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小鼠B细胞FcγRII的个体发生与分布

Ontogeny and distribution of the murine B cell Fc gamma RII.

作者信息

Foy T M, Lynch R G, Waldschmidt T J

机构信息

Department of Pathology, University of Iowa College of Medicine, Iowa City 52242.

出版信息

J Immunol. 1992 Sep 1;149(5):1516-23.

PMID:1387140
Abstract

The distribution and expression of the IgG FcRII (Fc gamma RII) on normal murine B cells was examined. Using multicolor flow cytometry, spleens from neonatal mice of increasing age and adult bone marrow were analyzed for expression of the Fc gamma RII. In addition, B cells from peripheral lymphoid organs, as well as panel of B cell tumors, were tested. The results demonstrate that the Fc gamma RII is expressed on all pre-B cells and immature B cells in the neonatal spleen and adult bone marrow, on all mature B cells in peripheral lymphoid organs, and on switched B cells in Peyer's patches. Furthermore, the Fc gamma RII was found to be present on B cell tumors representative of all stages of B cell maturation and differentiation. Taken together, the results indicate that Fc gamma RII is expressed during the entire lifetime of the B cell. In addition, examination of spleen cells from neonatal mice revealed a large number of pre-B cells, phenotypically defined as B220+, IgM-. These pre-B cells were present at birth, peaked in number between 2 and 3 wk of age, and became a minor population by day 30. Further phenotypic analysis of these cells demonstrated the expression of the BLA-1 and BP-1 Ag, and the lack of T cell and NK cell markers, thus confirming their assignment to the B cell lineage. Finally, the Fc gamma RII present on these pre-B cells was shown to be functional, by virtue of its ability to bind aggregated IgG.

摘要

对正常小鼠B细胞上IgG FcRII(FcγRII)的分布和表达进行了检测。使用多色流式细胞术,分析了不同日龄新生小鼠的脾脏以及成年骨髓中FcγRII的表达情况。此外,还检测了外周淋巴器官中的B细胞以及一组B细胞肿瘤。结果表明,FcγRII在新生脾脏和成年骨髓中的所有前B细胞和未成熟B细胞、外周淋巴器官中的所有成熟B细胞以及派伊尔结中的转换B细胞上均有表达。此外,在代表B细胞成熟和分化各个阶段的B细胞肿瘤中也发现了FcγRII。综合来看,结果表明FcγRII在B细胞的整个生命周期中均有表达。此外,对新生小鼠脾脏细胞的检测发现了大量前B细胞,其表型定义为B220 +、IgM -。这些前B细胞在出生时就存在,数量在2至3周龄时达到峰值,到30天时成为少数群体。对这些细胞的进一步表型分析表明它们表达BLA - 1和BP - 1抗原,且缺乏T细胞和NK细胞标志物,从而证实它们属于B细胞谱系。最后,这些前B细胞上的FcγRII因其能够结合聚集的IgG而被证明具有功能。

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