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突变的EL-4胸腺瘤细胞通过直接细胞相互作用多克隆激活小鼠和人类B细胞。

Mutant EL-4 thymoma cells polyclonally activate murine and human B cells via direct cell interaction.

作者信息

Zubler R H, Erard F, Lees R K, Van Laer M, Mingari C, Moretta L, MacDonald H R

出版信息

J Immunol. 1985 Jun;134(6):3662-8.

PMID:3886789
Abstract

In this report we show that three mutagenized sublines of (murine) EL-4 thymoma cells can constitutively activate human and/or murine B cells via an MHC-nonrestricted cell-cell interaction. The activation signal is not by itself mitogenic but renders B cells capable of proliferating in response to interleukin 2 (IL 2). In addition, one of the mutant EL-4 sublines can constitutively respond by release of IL 2 in the presence of IL 1-containing macrophage (P388D1) supernatant. The exact relationships between these functional properties of the mutant EL-4 thymoma cells and those associated with activated normal T helper-cells remain to be established. However, the EL-4 cells provide a unique system to study in parallel murine and human B cell responses. In particular, the following observations were made during the present study. First, anti-Ig antibodies (anti-Ig) were required for B cell activation in conjunction with two EL-4 sublines acting only on murine B cells, whereas with a third subline acting on both murine and human B cells, anti-Ig was not required. Anti-Ig by itself did not lead to significant B cell activation in the absence of mutant EL-4 (or normal T) cells. Second, the growth factor-stimulated proliferation of EL-4-activated B cells, following separation of the B cells from the EL-4 cells, lasted only 2 days. These results, thus, indicate that the requirement for a surface Ig-mediated B cell activation signal depends on the quality/intensity of a direct T cell signal and that cell-cell interactions may exert a more stringent control over the growth factor responsiveness of B cells as compared with T cells.

摘要

在本报告中,我们表明(小鼠)EL-4胸腺瘤细胞的三个诱变亚系可通过MHC非限制性细胞间相互作用组成性激活人和/或小鼠B细胞。激活信号本身不是促有丝分裂的,但能使B细胞在白细胞介素2(IL-2)刺激下增殖。此外,其中一个突变EL-4亚系在含有IL-1的巨噬细胞(P388D1)上清液存在时,可通过释放IL-2组成性应答。突变EL-4胸腺瘤细胞的这些功能特性与活化的正常T辅助细胞相关功能特性之间的确切关系仍有待确定。然而,EL-4细胞提供了一个独特的系统,可同时研究小鼠和人类B细胞反应。特别是,在本研究中观察到以下情况。首先,对于仅作用于小鼠B细胞的两个EL-4亚系,B细胞激活需要抗Ig抗体,而对于同时作用于小鼠和人类B细胞的第三个亚系,则不需要抗Ig抗体。在没有突变EL-4(或正常T)细胞的情况下,抗Ig本身不会导致显著的B细胞激活。其次,在将B细胞与EL-4细胞分离后,EL-4激活的B细胞在生长因子刺激下的增殖仅持续2天。因此,这些结果表明,表面Ig介导的B细胞激活信号的需求取决于直接T细胞信号的质量/强度,并且与T细胞相比,细胞间相互作用可能对B细胞的生长因子反应性施加更严格的控制。

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