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与EL-4 T细胞共培养的人初始B细胞在产生浆细胞之前模拟生发中心相关的B细胞阶段。Bcl-2蛋白和信使RNA水平的一致变化。

Human naive B cells cultured with EL-4 T cells mimic a germinal center-related B cell stage before generating plasma cells. Concordant changes in Bcl-2 protein and messenger RNA levels.

作者信息

Grimaître M, Werner-Favre C, Kindler V, Zubler R H

机构信息

Department of Medicine, Hôpitaux Universitaires de Genève, Hôpital Cantonal, Geneva, Switzerland.

出版信息

Eur J Immunol. 1997 Jan;27(1):199-205. doi: 10.1002/eji.1830270130.

Abstract

The T cell-dependent B cell response in vivo occurs in organized microenvironments. Alternative routes exist in that early plasma cells are generated in the T zone while others emerge later from the germinal center (GC) reaction. We investigated whether B cell stages resembling those defined in vivo/ex vivo might be induced in an in vitro system in which naive human B cells are activated by EL-4 T cells and cytokines. Adult peripheral blood- or cord blood-derived B cells were found to mimic an early activated stage (CD38(low), IgD+, increased CD5+) followed by a centroblastic GC-related stage (CD38(int), CD77+, CD95(Fas)+, Bcl-2 protein(low)) before differentiating into morphologically typical, CD38(high), Fas- plasma cells of an immature type (Bcl-2(low), VLA-5-). The GC-related cells and the plasma cells exhibited spontaneous apoptosis in medium, the former also undergoing anti-Fas antibody-induced apoptosis in medium as well as during CD40L exposure in the EL-4 cultures. These Bcl-2(low) cells maintained a high viability in contact with EL-4 cells. Thus, some, major B cell stages with typical functional features as described for cells in vivo/ex vivo are sequentially generated in this in vitro system and the kinetics of the changes can be analyzed in a synchronized cell population. With regard to previous apparently conflicting observations on the Bcl-2 mRNA level in GC B cells, we performed competitive reverse-transcription polymerase chain reaction. Concordant changes in Bcl-2 mRNA and protein levels were found, i.e. during Bcl-2 down-regulation in the GC-related B cells in ongoing EL-4 cultures or in medium, and during a more modest up-regulation upon contact with fresh EL-4 cells. Regulation of Bcl-2 protein, therefore, predominantly occurred at the mRNA steady-state level.

摘要

体内T细胞依赖性B细胞反应发生在有组织的微环境中。存在其他途径,即早期浆细胞在T区产生,而其他浆细胞则在生发中心(GC)反应后期出现。我们研究了在体外系统中是否可以诱导出类似于体内/体外定义的B细胞阶段,在该系统中,幼稚人B细胞被EL-4 T细胞和细胞因子激活。发现成人外周血或脐带血来源的B细胞先模拟早期激活阶段(CD38低、IgD +、CD5增加),随后是中心母细胞GC相关阶段(CD38中、CD77 +、CD95(Fas)+、Bcl-2蛋白低),然后分化为形态典型的、CD38高、Fas - 的未成熟型浆细胞(Bcl-2低、VLA-5 -)。GC相关细胞和浆细胞在培养基中表现出自发性凋亡,前者在培养基中以及在EL-4培养物中暴露于CD40L期间也会经历抗Fas抗体诱导的凋亡。这些Bcl-2低的细胞在与EL-4细胞接触时保持高活力。因此,在这个体外系统中依次产生了一些具有体内/体外细胞所描述的典型功能特征的主要B细胞阶段,并且可以在同步细胞群体中分析变化的动力学。关于先前关于GC B细胞中Bcl-2 mRNA水平的明显相互矛盾的观察结果,我们进行了竞争性逆转录聚合酶链反应。发现Bcl-2 mRNA和蛋白水平存在一致变化,即在正在进行的EL-4培养物或培养基中GC相关B细胞中Bcl-2下调期间,以及在与新鲜EL-4细胞接触时更适度的上调期间。因此,Bcl-2蛋白的调节主要发生在mRNA稳态水平。

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