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基于微小膜 IgE 的抗肿瘤细胞疫苗。

An antitumor cellular vaccine based on a mini-membrane IgE.

机构信息

Department of Biology and Genetics, Università degli Studi di Milano, Milan, Italy.

出版信息

J Immunol. 2012 Jan 1;188(1):103-10. doi: 10.4049/jimmunol.1101842. Epub 2011 Nov 28.

DOI:10.4049/jimmunol.1101842
PMID:22124126
Abstract

The IgE-mediated immune system activation can be redirected to combat tumors. Mouse and human IgE have been shown to provide a potent adjuvant effect in antitumor vaccination, with a crucial role played by FcεRI. This effect results from T cell-mediated adaptive immune response. Modified vaccinia virus Ankara (MVA) has been used to infect IgE-loaded tumor cells. These results led to a shift toward a highly safe protocol employing membrane IgE (mIgE), thus eliminating any possible anaphylactogenicity caused by circulating IgE. Evidence that human mIgE and a truncated version lacking IgE Fabs (tmIgE) bind and activate FcεRI has been fundamental and forms the core of this report. Human tmIgE has been engineered into a recombinant MVA (rMVA-tmIgE), and the expression of tmIgE and its transport to the surface of rMVA-tmIgE-infected cells has been detected by Western blot and cytofluorimetry, respectively. FcεRI activation by tmIgE has been confirmed by the release of β-hexosaminidase in a cell-to-cell contact assay using human FcεRI-transfected RBL-SX38 cells. The rMVA-tmIgE antitumor vaccination strategy has been investigated in FcεRIα(-/-) human FcεRIα(+) mice, with results indicating a level of protection comparable to that obtained using soluble human IgE tumor cell loading. The rMVA-tmIgE vector represents a device that suits safe IgE-based antitumor vaccines, harboring the possibility to couple tmIgE with other gene insertions that might enhance the antitumor effect, thus bringing the field closer to the clinics.

摘要

IgE 介导的免疫系统激活可以被重新定向用于抗肿瘤。已经证明,小鼠和人 IgE 在抗肿瘤疫苗接种中提供了强大的佐剂效应,FcεRI 发挥了关键作用。这种效应来自 T 细胞介导的适应性免疫反应。已使用改良安卡拉牛痘病毒(MVA)感染 IgE 负载的肿瘤细胞。这些结果导致转向高度安全的方案,采用膜 IgE(mIgE),从而消除了由循环 IgE 引起的任何可能的过敏原性。证据表明,人 mIgE 和缺乏 IgE Fabs(tmIgE)的截断版本结合并激活 FcεRI,这是基础性的,也是本报告的核心。人 tmIgE 已被工程化为重组 MVA(rMVA-tmIgE),并通过 Western blot 和细胞荧光术分别检测 tmIgE 的表达及其转运到 rMVA-tmIgE 感染细胞的表面。通过使用转染人 FcεRI 的 RBL-SX38 细胞进行细胞间接触测定,证实了 tmIgE 通过 FcεRI 激活导致β-己糖胺酶的释放。已经在 FcεRIα(-/-)人 FcεRIα(+)小鼠中研究了 rMVA-tmIgE 抗肿瘤疫苗接种策略,结果表明该策略的保护水平与使用可溶性人 IgE 肿瘤细胞负载获得的保护水平相当。rMVA-tmIgE 载体是一种适合安全 IgE 抗肿瘤疫苗的装置,具有将 tmIgE 与其他可能增强抗肿瘤效果的基因插入物结合的可能性,从而使该领域更接近临床。

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