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派尔集合淋巴结生发中心细胞的表面表型:对生发中心在B细胞分化中作用的启示

Surface phenotype of Peyer's patch germinal center cells: implications for the role of germinal centers in B cell differentiation.

作者信息

Butcher E C, Rouse R V, Coffman R L, Nottenburg C N, Hardy R R, Weissman I L

出版信息

J Immunol. 1982 Dec;129(6):2698-707.

PMID:6982940
Abstract

The surface phenotype of Peyer's patch germinal center lymphoid cells in the mouse is described. It is confirmed that most germinal center lymphocytes bind high levels of peanut agglutination (PNA), a lectin with specificity for terminal galactosyl residues. It is shown that germinal center lymphocytes can be identified in cell suspensions as a discrete PNAhi population distinct from other B cells, plasma cells, and most T cells, which bind only low levels of PNA. Using fluorescence-labeled PNA as a marker in dual fluorescence studies, we found that the majority of Peyer's patch germinal center cells are B lymphocytes: PNAhi Peyer's patch cells express B220, the B lineage-specific form of the T200 family of molecules, as well as low levels of surface Ig. They do not express the T cell-lineage antigens Thy-1, Lyt-1, or Lyt-2 (only 1 to 3% positive). They bear lower levels of H2-K than PNAlo B cells, but two to three times the level of surface I-A-encoded determinants. A discrete but variable subpopulation of PNAhi Peyer's patch cells bear ThB in AKR/c mice, but BALB/c PNAhi lymphocytes are ThB-. About 10 to 30% bear surface IgM or IgG, but in contrast to essentially all PNAlo B lymphocytes in this site, they express no detectable surface IgD. The majority of Peyer's patch germinal center cells bear surface IgA, and this IgA is allelically excluded in F1 mice, indicating it is synthesized by the germinal center cells themselves. In fact, germinal centers contain most of the IgA-bearing cells in Peyer's patches (70 to 85%). These findings lend considerable support to the concept that germinal centers in Peyer's patches are the site of generation of precursors of the IgA-secreting plasma cells that characterize mucosal immune responses, and also suggest that germinal centers may play an important role in the process of heavy chain class switching.

摘要

本文描述了小鼠派尔集合淋巴结生发中心淋巴细胞的表面表型。已证实,大多数生发中心淋巴细胞能与高水平的花生凝集素(PNA)结合,PNA是一种对末端半乳糖基残基具有特异性的凝集素。研究表明,在细胞悬液中,生发中心淋巴细胞可作为一个离散的PNA高表达群体被识别出来,该群体不同于其他仅结合低水平PNA的B细胞、浆细胞和大多数T细胞。在双荧光研究中,使用荧光标记的PNA作为标志物,我们发现派尔集合淋巴结生发中心的大多数细胞是B淋巴细胞:PNA高表达的派尔集合淋巴结细胞表达B220,即T200分子家族的B谱系特异性形式,以及低水平的表面免疫球蛋白。它们不表达T细胞谱系抗原Thy-1、Lyt-1或Lyt-2(只有1%至3%呈阳性)。与PNA低表达的B细胞相比,它们的H2-K水平较低,但表面I-A编码决定簇的水平是其两到三倍。在AKR/c小鼠中,PNA高表达的派尔集合淋巴结细胞中有一个离散但可变的亚群表达ThB,但BALB/c小鼠的PNA高表达淋巴细胞不表达ThB。约10%至30%的细胞带有表面免疫球蛋白M或免疫球蛋白G,但与该部位基本上所有的PNA低表达B淋巴细胞不同,它们不表达可检测到的表面免疫球蛋白D。派尔集合淋巴结生发中心的大多数细胞带有表面免疫球蛋白A,并且在F1小鼠中这种免疫球蛋白A存在等位基因排斥现象,这表明它是由生发中心细胞自身合成的。事实上,生发中心包含派尔集合淋巴结中大多数携带免疫球蛋白A的细胞(70%至85%)。这些发现为以下概念提供了有力支持,即派尔集合淋巴结中的生发中心是分泌免疫球蛋白A的浆细胞前体产生的部位,而这些浆细胞是黏膜免疫反应的特征,同时也表明生发中心可能在重链类别转换过程中发挥重要作用。

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