小鼠B细胞组织相关表型异质性的研究。

P Balogh, A Kumánovics, I Juhász
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引用次数: 1

摘要

B细胞的发育伴随着它们特异性进入外周淋巴组织的能力。最近,我们描述了一种新的大鼠单克隆抗体(IBL-2;IgG2b/kappa)与细胞表面26/29-kD异二聚体结构反应。该单抗已被发现识别不同组织来源的小鼠外周血B细胞。大多数脾脏B细胞以及骨髓中的成熟B细胞都可以用这种单抗染色,而从LN或Peyer's斑块中分离的B淋巴细胞仅显示微不足道的反应性。我们通过多参数流式细胞术分析骨髓中b细胞前体表面IBL-2抗原表达与l选择的关系,进一步扩展了这些观察结果。在B220阳性区室中,可观察到不同ibl -2反应亚群之间l -选择素表达的显著差异。此外,我们研究了在将正常未选择的脾淋巴细胞过继转移到SCID受体(Spl-SCID)后,是否可以发现与正常小鼠相似的组织相关表型异质性的证据。研究发现大部分脾B细胞保留了其IBL-2反应性,而LN B细胞在spll - scid中失去了IBL-2抗原。这些数据表明,SCID小鼠的表型差异可能是B淋巴细胞从脾脏向淋巴结迁移的结果,而IBL-2抗原表达的改变与这一过程有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Studies on the tissue-related phenotypic heterogeneity of murine B cells.

The development of B cells is accompanied by their ability to specifically enter the peripheral lymphoid tissues. Recently, we described a novel rat monoclonal antibody (IBL-2; IgG2b/kappa) reacting with a 26/29-kD heterodimeric structure of the cell surface. This mAb has been found to recognize differentially the peripheral B cells of mice depending on their tissue origin. The majority of splenic B cells as well as the mature B cells in the bone marrow were stained with this mAb, whereas the B lymphocytes isolated from LN or Peyer's patches displayed only negligible reactivity. We extended these observations by analyzing the relationship between the expression of IBL-2 antigen and L-selection on the surface of B-cell precursors in the bone marrow by multiparameter flow cytometry. Within the B220 positive compartment, a significant difference of L-selectin expression could be observed between the various IBL-2-reactive subsets. Furthermore, we investigated whether evidences for the establishment of tissue-associated phenotypic heterogeneity similar to that found in normal mice could be found upon the adoptive transfer of normal unselected splenic lymphocytes into SCID recipients (Spl-SCID). It has been found that a large part of the splenic B cells preserved their IBL-2 reactivity, whereas the LN B cells had lost the IBL-2 antigen in Spl-SCID. These data indicate that the phenotypic difference within the SCID mice may be the result of the migration of B lymphocytes from the spleen toward the lymph nodes, and the altered expression of the IBL-2 antigen correlates with this process.

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