A Nano‐Autophagy Inhibitor Triggering Reciprocal Feedback Control of Cholesterol Depletion for Solid Tumor Therapy

Author:

Zhang Pengfei1ORCID,Shi Yanfeng2ORCID,Xu Yuanhong12ORCID,Liang Ye1,Huang Chao2,Zhong Di3,Zhang Zhilei1,Yu Yongbo1,Zhang Zhao1,Zhang Jianfeng1,Yu Lei2,Zuo Yuhui2,Wang Xinsheng1,Niu Haitao1

Affiliation:

1. Department of Urology the Affiliated Hospital of Qingdao University Qingdao 266003 China

2. Institute of Biomedical Engineering College of Life Sciences Qingdao University Qingdao 266071 China

3. Department of Genetics and Cell Biology Basic Medical College Qingdao University Qingdao Shandong 266071 China

Abstract

AbstractSolid tumors are characterized by enhanced metabolism of lipid, particularly cholesterol, inspiring the exploration of metabolic therapy through cholesterol oxidase (COD)‐mediated cholesterol deprivation. However, the therapeutic efficacy of COD is limited due to the hypoxic tumor microenvironment and the protective autophagy triggered by cholesterol deprivation. Herein, a combination therapy for metabolically treating solid tumors through COD in conjunction with molybdenum oxide nanodots (MONDs), which serve as both potent oxygen generators and autophagy inhibitors, is reported. MONDs convert H2O2 (arising from COD‐mediated cholesterol oxidation) into O2, which is then recycled by COD to form reciprocal feedback for cholesterol depletion. Concurrently, MONDs can overcome autophagy‐induced therapeutic resistance frequently occurring in conventional nutrient deprivation therapy by activating AKT/mTOR pathway phosphorylation. Combination therapy in the xenograft model results in an ≈5‐fold increase in therapeutic efficiency as compared with COD treatment alone. This functionally cooperative metabolic coupling strategy holds great promise as a novel polytherapy approach that will benefit patients with solid tumors.

Funder

National Natural Science Foundation of China

Publisher

Wiley

Subject

Pharmaceutical Science,Biomedical Engineering,Biomaterials

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