Inhibition of 3-D Tumor Spheroids by Timed-Released Hydrophilic and Hydrophobic Drugs from Multilayered Polymeric Microparticles
Wei Li Lee
School of Materials Science and Engineering, Nanyang Technological University, 50 Nanyang Avenue, 639798 Singapore
Search for more papers by this authorWei Mei Guo
Molecular Engineering Laboratory, A*STAR, Proteos #03–13, 61 Biopolis Drive, 138673 Singapore
Search for more papers by this authorVincent H. B. Ho
Molecular Engineering Laboratory, A*STAR, Proteos #03–13, 61 Biopolis Drive, 138673 Singapore
Search for more papers by this authorAmitaksha Saha
School of Materials Science and Engineering, Nanyang Technological University, 50 Nanyang Avenue, 639798 Singapore
Search for more papers by this authorHan Chung Chong
School of Biological Sciences, Nanyang Technological University, 60 Nanyang Drive, 637551 Singapore
Search for more papers by this authorNguan Soon Tan
School of Biological Sciences, Nanyang Technological University, 60 Nanyang Drive, 637551 Singapore
Search for more papers by this authorErn Yu Tan
Department of General Surgery, Tan Tock Seng Hospital, 11 Jalan Tan Tock Seng, 308433 Singapore
Search for more papers by this authorCorresponding Author
Say Chye Joachim Loo
School of Materials Science and Engineering, Nanyang Technological University, 50 Nanyang Avenue, 639798 Singapore
E-mail: [email protected]Search for more papers by this authorWei Li Lee
School of Materials Science and Engineering, Nanyang Technological University, 50 Nanyang Avenue, 639798 Singapore
Search for more papers by this authorWei Mei Guo
Molecular Engineering Laboratory, A*STAR, Proteos #03–13, 61 Biopolis Drive, 138673 Singapore
Search for more papers by this authorVincent H. B. Ho
Molecular Engineering Laboratory, A*STAR, Proteos #03–13, 61 Biopolis Drive, 138673 Singapore
Search for more papers by this authorAmitaksha Saha
School of Materials Science and Engineering, Nanyang Technological University, 50 Nanyang Avenue, 639798 Singapore
Search for more papers by this authorHan Chung Chong
School of Biological Sciences, Nanyang Technological University, 60 Nanyang Drive, 637551 Singapore
Search for more papers by this authorNguan Soon Tan
School of Biological Sciences, Nanyang Technological University, 60 Nanyang Drive, 637551 Singapore
Search for more papers by this authorErn Yu Tan
Department of General Surgery, Tan Tock Seng Hospital, 11 Jalan Tan Tock Seng, 308433 Singapore
Search for more papers by this authorCorresponding Author
Say Chye Joachim Loo
School of Materials Science and Engineering, Nanyang Technological University, 50 Nanyang Avenue, 639798 Singapore
E-mail: [email protected]Search for more papers by this authorAbstract
First-line cancer chemotherapy necessitates high parenteral dosage and repeated dosing of a combination of drugs over a prolonged period. Current commercially available chemotherapeutic agents, such as Doxil and Taxol, are only capable of delivering single drug in a bolus dose. The aim of this study is to develop dual-drug-loaded, multilayered microparticles and to investigate their antitumor efficacy compared with single-drug-loaded particles. Results show hydrophilic doxorubicin HCl (DOX) and hydrophobic paclitaxel (PTX) localized in the poly(dl-lactic-co-glycolic acid, 50:50) (PLGA) shell and in the poly(l-lactic acid) (PLLA) core, respectively. The introduction of poly[(1,6-bis-carboxyphenoxy) hexane] (PCPH) into PLGA/PLLA microparticles causes PTX to be localized in the PLLA and PCPH mid-layers, whereas DOX is found in both the PLGA shell and core. PLGA/PLLA/PCPH microparticles with denser shells allow better control of DOX release. A delayed release of PTX is observed with the addition of PCPH. Three-dimensional MCF-7 spheroid studies demonstrate that controlled co-delivery of DOX and PTX from multilayered microparticles produces a greater reduction in spheroid growth rate compared with single-drug-loaded particles. This study provides mechanistic insights into how distinctive structure of multilayered microparticles can be designed to modulate the release profiles of anticancer drugs, and how co-delivery can potentially provide better antitumor response.
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