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人类骨髓中B淋巴细胞亚群的表型研究。

A phenotypic study of B lymphocyte subpopulations in human bone marrow.

作者信息

Chapple M R, MacLennan I C, Johnson G D

机构信息

Department of Immunology, Medical School, Birmingham, UK.

出版信息

Clin Exp Immunol. 1990 Jul;81(1):166-72. doi: 10.1111/j.1365-2249.1990.tb05309.x.

Abstract

The regulatory mechanisms that monitor the size of the peripheral B cell pool and determine cell death or survival are poorly understood. In rodents B lymphopoiesis is maintained at a high rate throughout adult life, and under resting conditions there is little recruitment into the long-lived peripheral pool; it therefore follows that most newly formed B lymphocytes have a very short lifespan. The maturation stages of B lymphopoiesis in humans and in experimental mammals appear to be similar. We have determined the phenotype of sIgM- and sIgD-expressing cells from normal adult human bone-marrow and peripheral blood by dual immunofluorescence with an extensive panel of monoclonal antibodies representative of major B cell clusters, in order to identify antigenic differences that may play a regulatory role. Antibodies of the CD21, CD22 and CD9 clusters, the unclustered restricted B antibody 7-F-7 and anti-IgD were reactive with different proportions of sIgM+ cells in blood and bone marrow; 29.5% (range 5-60%) of sIgM+ cells in marrow were sIgD- and most of these cells were also CD21- and CD22-, thus defining a unique marrow population. However, newly formed and mature re-circulating cells comprising the sIgM+sIgD+ population could not be distinguished by the panel of antibodies.

摘要

目前对监测外周B细胞库大小并决定细胞死亡或存活的调节机制了解甚少。在啮齿动物中,B淋巴细胞生成在成年期始终保持较高速率,在静息条件下,很少有细胞招募进入长寿的外周库;因此,大多数新形成的B淋巴细胞寿命非常短。人类和实验性哺乳动物中B淋巴细胞生成的成熟阶段似乎相似。我们通过使用代表主要B细胞簇的大量单克隆抗体进行双重免疫荧光,确定了正常成年人类骨髓和外周血中表达sIgM和sIgD的细胞的表型,以识别可能起调节作用的抗原差异。CD21、CD22和CD9簇的抗体、未聚类的限制性B抗体7-F-7和抗IgD与血液和骨髓中不同比例的sIgM+细胞发生反应;骨髓中29.5%(范围5-60%)的sIgM+细胞为sIgD-,且这些细胞中的大多数也为CD21-和CD22-,从而定义了一个独特的骨髓群体。然而,由sIgM+sIgD+群体组成的新形成的和成熟的再循环细胞无法通过该组抗体进行区分。

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