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IgM受体介导的IgH 3'增强子反式激活将一种新型的Elf-1-AP-1蛋白复合物与增强子功能的发育调控联系起来。

IgM receptor-mediated transactivation of the IgH 3' enhancer couples a novel Elf-1-AP-1 protein complex to the developmental control of enhancer function.

作者信息

Grant P A, Thompson C B, Pettersson S

机构信息

Center for Biotechnology, Karolinska Institute, Novum, Huddinge, Sweden.

出版信息

EMBO J. 1995 Sep 15;14(18):4501-13. doi: 10.1002/j.1460-2075.1995.tb00129.x.

Abstract

The function of the temporally regulated B lymphocyte-specific immunoglobulin heavy chain (IgH) 3' enhancer has been linked to the IgH class switch machinery, but the physiological mechanism(s) of activation has not been discerned. Following crosslinking of the IgM receptor, we demonstrate that the enhancer is transactivated in the B lymphoma cell line BAL-17. In both induced primary B lymphocytes and BAL-17 cells, the enhancer activation is concomitant with the recruitment of a novel DNA binding complex, nuclear factor of activated B cells (NFAB). NFAB contains the tissue-restricted Ets protein Elf-1 and the AP-1 factors Jun-B and c-Fos, which bind to a novel 3' enhancer ETS-AP-1 motif. IgM receptor-mediated activation or stimulation by phorbol-ester in BAL-17 cells demonstrates that the ETS-AP-1 motif, when linked to a heterologous gene, can confer a ligand/receptor-dependent response. In NIH 3T3 cells, Elf-1 expression is required for efficient ETS-AP-1 promoter activity in response to stimulation by 12-O-tetradecanylphorbol 13-acetate. Our results suggest a biological role for Elf-1 in the regulation of IgH gene expression, attribute a functional role for receptor-induced AP-1 proteins in B lymphocytes and provide evidence for a direct link between IgM receptor-mediated signalling and 3' enhancer activation.

摘要

时间调控的B淋巴细胞特异性免疫球蛋白重链(IgH)3'增强子的功能已与IgH类别转换机制相关联,但激活的生理机制尚未明确。在IgM受体交联后,我们证明该增强子在B淋巴瘤细胞系BAL-17中被反式激活。在诱导的原代B淋巴细胞和BAL-17细胞中,增强子激活与一种新型DNA结合复合物——活化B细胞核因子(NFAB)的募集同时发生。NFAB包含组织限制性Ets蛋白Elf-1以及AP-1因子Jun-B和c-Fos,它们与一个新型的3'增强子ETS-AP-1基序结合。BAL-17细胞中IgM受体介导的激活或佛波酯刺激表明,当与异源基因相连时,ETS-AP-1基序可赋予配体/受体依赖性反应。在NIH 3T3细胞中,Elf-1表达是12-O-十四烷酰佛波醇13-乙酸酯刺激后有效ETS-AP-1启动子活性所必需的。我们的结果表明Elf-1在IgH基因表达调控中具有生物学作用,确定了受体诱导的AP-1蛋白在B淋巴细胞中的功能作用,并为IgM受体介导的信号传导与3'增强子激活之间的直接联系提供了证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/943a/394542/c47c65a5dc00/emboj00042-0126-a.jpg

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