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B细胞刺激因子-1和抗B细胞表面抗原抗体对小鼠前B细胞系中II类基因表达的差异诱导作用。

Differential induction of class II gene expression in murine pre-B-cell lines by B-cell stimulatory factor-1 and by antibodies to B-cell surface antigens.

作者信息

Polla B S, Ohara J, Paul W E, Nabavi N, Myer A, Liou H C, Shen F W, Gillis S, Bonventre J V, Glimcher L H

机构信息

Department of Cancer Biology, Harvard School of Public Health, Boston, MA 02115.

出版信息

J Mol Cell Immunol. 1988;3(6):363-73.

PMID:3151065
Abstract

We have previously reported that BSF-1 and an alloantibody to the B-cell differentiation antigen Lyb2 induce class II gene expression in two Ia negative pre-B-cell lines. Two questions were asked in these studies. The first question is whether the different stimuli which we and others have shown to induce class II expression in B-cells act via the same signal transduction mechanisms. The second question is whether the traditionally accepted pathway of B-cell differentiation, as defined by immunoglobulin (Ig) gene rearrangement, is applicable to other events that occur during B-cell differentiation. In this report, we have therefore examined a large panel of pre-B-cell lines at different stages of Ig gene rearrangement in an attempt to 1) identify the stage in B-cell development where class II gene expression occurs and where it becomes inducible by BSF-1 or anti-Lyb2, and 2) compare the signal transduction mechanisms used by these ligands. The majority of pre-B-cell lines tested did not express BSF-1 receptors and were consequently noninducible for class II by BSF-1; such cell lines were, however, inducible for class II expression by anti-Lyb2 and, in addition, by antibodies to the B220 membrane glycoprotein. The induction of class II molecules by BSF-1 and by anti-Lyb2 and anti-B220 differed in several respects: 1) Induction by anti-Lyb2 and anti-B220 did not require the presence of BSF-1 receptors; 2) BSF-1 selectively induced class II antigen expression while anti-Lyb2 and anti-B220 induced the expression of other surface markers as well; and 3) PGE2 inhibited BSF-1 but not antibody-mediated class II induction. Finally, the presence of receptors for BSF-1 and the baseline expression of cell surface Ia was shown to be unlinked to Ig gene rearrangement and expression in this series of pre-B-cell lines. The independent regulation of Ia and Ig genes observed here may reflect a branching rather than a linear pathway for B-cell differentiation. The differentiation of pre-B-cells to mature Ig-secreting cells should probably not be defined solely by rearrangement of Ig genes, since this is likely to represent an oversimplified view of B-cell differentiation.

摘要

我们之前报道过,BSF-1和针对B细胞分化抗原Lyb2的同种异体抗体可诱导两个Ia阴性前B细胞系中的II类基因表达。这些研究提出了两个问题。第一个问题是,我们和其他人已证明能在B细胞中诱导II类表达的不同刺激,是否通过相同的信号转导机制起作用。第二个问题是,由免疫球蛋白(Ig)基因重排定义的传统上被接受的B细胞分化途径,是否适用于B细胞分化过程中发生的其他事件。因此,在本报告中,我们检测了一大组处于Ig基因重排不同阶段的前B细胞系,试图1)确定B细胞发育中II类基因表达发生的阶段以及该阶段它可被BSF-1或抗Lyb2诱导的阶段,2)比较这些配体所使用的信号转导机制。大多数被检测的前B细胞系不表达BSF-1受体,因此不能被BSF-1诱导表达II类;然而,这些细胞系可被抗Lyb2以及抗B220膜糖蛋白抗体诱导表达II类。BSF-1、抗Lyb2和抗B220诱导II类分子表达在几个方面存在差异:1)抗Lyb2和抗B220诱导表达不需要BSF-1受体的存在;2)BSF-1选择性诱导II类抗原表达,而抗Lyb2和抗B220还诱导其他表面标志物的表达;3)前列腺素E2抑制BSF-1介导的II类诱导,但不抑制抗体介导的II类诱导。最后,在这一系列前B细胞系中,BSF-1受体的存在和细胞表面Ia的基线表达与Ig基因重排和表达无关。此处观察到的Ia和Ig基因的独立调节可能反映了B细胞分化的分支而非线性途径。前B细胞向成熟Ig分泌细胞的分化可能不应仅由Ig基因重排来定义,因为这可能代表了对B细胞分化的过度简化的观点。

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