Small circular RNAs as vaccines for cancer immunotherapy

被引:0
|
作者
Yu Zhang [1 ]
Xiang Liu [2 ]
Tingting Shen [1 ]
Qiyan Wang [2 ]
Shurong Zhou [1 ]
Suling Yang [1 ]
Shimiao Liao [1 ]
Ting Su [1 ]
Lei Mei [3 ]
Bei Zhang [1 ]
Khoa Huynh [4 ]
Linying Xie [4 ]
Youzhong Guo [5 ]
Chunqing Guo [6 ]
Katarzyna M. Tyc [7 ]
Xufeng Qu [4 ]
Xiang-Yang Wang [4 ]
Jinze Liu [7 ]
Guizhi Zhu [4 ]
机构
[1] University of Michigan,Department of Pharmaceutical Sciences, College of Pharmacy
[2] Chinese Academy of Sciences,The Key Laboratory of Zhejiang Province for Aptamers and Theranostics, Hangzhou Institute of Medicine (HIM)
[3] Donghua University,College of Biological Science and Medical Engineering
[4] Virginia Commonwealth University,Department of Biostatistics, School of Medicine; Bioinformatics Shared Resource, Massey Cancer Center
[5] Virginia Commonwealth University,Genomics Core
[6] Virginia Commonwealth University,Department of Medicinal Chemistry, School of Pharmacy
[7] Virginia Commonwealth University,Department of Human and Molecular Genetics and Institute of Molecular Medicine, School of Medicine; Massey Cancer Center
[8] University of Michigan,Bioinnovations in Brain Cancer, Biointerfaces Institute; The Developmental Therapeutics Program, Rogel Cancer Center; Center for RNA Biomedicine; MI
关键词
D O I
10.1038/s41551-025-01344-5
中图分类号
学科分类号
摘要
Messenger RNA vaccines have shown strong prophylactic efficacy against viral infections. Here we show that antigen-encoding small circular RNAs (circRNAs) loaded in lipid nanoparticles elicit potent and durable T cell responses for robust tumour immunotherapy after subcutaneous injection in mice, particularly when combined with immune checkpoint inhibition. The small circRNA vaccines are highly stable and show low levels of activation of protein kinase R as well as low cytotoxicity, enabling long-lasting antigen translation (longer than 1 week in cells). Relative to large protein-encoding unmodified or modified mRNAs and circRNAs, small circRNA vaccines elicited up to 10-fold antigen-specific T cells in mice and accounted for 30–75% of the total peripheral CD8+ T cells over 6 months. Small circRNA vaccines encoding tumour-associated antigens, neoantigens and oncoviral or viral antigens elicited substantial CD8+ and CD4+ T cell responses in young adult mice and in immunosenescent aged mice. Combined with immune checkpoint inhibition, monovalent and multivalent circRNA vaccines reduced tumour-induced immunosuppression and inhibited poorly immunogenic mouse tumours, including melanoma resistant to immune checkpoint blockade.
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页码:249 / 267
页数:18
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