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Iron Oxide Nanoparticles as Autophagy Intervention Agents Suppress Hepatoma Growth by Enhancing Tumoricidal Autophagy

Yuexia Xie, Jiana Jiang, Qianyun Tang, Hanbing Zou, Xue Zhao, Hongmei Liu, Ding Ma, Chenlei Cai, Yan Zhou, Xiaojing Chen, Jun Pu, Peifeng Liu

2020Advanced Science56 citationsDOIOpen Access PDF

Abstract

Abstract The combined treatment with nanoparticles and autophagy inhibitors, such as chloroquine (CQ) and hydroxychloroquine (HCQ), is extensively explored for cancer therapy. However, the toxicity of autophagy inhibitors and their unselective for tumoricidal autophagy have seriously hindered the application of the combined treatment. In this study, a carboxy‐functional iron oxide nanoparticle (Fe 2 O 3 @DMSA) is designed and identified to significantly exert an antitumor effect without adding CQ or HCQ. Further investigation indicates that the effective inhibition effect of Fe 2 O 3 @DMSA alone on hepatoma growth is triggered by inhibiting the fusion of autophagosomes and lysosomes to enhance tumoricidal autophagy, which is induced by intracellular iron‐retention‐induced sustained reactive oxygen species (ROS) production. Furthermore, in two hepatoma‐bearing mouse models, Fe 2 O 3 @DMSA alone effectively suppresses the growth of tumors without obvious toxic side effects. These studies offer a promising strategy for cancer therapy.

Topics & Concepts

AutophagyReactive oxygen speciesHydroxychloroquineChloroquineIntracellularChemistryCancer researchPharmacologyCancer cellNanoparticlePinocytosisCancerCell biologyEndocytosisBiochemistryApoptosisMedicineBiologyReceptorNanotechnologyImmunologyCoronavirus disease 2019 (COVID-19)Materials scienceInternal medicineMalariaDiseaseInfectious disease (medical specialty)Autophagy in Disease and TherapySphingolipid Metabolism and SignalingExtracellular vesicles in disease
Iron Oxide Nanoparticles as Autophagy Intervention Agents Suppress Hepatoma Growth by Enhancing Tumoricidal Autophagy | Litcius