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一种新型的B细胞介导的IgE免疫复合物向脾脏滤泡的转运。

A novel B cell-mediated transport of IgE-immune complexes to the follicle of the spleen.

作者信息

Hjelm Fredrik, Karlsson Mikael C I, Heyman Birgitta

机构信息

Department of Genetics and Pathology, Rudbeck Laboratory, Uppsala University, Uppsala, Sweden.

出版信息

J Immunol. 2008 May 15;180(10):6604-10. doi: 10.4049/jimmunol.180.10.6604.

Abstract

Ag administered i.v. to mice along with specific IgE or IgG2a induces higher Ab- and CD4(+) T cell responses than Ag administered alone. The IgE effect is completely dependent on the low-affinity receptor for IgE, CD23, whereas the IgG2a effect depends on activating FcgammaRs. In vitro studies suggest that IgE/Ag is presented more efficiently than Ag alone to CD4(+) T cells by CD23(+) B cells and that IgG2a/Ag is presented by FcgammaR(+) dendritic cells (DCs). In this study, we investigate in vivo the early events leading to IgE- and IgG2a-mediated enhancement of immune responses. OVA administered i.v. in PBS in combination with specific IgE binds circulating B cells after 5 min and is found in B cell follicles bound to follicular B cells (CD23(high)) after 30 min. This novel B cell-dependent route of entry is specific for IgE because IgG2a-Ag complexes were trapped in the marginal zone. OVA-specific CD4(+) T cells were found at the T-B border in the T cell zones 12 h after immunization both with IgE/OVA or IgG2a/OVA and proliferated vigorously after 3 days. The findings suggest that IgE- and IgG2a-immune complexes are efficient stimulators of early CD4(+) T cell responses and that Ag bound to IgE has a specific route for transportation into follicles.

摘要

静脉注射给小鼠的抗原与特异性IgE或IgG2a一起给药时,比单独给予抗原能诱导更高的抗体和CD4(+) T细胞反应。IgE的作用完全依赖于IgE的低亲和力受体CD23,而IgG2a的作用则依赖于激活FcγRs。体外研究表明,CD23(+) B细胞将IgE/抗原比单独抗原更有效地呈递给CD4(+) T细胞,而IgG2a/抗原则由FcγR(+)树突状细胞(DCs)呈递。在本研究中,我们在体内研究导致IgE和IgG2a介导的免疫反应增强的早期事件。静脉注射于PBS中的OVA与特异性IgE联合给药后5分钟结合循环中的B细胞,30分钟后在与滤泡B细胞(CD23(高))结合的B细胞滤泡中发现。这种新的依赖B细胞的进入途径对IgE具有特异性,因为IgG2a-抗原复合物被困在边缘区。免疫12小时后,在T细胞区的T-B边界发现OVA特异性CD4(+) T细胞,用IgE/OVA或IgG2a/OVA免疫3天后,这些细胞大量增殖。这些发现表明,IgE和IgG2a免疫复合物是早期CD4(+) T细胞反应的有效刺激物,并且与IgE结合的抗原具有进入滤泡的特定途径。

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