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Crucial Role of Tumor Necrosis Factor Receptor 1 Expression on Nonhematopoietic Cells for B Cell Localization within the Splenic White Pulp

机译:肿瘤坏死因子受体1表达对非造血细胞在脾白浆内B细胞定位的关键作用。

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摘要

During immune responses the initial activation of B cells takes place in T cell zones of periarteriolar lymphoid sheaths (PALS) of the splenic white pulp. After initial activation, B cells migrate into the primary follicles and, in association with follicular dendritic cells (FDCs), undergo clonal expansion and differentiation giving rise to germinal centers (GCs). Peanut agglutinin binding (PNA+) cells of the GC differentiate further into memory or plasma cells. Here we report that in tumor necrosis factor receptor 1–deficient mice (TNFR1−/−), the location of B cells was altered and that plasma cells were abnormally distributed in the splenic PALS. In contrast to lymphotoxin α–deficient mice (LTα−/−), bone marrow or fetal liver transplantation did not correct the abnormal organization of the spleen, location of B cells, the lack of an FDC network, nor the antibody response in TNFR1−/− mice. These results argue for a crucial role of TNFR1 expression on nonhematopoietic cells for the maintenance of the splenic architecture and proper B cell location. In addition, the lack in development of an FDC network after adoptive transfer suggests that either FDCs are not of bone marrow origin or that they depend on signals from nonhematopoietic cells for maturation.
机译:在免疫反应过程中,B细胞的初始激活发生在脾脏白髓的小动脉周围淋巴鞘(PALS)的T细胞区域。初始激活后,B细胞迁移到初级卵泡中,并与卵泡树突状细胞(FDC)结合,经历克隆扩增和分化,从而形成生发中心(GC)。 GC的花生凝集素结合(PNA +)细胞进一步分化为记忆细胞或浆细胞。在这里,我们报道在肿瘤坏死因子受体1缺陷型小鼠(TNFR1-/-)中,B细胞的位置发生了改变,浆细胞在脾PALS中异常分布。与缺乏淋巴毒素α的小鼠(LTα-/-)相比,骨髓或胎儿肝移植不能纠正脾脏的异常组织,B细胞的位置,缺乏FDC网络,也不能纠正TNFR1-中的抗体反应/-小鼠。这些结果证明了TNFR1在非造血细胞上的表达对于维持脾脏结构和正确的B细胞定位至关重要。另外,过继转移后缺乏FDC网络的发展表明FDC不是源自骨髓,或者它们依赖于非造血细胞的信号来成熟。

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