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新生儿 FcR 过表达增强转基因小鼠的体液免疫反应。

Neonatal FcR overexpression boosts humoral immune response in transgenic mice.

机构信息

Department of Immunology, Institute of Biology, Faculty of Science, Eötvös Loránd University, Budapest, Hungary.

出版信息

J Immunol. 2011 Jan 15;186(2):959-68. doi: 10.4049/jimmunol.1000353. Epub 2010 Dec 8.

DOI:10.4049/jimmunol.1000353
PMID:21148035
Abstract

The neonatal FcR (FcRn) regulates IgG and albumin homeostasis, mediates maternal IgG transport, takes active part in phagocytosis, and delivers Ag for presentation. We have previously shown that overexpression of FcRn in transgenic (Tg) mice extends the half-life of mouse IgG by reducing its clearance. In this paper, we demonstrate that immunization of these mice with OVA and trinitrophenyl-conjugated human IgG results in a 3- to 10-fold increase of Ag-specific IgM and IgG in serum. The IgM increase was unexpected because FcRn does not bind IgM. Our results showed that the affinity of the Ag-specific IgG was at least as good in Tg mice as in the wild-type (wt) controls, implying appropriate affinity maturation in both groups. Influenza vaccination produced a 2-fold increase in the amount of virus-specific Ab in Tg animals, which proved twice as efficient in a hemagglutination inhibition assay as was the case in wt controls. After immunization, Tg mice displayed significantly larger spleens containing a higher number of Ag-specific B cells and plasma cells, as well as many more granulocytes and dendritic cells, analyzed by ELISPOT and flow cytometric studies. The neutrophils from these Tg mice expressed the Tg FcRn and phagocytosed IgG immune complexes more efficiently than did those from wt mice. These results show that FcRn overexpression not only extends the IgG half-life but also enhances the expansion of Ag-specific B cells and plasma cells. Although both effects increase the level of Ag-specific IgG, the increase in immune response and IgG production seems to be more prominent compared with the reduced IgG clearance.

摘要

新生儿 Fc 受体 (FcRn) 调节 IgG 和白蛋白的动态平衡,介导母体 IgG 的转运,积极参与吞噬作用,并递送抗原进行呈递。我们之前已经表明,在转基因 (Tg) 小鼠中过表达 FcRn 通过减少其清除来延长小鼠 IgG 的半衰期。在本文中,我们证明用 OVA 和三硝基苯缀合的人 IgG 免疫这些小鼠会导致血清中抗原特异性 IgM 和 IgG 增加 3 到 10 倍。IgM 的增加出乎意料,因为 FcRn 不结合 IgM。我们的结果表明,在 Tg 小鼠中,抗原特异性 IgG 的亲和力至少与野生型 (wt) 对照组一样好,这意味着两组都有适当的亲和力成熟。流感疫苗接种在 Tg 动物中产生了 2 倍的病毒特异性 Ab 量,在血凝抑制测定中比 wt 对照组的效果高出一倍。免疫后,Tg 小鼠的脾脏明显增大,其中含有更多数量的抗原特异性 B 细胞和浆细胞,以及更多的粒细胞和树突状细胞,通过 ELISPOT 和流式细胞术研究进行分析。来自这些 Tg 小鼠的中性粒细胞比来自 wt 小鼠的中性粒细胞更有效地表达 Tg FcRn 并吞噬 IgG 免疫复合物。这些结果表明,FcRn 过表达不仅延长了 IgG 的半衰期,而且增强了抗原特异性 B 细胞和浆细胞的扩增。尽管这两种效应都增加了抗原特异性 IgG 的水平,但与减少 IgG 清除相比,免疫反应和 IgG 产生的增加似乎更为突出。

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