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Cytosolic Delivery of Thiolated Neoantigen Nano‐Vaccine Combined with Immune Checkpoint Blockade to Boost Anti‐Cancer T Cell Immunity

Although tumor‐specific neoantigen‐based cancer vaccines hold tremendous potential, it still faces low cross‐presentation associated with severe degradation via endocytosis pathway. Herein, a thiolated nano‐vaccine allowing direct cytosolic delivery of neoantigen and Toll like receptor 9 agonist CpG...

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Autores principales: Zhang, Da, Lin, Ziguo, Wu, Ming, Cai, Zhixiong, Zheng, Youshi, He, Lei, Li, Zhenli, Zhou, Jie, Sun, Liqin, Chen, Geng, Zeng, Yongyi, Li, Juan, Liu, Jingfeng, Yang, Huanghao, Liu, Xiaolong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7967047/
https://www.ncbi.nlm.nih.gov/pubmed/33747739
http://dx.doi.org/10.1002/advs.202003504
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author Zhang, Da
Lin, Ziguo
Wu, Ming
Cai, Zhixiong
Zheng, Youshi
He, Lei
Li, Zhenli
Zhou, Jie
Sun, Liqin
Chen, Geng
Zeng, Yongyi
Li, Juan
Liu, Jingfeng
Yang, Huanghao
Liu, Xiaolong
author_facet Zhang, Da
Lin, Ziguo
Wu, Ming
Cai, Zhixiong
Zheng, Youshi
He, Lei
Li, Zhenli
Zhou, Jie
Sun, Liqin
Chen, Geng
Zeng, Yongyi
Li, Juan
Liu, Jingfeng
Yang, Huanghao
Liu, Xiaolong
author_sort Zhang, Da
collection PubMed
description Although tumor‐specific neoantigen‐based cancer vaccines hold tremendous potential, it still faces low cross‐presentation associated with severe degradation via endocytosis pathway. Herein, a thiolated nano‐vaccine allowing direct cytosolic delivery of neoantigen and Toll like receptor 9 agonist CpG‐ODN is developed. This approach is capable of bypassing the endo‐/lysosome degradation, increasing uptake and local concentration of neoantigen and CpG‐ODN to activate antigen‐presenting cells, significantly strengthening the anti‐cancer T‐cell immunity. In vivo immunization with thiolated nano‐vaccine enhanced the lymph organ homing and promoted the antigen presentation on dendritic cells, effectively inhibited tumor growth, and significantly prolonged the survival of H22‐bearing mice. Strikingly, further combination of the thiolated nano‐vaccine with anti‐programmed cell death protein‐1 antibody (αPD‐1) could efficiently reverse immunosuppression and enhance response rate of tumors, which led to enhanced tumor elimination, complete prevention of tumor re‐challenge, and long‐term survival above 150 d. Collectively, a versatile methodology to design cancer vaccines for strengthening anti‐cancer T‐cell immunity in solid tumors is presented, which could be further remarkably enhanced by combining with immune checkpoint inhibitors.
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spelling pubmed-79670472021-03-19 Cytosolic Delivery of Thiolated Neoantigen Nano‐Vaccine Combined with Immune Checkpoint Blockade to Boost Anti‐Cancer T Cell Immunity Zhang, Da Lin, Ziguo Wu, Ming Cai, Zhixiong Zheng, Youshi He, Lei Li, Zhenli Zhou, Jie Sun, Liqin Chen, Geng Zeng, Yongyi Li, Juan Liu, Jingfeng Yang, Huanghao Liu, Xiaolong Adv Sci (Weinh) Full Papers Although tumor‐specific neoantigen‐based cancer vaccines hold tremendous potential, it still faces low cross‐presentation associated with severe degradation via endocytosis pathway. Herein, a thiolated nano‐vaccine allowing direct cytosolic delivery of neoantigen and Toll like receptor 9 agonist CpG‐ODN is developed. This approach is capable of bypassing the endo‐/lysosome degradation, increasing uptake and local concentration of neoantigen and CpG‐ODN to activate antigen‐presenting cells, significantly strengthening the anti‐cancer T‐cell immunity. In vivo immunization with thiolated nano‐vaccine enhanced the lymph organ homing and promoted the antigen presentation on dendritic cells, effectively inhibited tumor growth, and significantly prolonged the survival of H22‐bearing mice. Strikingly, further combination of the thiolated nano‐vaccine with anti‐programmed cell death protein‐1 antibody (αPD‐1) could efficiently reverse immunosuppression and enhance response rate of tumors, which led to enhanced tumor elimination, complete prevention of tumor re‐challenge, and long‐term survival above 150 d. Collectively, a versatile methodology to design cancer vaccines for strengthening anti‐cancer T‐cell immunity in solid tumors is presented, which could be further remarkably enhanced by combining with immune checkpoint inhibitors. John Wiley and Sons Inc. 2021-01-29 /pmc/articles/PMC7967047/ /pubmed/33747739 http://dx.doi.org/10.1002/advs.202003504 Text en © 2021 The Authors. Advanced Science published by Wiley‐VCH GmbH This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Full Papers
Zhang, Da
Lin, Ziguo
Wu, Ming
Cai, Zhixiong
Zheng, Youshi
He, Lei
Li, Zhenli
Zhou, Jie
Sun, Liqin
Chen, Geng
Zeng, Yongyi
Li, Juan
Liu, Jingfeng
Yang, Huanghao
Liu, Xiaolong
Cytosolic Delivery of Thiolated Neoantigen Nano‐Vaccine Combined with Immune Checkpoint Blockade to Boost Anti‐Cancer T Cell Immunity
title Cytosolic Delivery of Thiolated Neoantigen Nano‐Vaccine Combined with Immune Checkpoint Blockade to Boost Anti‐Cancer T Cell Immunity
title_full Cytosolic Delivery of Thiolated Neoantigen Nano‐Vaccine Combined with Immune Checkpoint Blockade to Boost Anti‐Cancer T Cell Immunity
title_fullStr Cytosolic Delivery of Thiolated Neoantigen Nano‐Vaccine Combined with Immune Checkpoint Blockade to Boost Anti‐Cancer T Cell Immunity
title_full_unstemmed Cytosolic Delivery of Thiolated Neoantigen Nano‐Vaccine Combined with Immune Checkpoint Blockade to Boost Anti‐Cancer T Cell Immunity
title_short Cytosolic Delivery of Thiolated Neoantigen Nano‐Vaccine Combined with Immune Checkpoint Blockade to Boost Anti‐Cancer T Cell Immunity
title_sort cytosolic delivery of thiolated neoantigen nano‐vaccine combined with immune checkpoint blockade to boost anti‐cancer t cell immunity
topic Full Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7967047/
https://www.ncbi.nlm.nih.gov/pubmed/33747739
http://dx.doi.org/10.1002/advs.202003504
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