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CD20(全B细胞)抗原在人T淋巴细胞亚群上低水平表达。

CD20 (pan-B cell) antigen is expressed at a low level on a subpopulation of human T lymphocytes.

作者信息

Hultin L E, Hausner M A, Hultin P M, Giorgi J V

机构信息

Department of Medicine, UCLA School of Medicine, 90024.

出版信息

Cytometry. 1993;14(2):196-204. doi: 10.1002/cyto.990140212.

DOI:10.1002/cyto.990140212
PMID:7679964
Abstract

Despite the previous description of the leukocyte differentiation antigen CD20 as B cell restricted, the findings reported here indicate that a small subset of human T cells expresses low levels of CD20 or a cross-reacting antigen. Three different CD20 monoclonal antibodies (mAb), Leu16, B1, and 1F5, reacted with the T cell subset. B cells that expressed CD20 were CD20bright and constituted an average of 9.2 +/- 3.3% of adult PBL. Meanwhile, T cells that expressed CD20 were CD20dim and represented 2.4 +/- 1.5% of the PBL. This population may have been overlooked in previous studies due to the low level of CD20 expression per T cell and the small size of the subset in most individuals. Blocking studies indicated that CD20 mAb binding to CD3+ cells was due to the antigen-reactive regions of the CD20 antibodies and was not a result of Fc receptor binding, or non-specific fluorochrome or protein binding. The T cell nature of the CD20dim CD3+ cells was confirmed by the rapid rise in the intracellular calcium concentration ([Ca2+]i) of CD20dim cells observed following treatment with CD3 mAb but not following treatment with anti-human immunoglobulin (Ig). Extensive three-color immunophenotypic analyses indicated that CD20dim T cells were phenotypically heterogeneous and displayed a leukocyte differentiation profile that was slightly different than that of CD20- T cells. Thus, the CD20dim T cells were more likely than CD20- T cells to be gamma/delta T cell antigen receptor positive (14% vs. 3.4%), CD8+ (57% vs. 33%), and CD45RO+ (82% vs. 51%); fewer were CD38+ (5% vs. 24%) or CD4+ (35% vs. 61%).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

尽管先前将白细胞分化抗原CD20描述为B细胞限制性抗原,但此处报道的研究结果表明,一小部分人类T细胞表达低水平的CD20或一种交叉反应性抗原。三种不同的CD20单克隆抗体(mAb),即Leu16、B1和1F5,可与该T细胞亚群发生反应。表达CD20的B细胞CD20呈高表达状态,在成人外周血淋巴细胞(PBL)中平均占9.2±3.3%。同时,表达CD20的T细胞CD20呈低表达状态,占PBL的2.4±1.5%。由于每个T细胞的CD20表达水平较低且在大多数个体中该亚群规模较小,这一群体在先前的研究中可能被忽视了。阻断研究表明,CD20 mAb与CD3 + 细胞的结合是由于CD20抗体的抗原反应区域,而非Fc受体结合、非特异性荧光染料或蛋白质结合的结果。在用CD3 mAb处理后观察到CD20低表达细胞的细胞内钙浓度([Ca2 + ]i)迅速升高,而用抗人免疫球蛋白(Ig)处理后未出现此现象,从而证实了CD20低表达CD3 + 细胞的T细胞性质。广泛的三色免疫表型分析表明,CD20低表达T细胞在表型上具有异质性,其白细胞分化谱与CD20阴性T细胞略有不同。因此,CD20低表达T细胞比CD20阴性T细胞更有可能为γ/δ T细胞抗原受体阳性(14%对3.4%)、CD8 +(57%对33%)和CD45RO +(82%对51%);CD38 +(5%对24%)或CD4 +(35%对61%)的细胞较少。(摘要截于250字)

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