Preclinical Assessment of Enhanced Chemodynamic Therapy by an FeMnO x -Based Nanocarrier: Tumor-Microenvironment-Mediated Fenton Reaction and ROS-Induced Chemotherapeutic for Boosted Antitumor Activity.
Worku Batu DirersaTzu-Chun KanGirum GetachewAswandi WibriantoSonjid OchirbatAkash S RasalJungshan ChangJia-Yaw ChangPublished in: ACS applied materials & interfaces (2023)
In recent studies, iron-containing Fenton nanocatalysts have demonstrated significant promise for clinical use due to their effective antitumor activity and low cytotoxicity. A new approach was reported in this work utilizing cation exchange synthesis to fabricate FeMnO x nanoparticles (NPs) that boost Fenton reactions and responses to the tumor microenvironment (TME) for chemodynamic therapy (CDT) and chemotherapy (CT). Within the TME, the redox metal pair of Fe 2+ /Mn 2+ helps break down endogenous hydrogen peroxide (H 2 O 2 ) into very harmful hydroxyl radicals (•OH) while simultaneously deactivating glutathione (GSH) to boost CDT performance. To further enhance the therapeutic potential, FeMnO x NPs were encapsulated with thioketal-linked camptothecin (CPT-TK-COOH), a reactive oxygen species (ROS)-responsive prodrug, achieving a high CPT-loading capacity of up to 51.1%. Upon ROS generation through the Fenton reaction, the prodrug TK linkage was disrupted, releasing 80% of the CPT payload within 48 h. Notably, FeMnO x @CPT exhibited excellent dual-modal imaging capabilities, enabling magnetic resonance and fluorescence imaging for image-guided therapy. In vitro studies showed the cytocompatibility of FeMnO x NPs using MDA-Mb-231 and 4T1 cells, but in the presence of H 2 O 2 , they induced significant cytotoxicity, resulting in 80% cell death through CDT and CT effects. Upon intravenous administration, FeMnO x @CPT displayed remarkable tumor accumulation, which enhanced tumor suppression in xenografts through improved CDT and CT effects. Moreover, no significant adverse effects were observed in the FeMnO x NP-treated animals. In the current study, the FeMnO x @CPT anticancer platform, with its boosted •OH-producing capability and ROS-cleavable drug release, has been validated utilizing in vitro and animal studies, suggesting its capacity as a viable strategy for clinical trials.
Keyphrases
- hydrogen peroxide
- cell death
- reactive oxygen species
- drug release
- fluorescence imaging
- magnetic resonance
- contrast enhanced
- nitric oxide
- drug delivery
- dna damage
- computed tomography
- wastewater treatment
- clinical trial
- image quality
- dual energy
- cancer therapy
- diabetic rats
- photodynamic therapy
- high glucose
- high resolution
- cell cycle arrest
- magnetic resonance imaging
- positron emission tomography
- case control
- squamous cell carcinoma
- cell therapy
- low dose
- stem cells
- high throughput
- machine learning
- radiation therapy
- ionic liquid
- randomized controlled trial
- bone marrow
- human immunodeficiency virus
- mass spectrometry
- deep learning
- metal organic framework
- functional connectivity
- men who have sex with men
- double blind
- hiv testing