Anti-cancer liposomal chemophototherapy using bilayer-localized photosensitizer and cabazitaxel

Photodynamic therapy (PDT) is a non-invasive tumor ablation modality that can be enhanced in combination with concurrent chemotherapy. Previously, we demonstrated that liposomes containing a bilayer-anchored photosensitizer (porphyrin-phospholipid; PoP) can be loaded with drugs in their aqueous core...

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Bibliographic Details
Published in:Nano research 2022-05, Vol.15 (5), p.4302-4309
Main Authors: Sun, Boyang, Ghosh, Sanjana, He, Xuedan, Huang, Wei-Chiao, Quinn, Breandan, Tian, Meiling, Jahagirdar, Dushyant, Mabrouk, Moustafa T., Ortega, Joaquin, Zhang, Yumiao, Shao, Shuai, Lovell, Jonathan F.
Format: Article
Language:English
Subjects:
Ablation
Antitumor agents
Atomic/Molecular Structure and Spectra
Biocompatibility
Biomedicine
Biotechnology
Chemistry and Materials Science
Chemotherapy
Condensed Matter Physics
Cytotoxicity
Drug delivery
Drug delivery systems
Hydrophobicity
Intravenous administration
Irradiation
Lasers
Liposomes
Materials Science
Nanotechnology
Pharmacokinetics
Phospholipids
Photodynamic therapy
Porphyrins
Research Article
Stability analysis
Toxicity
Tumors
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Summary:Photodynamic therapy (PDT) is a non-invasive tumor ablation modality that can be enhanced in combination with concurrent chemotherapy. Previously, we demonstrated that liposomes containing a bilayer-anchored photosensitizer (porphyrin-phospholipid; PoP) can be loaded with drugs in their aqueous core to improve drug delivery and tumor ablation upon target tissue irradiation with red-light. In the present work, we demonstrate that this concept can be extended to drugs loaded within the hydrophobic bilayer of liposomes. Cabazitaxel (CTX) is a potent second generation taxane anti-cancer drug that was loaded in the bilayer of liposomes also containing 0.1 molar% PoP, generating CTX-loaded PoP liposomes (CTX-PoP-Lip). CTX-PoP-Lip showed unilamellar vesicle morphology, and exhibited integrity in storage and serum, while maintaining drug stability under laser irradiation. In vitro cell killing evaluation showed that red-light laser irradiation induced cytotoxicity in cells incubated with CTX-PoP-Lip, compared to control treatments. In vivo pharmacokinetic analysis revealed that following intravenous administration to mice, CTX and PoP exhibited somewhat altered circulation profiles, suggesting that the CTX may have exchanged with serum factors in blood. Nevertheless, when a single treatment of CTX-PoP-Lip with laser irradiation was administered to mice bearing human MIA Paca-2 tumors, tumors were effectively ablated whereas the equivalent chemotherapy and PDT monotherapies were ineffective. These results demonstrate the versatility of liposome delivery systems for achieving tumor ablation with chemophototherapy.
ISSN:1998-0124
1998-0000
DOI:10.1007/s12274-022-4090-3