Systemic RNA delivery to dendritic cells exploits antiviral defence for cancer immunotherapy

抗原 生物 癌症免疫疗法 启动(农业) 核糖核酸 效应器 免疫疗法 细胞生物学 免疫学 T细胞 抗原提呈细胞 树突状细胞 免疫系统 基因 遗传学 植物 发芽
作者
Lena M. Kranz,Mustafa Diken,Heinrich Haas,Sebastian Kreiter,Carmen Loquai,Kerstin C. Reuter,Martin Meng,Daniel Fritz,Fulvia Vascotto,Hossam Hefesha,Christian Grunwitz,Mathias Vormehr,Yves Hüsemann,Abderraouf Selmi,Andreas N. Kuhn,Janina Buck,Evelyna Derhovanessian,Richard Rae,Sebastian Attig,Jan Diekmann,Robert A. Jabulowsky,Sandra Heesch,Jessica C. Hassel,Peter Langguth,Stephan Grabbe,Christoph Huber,Özlem Türeci,Uğur Şahin
出处
期刊:Nature [Springer Nature]
卷期号:534 (7607): 396-401 被引量:1362
标识
DOI:10.1038/nature18300
摘要

Lymphoid organs, in which antigen presenting cells (APCs) are in close proximity to T cells, are the ideal microenvironment for efficient priming and amplification of T-cell responses. However, the systemic delivery of vaccine antigens into dendritic cells (DCs) is hampered by various technical challenges. Here we show that DCs can be targeted precisely and effectively in vivo using intravenously administered RNA-lipoplexes (RNA-LPX) based on well-known lipid carriers by optimally adjusting net charge, without the need for functionalization of particles with molecular ligands. The LPX protects RNA from extracellular ribonucleases and mediates its efficient uptake and expression of the encoded antigen by DC populations and macrophages in various lymphoid compartments. RNA-LPX triggers interferon-α (IFNα) release by plasmacytoid DCs and macrophages. Consequently, DC maturation in situ and inflammatory immune mechanisms reminiscent of those in the early systemic phase of viral infection are activated. We show that RNA-LPX encoding viral or mutant neo-antigens or endogenous self-antigens induce strong effector and memory T-cell responses, and mediate potent IFNα-dependent rejection of progressive tumours. A phase I dose-escalation trial testing RNA-LPX that encode shared tumour antigens is ongoing. In the first three melanoma patients treated at a low-dose level, IFNα and strong antigen-specific T-cell responses were induced, supporting the identified mode of action and potency. As any polypeptide-based antigen can be encoded as RNA, RNA-LPX represent a universally applicable vaccine class for systemic DC targeting and synchronized induction of both highly potent adaptive as well as type-I-IFN-mediated innate immune mechanisms for cancer immunotherapy.
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