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B-lymphocyte heterogeneity: ontogenetic development and organ distribution of B-lymphocyte populations defined by their density of surface immunoglobulin

机译:B淋巴细胞异质性:由B淋巴细胞群体的表面免疫球蛋白密度定义的发育发育和器官分布

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摘要

The density of total Ig and of IgM, IgG1, IgG2, and IgA on the surface of adult murine splenic B lymphocytes was measured using the technique of rapid flow microfluorometry. In addition, the density of total surface Ig and of IgM on B lymphocytes derived from adult bone marrow, lymph nodes, and Peyer's patches, and from neonatal spleen was determined. Adult spleen and lymph node B lymphocytes are characterized by the presence of a large population of cells with a low-to- intermediate density of total surface Ig, which is seen as a peak in the fluorescence profiles when these cells are labeled with fluorescein- conjugated (F1) anti-Ig. This peak is not detected when neonatal spleen or adult bone marrow are examined; the development of this peak among spleen cells occurs during the first 4 wk of life. Although the characteristic fluorescence intensity peak is not seen when adult spleen cells are labeled with Fl anti-mu, changes in the density of surface IgM do occur during the first few weeks of life and are detected as a decrease in the frequency of cells which have relatively large amounts of surface IgM. The differences seen in the fluorescence patterns of adult spleen cells labeled with Fl anti-Ig and Fl anti-mu may be due to the appearance of IgD on the surface of mature splenic B lymphocytes. This is supported by the similarity of the fluorescence profiles of adult bone marrow cells stained with Fl anti-Ig and Fl anti- mu, as the latter population of cells is reported to lack surface IgD.
机译:使用快速流式荧光法测定成年鼠脾脏B淋巴细胞表面上的总Ig以及IgM,IgG1,IgG2和IgA的密度。另外,测定了来自成年骨髓,淋巴结和派伊尔氏淋巴结以及新生脾脏的B淋巴细胞的总表面Ig和IgM的密度。成年脾脏和淋巴结B淋巴细胞的特征是存在大量的细胞,其总表面Ig的密度为中低密度,当这些细胞用荧光素缀合标记时,在荧光分布图中被视为峰值(F1)抗Ig。检查新生儿脾脏或成年骨髓时未检测到该峰。脾细胞中此峰值的发展发生在生命的前4周内。尽管当用Fl抗-mu标记成年脾细胞时看不到特征性的荧光强度峰,但在生命的最初几周内确实发生了表面IgM密度的变化,并被检测为具有相对大量的表面IgM。用F1抗-Ig和F1抗-mu标记的成年脾细胞的荧光模式中的差异可能是由于在成熟的脾脏B淋巴细胞的表面上出现了IgD。这被成年的骨髓细胞用F1抗Ig和F1抗Mu染色的荧光图谱的相似性所支持,因为据报道后者的细胞群缺乏表面IgD。

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