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抗肿瘤IgE佐剂活性:FcεRI的关键作用。

Antitumor IgE adjuvanticity: key role of Fc epsilon RI.

作者信息

Nigro Elisa A, Brini Anna T, Soprana Elisa, Ambrosi Alessandro, Dombrowicz David, Siccardi Antonio G, Vangelista Luca

机构信息

Department of Biology and Genetics, University of Milan, Milan, Italy.

出版信息

J Immunol. 2009 Oct 1;183(7):4530-6. doi: 10.4049/jimmunol.0900842. Epub 2009 Sep 11.

DOI:10.4049/jimmunol.0900842
PMID:19748979
Abstract

Working with C57BL/6 mouse tumor models, we had previously demonstrated that vaccination with IgE-coated tumor cells can protect against tumor challenge, an observation that supports the involvement of IgE in antitumor immunity. The adjuvant effect of IgE was shown to result from eosinophil-dependent priming of the T cell-mediated adaptive immune response. The protective effect is likely to be mediated by the interaction of tumor cell-bound IgE with receptors, which then trigger the release of mediators, recruitment of effector cells, cell killing and tumor Ag cross-priming. It was therefore of utmost importance to demonstrate the strict dependence of the protective effect on IgE receptor activation. First, the protective effect of IgE was confirmed in a BALB/c tumor model, in which IgE-loaded modified VV Ankara-infected tumor cells proved to be an effective cellular vaccine. However, the protective effect was lost in Fc(epsilon)RIalpha(-/-) (but not in CD23(-/-)) knockout mice, showing the IgE-Fc(epsilo)nRI interaction to be essential. Moreover, human IgE (not effective in BALB/c mice) had a protective effect in the humanized knockin mouse (Fc(epsilon)RIalpha(-/-) hFc(epsilon)RIalpha(+)). This finding suggests that the adjuvant effect of IgE could be exploited for human therapeutics.

摘要

在C57BL/6小鼠肿瘤模型的研究中,我们之前已经证明,用IgE包被的肿瘤细胞进行疫苗接种可以抵御肿瘤攻击,这一观察结果支持了IgE参与抗肿瘤免疫。IgE的佐剂效应被证明是由嗜酸性粒细胞依赖性启动T细胞介导的适应性免疫反应所致。这种保护作用可能是由肿瘤细胞结合的IgE与受体的相互作用介导的,进而触发介质的释放、效应细胞的募集、细胞杀伤和肿瘤抗原交叉启动。因此,证明保护作用对IgE受体激活的严格依赖性至关重要。首先,在BALB/c肿瘤模型中证实了IgE的保护作用,在该模型中,负载IgE的改良安卡拉痘苗病毒感染的肿瘤细胞被证明是一种有效的细胞疫苗。然而,在Fc(ε)RIα(-/-)(而非CD23(-/-))基因敲除小鼠中,保护作用消失了,这表明IgE-Fc(ε)RI相互作用至关重要。此外,人IgE(在BALB/c小鼠中无效)在人源化敲入小鼠(Fc(ε)RIα(-/-) hFc(ε)RIα(+))中具有保护作用。这一发现表明,IgE的佐剂效应可用于人类治疗。

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