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通过与肿瘤相关抗原进行蛋白质转移工程改造的流感病毒样颗粒可诱导保护性抗肿瘤免疫。

Influenza virus-like particles engineered by protein transfer with tumor-associated antigens induces protective antitumor immunity.

作者信息

Patel Jaina M, Vartabedian Vincent F, Kim Min-Chul, He Sara, Kang Sang-Moo, Selvaraj Periasamy

机构信息

Department of Pathology and Laboratory Medicine, Emory University School of Medicine, Atlanta, 30322, Georgia.

出版信息

Biotechnol Bioeng. 2015 Jun;112(6):1102-10. doi: 10.1002/bit.25537. Epub 2015 Apr 17.

DOI:10.1002/bit.25537
PMID:25689082
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4621003/
Abstract

Delivery of antigen in particulate form using either synthetic or natural particles induces stronger immunity than soluble forms of the antigen. Among naturally occurring particles, virus-like particles (VLPs) have been genetically engineered to express tumor-associated antigens (TAAs) and have shown to induce strong TAA-specific immune responses due to their nano-particulate size and ability to bind and activate antigen-presenting cells. In this report, we demonstrate that influenza VLPs can be modified by a protein transfer technology to express TAAs for induction of effective antitumor immune responses. We converted the breast cancer HER-2 antigen to a glycosylphosphatidylinositol (GPI)-anchored form and incorporated GPI-HER-2 onto VLPs by a rapid protein transfer process. Expression levels on VLPs depended on the GPI-HER-2 concentration added during protein transfer. Vaccination of mice with protein transferred GPI-HER-2-VLPs induced a strong Th1 and Th2-type anti-HER-2 antibody response and protected mice against a HER-2-expressing tumor challenge. The Soluble form of GPI-HER-2 induced only a weak Th2 response under similar conditions. These results suggest that influenza VLPs can be enriched with TAAs by protein transfer to develop effective VLP-based subunit vaccines against cancer without chemical or genetic modifications and thus preserve the immune stimulating properties of VLPs for easier production of antigen-specific therapeutic cancer vaccines.

摘要

使用合成颗粒或天然颗粒以颗粒形式递送抗原比可溶性抗原诱导更强的免疫反应。在天然存在的颗粒中,病毒样颗粒(VLP)已通过基因工程改造以表达肿瘤相关抗原(TAA),并且由于其纳米颗粒大小以及结合和激活抗原呈递细胞的能力,已显示出可诱导强烈的TAA特异性免疫反应。在本报告中,我们证明流感病毒样颗粒可以通过蛋白质转移技术进行修饰,以表达TAA来诱导有效的抗肿瘤免疫反应。我们将乳腺癌HER-2抗原转化为糖基磷脂酰肌醇(GPI)锚定形式,并通过快速蛋白质转移过程将GPI-HER-2整合到病毒样颗粒上。病毒样颗粒上的表达水平取决于蛋白质转移过程中添加的GPI-HER-2浓度。用蛋白质转移的GPI-HER-2-病毒样颗粒对小鼠进行疫苗接种可诱导强烈的Th1和Th2型抗HER-2抗体反应,并保护小鼠免受表达HER-2的肿瘤攻击。在类似条件下,GPI-HER-2的可溶性形式仅诱导微弱的Th2反应。这些结果表明,流感病毒样颗粒可以通过蛋白质转移富集TAA,从而开发出有效的基于病毒样颗粒的癌症亚单位疫苗,而无需化学或基因修饰,从而保留病毒样颗粒的免疫刺激特性,以便更轻松地生产抗原特异性治疗性癌症疫苗。

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