busan 48513, Republic of Korea

5. Department of Polymer Engineering, Pukyong National University, Busan 48513, Republic of Korea

Abstract

In this study, diselenide (Se–Se) and disulfide (S–S) redox-responsive core-cross-linked (CCL) micelles were synthesized using poly(ethylene oxide)2k-b-poly(furfuryl methacrylate)1.5k (PEO2k-b-PFMA1.5k), and their redox sensitivity was compared. A single electron transfer-living radical polymerization technique was used to prepare PEO2k-b-PFMA1.5k from FMA monomers and PEO2k-Br initiators. An anti-cancer drug, doxorubicin (DOX), was incorporated into PFMA hydrophobic parts of the polymeric micelles, which were then cross-linked with maleimide cross-linkers, 1,6-bis(maleimide) hexane, dithiobis(maleimido) ethane and diselenobis(maleimido) ethane via Diels–Alder reaction. Under physiological conditions, the structural stability of both S–S and Se–Se CCL micelles was maintained; however, treatments with 10 mM GSH induced redox-responsive de-cross-linking of S–S and Se–Se bonds. In contrast, the S–S bond was intact in the presence of 100 mM H2O2, while the Se–Se bond underwent de-crosslinking upon the treatment. DLS studies revealed that the size and PDI of (PEO2k-b-PFMA1.5k-Se)2 micelles varied more significantly in response to changes in the redox environment than (PEO2k-b-PFMA1.5k-S)2 micelles. In vitro release studies showed that the developed micelles had a lower drug release rate at pH 7.4, whereas a higher release was observed at pH 5.0 (tumor environment). The micelles were non-toxic against HEK-293 normal cells, which revealed that they could be safe for use. Nevertheless, DOX-loaded S–S/Se–Se CCL micelles exhibited potent cytotoxicity against BT-20 cancer cells. Based on these results, the (PEO2k-b-PFMA1.5k-Se)2 micelles can be more sensitive drug carriers than (PEO2k-b-PFMA1.5k-S)2 micelles.

Funder

National Research Foundation of Korea

Publisher

MDPI AG

Subject

Pharmaceutical Science

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