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Distribution of lymphocytes identified by surface markers in murine strains with systemic lupus erythematosus-like syndromes

机译:通过表面标志物鉴定的淋巴细胞在系统性红斑狼疮样综合征小鼠品系中的分布

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摘要

The frequencies and absolute numbers of B and T cells in the lymphoid organs of five murine strains (NZB, (NZB X NZW)F1, BXSB, MRL/l, and MRL) with SLE-like syndromes were examined. We assessed the frequencies of cells bearing surface Ig, C3d and IgG Fc receptors, and theta-antigen. The sequential expression of Ig isotopes on developing B cells and the Ig isotypes expressed on adult B cells were ascertained. In addition, the Ly subsets and the expression of Ia antigens coded for by the I-J subregion of the mouse H-2 complex were examined. Compared to normal, older mice, New Zealand mice had low frequencies and absolute numbers of B cells, BXSB mice had a moderate B-cell proliferation, and MRL/l mice had normal absolute numbers of B cells but a reduced frequency concomitant with a massive T-cell proliferation. Old New Zealand mice and BXSB mice had reduced frequencies and absolute numbers of T cells compared to old controls. The developmental Ig-isotype diversity during the 1st wk of age was similar in normal mice and those with autoimmune manifestations. Mature B cells were present in lymphoid organs of New Zealand mice and BXSB mice as evidenced by the high frequency of C3d receptor-bearing cells and Ig-isotype expression (high ratio of IgM- to IgD-bearing cells) in adult spleen cells. Numbers of IgG Fc receptor-bearing cells were reduced in autoimmune mice with advanced age and disease. The proliferating T cells in MRL/l mice were found to be theta-antigen positive but Ly null. These theta+-, Ly null cells may have arisen from Ly123+ T cells. MRL/l and BXSB mice seemed normal in their content of T cells bearing Ia antigens coded for by the I-J subregion of H-2. Overall, mice with autoimmune manifestations appear to express perturbations in T and B cells with development of disease, and their patterns of change vary from one strain to another.
机译:检查了五种SLE样综合征的鼠类菌株(NZB,(NZB X NZW)F1,BXSB,MRL / l和MRL / n)的淋巴器官中B和T细胞的频率和绝对数量。我们评估了带有表面Ig,C3d和IgG Fc受体以及theta抗原的细胞的频率。确定了正在发育的B细胞上Ig同位素的顺序表达以及在成年B细胞上表达的Ig同种型。此外,检查了小鼠H-2复合物的I-J亚区的Ly亚群和Ia抗原的表达。与正常的,较年长的小鼠相比,新西兰小鼠的B细胞频率和绝对数量低,BXSB小鼠的B细胞增殖程度适中,而MRL / l小鼠的B细胞的绝对数量正常,但频率降低,而体积较大。 T细胞增殖。与旧对照组相比,旧的新西兰小鼠和BXSB小鼠的T细胞频率和绝对数量减少。正常小鼠和具有自身免疫表现的小鼠在第一周的发育中Ig同种型多样性相似。成熟的B细胞存在于新西兰小鼠和BXSB小鼠的淋巴器官中,这由成年脾细胞中C3d受体细胞的高频率和Ig同型表达(IgM与IgD的高比例)所证明。在具有高龄和疾病的自身免疫小鼠中,携带IgG Fc受体的细胞数量减少。发现在MRL / 1小鼠中增殖的T细胞是θ-抗原阳性但Ly无效。这些theta +-,Ly无效细胞可能来自Ly123 + T细胞。 MRL / 1和BXSB小鼠的T细胞中含有由H-2的I-J子区域编码的Ia抗原的含量似乎正常。总体而言,具有自身免疫表现的小鼠似乎随着疾病的发展而在T细胞和B细胞中表达扰动,并且它们的变化模式在一个品系之间变化。

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