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由Lyt-1、2、3和Thy-1抗原表达所定义的T细胞亚群。使用单克隆抗体进行的双参数免疫荧光和细胞毒性分析改变了当前的观点。

T cell subsets defined by expression of Lyt-1,2,3 and Thy-1 antigens. Two-parameter immunofluorescence and cytotoxicity analysis with monoclonal antibodies modifies current views.

作者信息

Ledbetter J A, Rouse R V, Micklem H S, Herzenberg L A

出版信息

J Exp Med. 1980 Aug 1;152(2):280-95. doi: 10.1084/jem.152.2.280.

Abstract

Using monoclonal antibodies and multiparameter fluorescence analyses, we show that the expression of Lyt-1, Lyt-2, and Lyt-3 on T cell subpopulations is more complex than was originally recognized by the cytotoxic depletion studies with conventional reagents that defined the Lyt-1+2+3+, Lyt-1+2-3-, and Lyt-1-2+3+ populations. We detect at least some Lyt-1 on all T (Thy-1-bearing) lymphocytes; however, in agreement with previous studies, we find that Lyt-2+3+ cells are more difficult to depelete with anti-Lyt-1 than Lyt-1+2-3- cells. Surprisingly, we found a small subpopulation of cells carrying relatively large amounts of Lyt-1 and no Thy-1 detectable by fluorescence-activated cell sorter analysis. We also detect cells with this phenotype histologically in B cell zones (primary follicles) and germinal centers in spleen and lymph nodes. In general, the Lyt-1 only population represents approximately 2% of spleen cells. The relative quantitative expression of Thy-1, Lyt-1, Lyt-2, and Lyt-3 changes systematically during T cell maturation. Among Lyt-1+2+3+ cells in the thymus, Thy-1 and Lyt-2 are high, whereas Lyt-1 is low. Among splenic T cells, in contrast, Thy-1 is low, Lyt-1 is high, and Lyt-2 and Lyt-3 are a little higher than in thymus. In general, Thy-1 expression is negatively correlated with Lyt-1. Thus, even among splenic and lymph node T cells subpopulations exist that tend to be either high Thy-1 and low Lyt-1 or vice versa. Lyt-2+3+ cells represent approximately 85% of thymocytes but only approximately 35% of splenic or lymph node T cells. The Lyt-2+3+ cells are found predominantly in the low Lyt-1, high Thy-1 subpopulation.

摘要

利用单克隆抗体和多参数荧光分析,我们发现T细胞亚群上Lyt-1、Lyt-2和Lyt-3的表达比最初用传统试剂进行的细胞毒性清除研究所认识的更为复杂,传统试剂定义了Lyt-1+2+3+、Lyt-1+2-3-和Lyt-1-2+3+群体。我们在所有T(表达Thy-1的)淋巴细胞上检测到至少一些Lyt-1;然而,与先前的研究一致,我们发现Lyt-2+3+细胞比Lyt-1+2-3-细胞更难被抗Lyt-1清除。令人惊讶的是,我们发现一小部分细胞携带相对大量的Lyt-1,通过荧光激活细胞分选分析未检测到Thy-1。我们还在脾脏和淋巴结的B细胞区(初级滤泡)和生发中心组织学上检测到具有这种表型的细胞。一般来说,仅表达Lyt-1的细胞群体约占脾细胞的2%。Thy-1、Lyt-1、Lyt-2和Lyt-3的相对定量表达在T细胞成熟过程中系统性地变化。在胸腺中的Lyt-1+2+3+细胞中,Thy-1和Lyt-2高,而Lyt-1低。相比之下,在脾T细胞中,Thy-1低,Lyt-1高,Lyt-2和Lyt-3比胸腺中的略高。一般来说,Thy-1表达与Lyt-1呈负相关。因此,即使在脾和淋巴结T细胞中也存在亚群,它们倾向于要么Thy-1高而Lyt-1低,要么反之。Lyt-2+3+细胞约占胸腺细胞的85%,但仅占脾或淋巴结T细胞的约35%。Lyt-2+3+细胞主要存在于低Lyt-1、高Thy-1亚群中。

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