Literature DB >> 32596861

On-Demand Autophagy Cascade Amplification Nanoparticles Precisely Enhanced Oxaliplatin-Induced Cancer Immunotherapy.

Xuhui Wang1, Man Li1, Kebai Ren1, Chunyu Xia1, Jianping Li1, Qianwen Yu1, Yue Qiu1, Zhengze Lu1, Yang Long1, Zhirong Zhang1, Qin He1.   

Abstract

Chemoimmunotherapy-induced antitumor immune response is highly dependent on tumor autophagy. When tumor cells are treated with chemoimmunotherapy, timely overactivated autophagy can not only lead more tumor cells to death, but also participate in the endogenous antigen presentation and immune stimulators secretion of dying cells, thus plays a vital role. However, timely and accurately overactivated tumor autophagy during chemoimmunotherapy is of great difficulty. Here, an on-demand autophagy cascade amplification nanoparticle (ASN) is reported to boost oxaliplatin-induced cancer immunotherapy. ASN is prepared by self-assemble of autophagy-responsible C-TFG micelle and is followed by electrostatic binding of oxaliplatin prodrug (HA-OXA). After entering tumor cells, the HA-OXA shell of ASN first responds to the reduction microenvironment and releases oxaliplatin to trigger tumor immunogenic cell death and mildly stimulates tumor autophagy. Then, the exposed C-TFG micelle can sensitively respond to oxaliplatin-induced autophagy and release a powerful autophagy inducer STF-62247, which precisely transforms autophagy to "overactivated" condition, leading tumor cells to autophagic death and enhance subsequent tumor antigen processing of the dying cells. In CT26 tumor-bearing mice, ASN exhibits optimal immune stimulation and antitumor efficiency due to its on-demand autophagy induction ability.
© 2020 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.

Entities:  

Keywords:  autophagic cell death; autophagy activation; autophagy-responsive; immunogenic cell death; oxaliplatin prodrug

Mesh:

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Year:  2020        PMID: 32596861     DOI: 10.1002/adma.202002160

Source DB:  PubMed          Journal:  Adv Mater        ISSN: 0935-9648            Impact factor:   30.849


  7 in total

1.  Autophagy responsive intra-intercellular delivery nanoparticles for effective deep solid tumor penetration.

Authors:  Fengling Wang; Dandan Xie; Wenjing Lai; Min Zhou; Jie Wang; Rufu Xu; Jingbing Huang; Rong Zhang; Guobing Li
Journal:  J Nanobiotechnology       Date:  2022-06-25       Impact factor: 9.429

Review 2.  Emerging nanomedicines for effective breast cancer immunotherapy.

Authors:  Amirhossein Bahreyni; Yasir Mohamud; Honglin Luo
Journal:  J Nanobiotechnology       Date:  2020-12-09       Impact factor: 10.435

Review 3.  Targeting regulated cell death in tumor nanomedicines.

Authors:  Qinghu Zeng; Xiangyi Ma; Yangmeihui Song; Qiqing Chen; Qiuling Jiao; Liqiang Zhou
Journal:  Theranostics       Date:  2022-01-01       Impact factor: 11.556

Review 4.  Immunogenic Cell Death Activates the Tumor Immune Microenvironment to Boost the Immunotherapy Efficiency.

Authors:  Zhilin Li; Xiaoqin Lai; Shiqin Fu; Long Ren; Hao Cai; Hu Zhang; Zhongwei Gu; Xuelei Ma; Kui Luo
Journal:  Adv Sci (Weinh)       Date:  2022-06-02       Impact factor: 17.521

5.  Tumor-targeted dual-starvation therapy based on redox-responsive micelle nanosystem with co-loaded LND and BPTES.

Authors:  Zhenxiang Fu; Huiping Du; Siyu Meng; Mengjiao Yao; Pan Zhao; Xiang Li; Xinmin Zheng; Zhang Yuan; Hui Yang; Kaiyong Cai; Liangliang Dai
Journal:  Mater Today Bio       Date:  2022-10-03

Review 6.  Non-apoptotic cell death-based cancer therapy: Molecular mechanism, pharmacological modulators, and nanomedicine.

Authors:  Xuan Wang; Peng Hua; Chengwei He; Meiwan Chen
Journal:  Acta Pharm Sin B       Date:  2022-04-01       Impact factor: 14.903

7.  Biomimetic nanoparticles blocking autophagy for enhanced chemotherapy and metastasis inhibition via reversing focal adhesion disassembly.

Authors:  Yesi Shi; Gan Lin; Huili Zheng; Dan Mu; Hu Chen; Zhixiang Lu; Pan He; Yang Zhang; Chao Liu; Zhongning Lin; Gang Liu
Journal:  J Nanobiotechnology       Date:  2021-12-24       Impact factor: 10.435

  7 in total

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