Transcriptional regulation of the Icam-1 gene in antigen receptor- and phorbol ester-stimulated B lymphocytes: role for transcription factor EGR1.

J S Maltzman; J A Carmen; J G Monroe

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Transcriptional regulation of the Icam-1 gene in antigen receptor- and phorbol ester-stimulated B lymphocytes: role for transcription factor EGR1.

机译：抗原受体和磷酸酯刺激的B淋巴细胞ICAM-1基因的转录调节：转录因子EGR1的作用。

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Intercellular adhesion molecule (ICAM) 1/CD54 plays an important role in T cell dependent B cell activation and for function of B lymphocytes as antigen-presenting cells. ICAM-1 expression is upregulated as a consequence of B lymphocyte antigen receptor (BCR) signaling, thereby serving to render antigen-stimulated B cells more receptive to T cell-mediated costimulatory signals. We have investigated BCR-induced expression of the Icam-1 gene in primary B cells and B cell lines and have found it to be dependent on BCR-induced expression of the transcription factor EGR1. Icam-1 transcription, induced by BCR cross-linking or bypassing the BCR with phorbol ester, is absent in a B cell line in which the EGR1-encoding gene (egr-1) is methylated and not expressed. A potential EGR1-binding site was located at -701 bp upstream of the murine Icam-1 gene transcription start site and shown by electrophoretic mobility shift assay to bind to murine EGR1. Mutation of this site in the context of 1.1 kb of the Icam-1 promoter significantly abrogated transcriptional induction by phorbol ester and anti-mu stimulation in primary B cells. A direct effect of EGR1 on the Icam-1 promoter is suggested by the ability of EGR1 expressed from an SV40-driven expression vector transactivate the wild-type Icam-1 promoter, whereas mutation of the EGR1 mutation of the EGR1 binding motif at -701 bp markedly compromises this induction. These data identify EGR1 as a signaling intermediate in BCR-stimulated B cell functional responses, specifically linking BCR signal transduction to induction of the Icam-1 gene. Furthermore, similar findings for BCR-induced CD44 gene induction (Maltzman, J.S., J.A. Carman, and J.G. Monroe. 1996. Role of EGR1 in regulation of stimulus-dependent CD44 transcription in B lymphocytes. Mol. Cell. Biol. In press) suggest that EGR1 may be an important signaling molecule for regulating levels of migration and adhesion molecules during humoral immune responses.

机译：细胞间粘附分子（ICAM）1 / CD54在T细胞依赖性B细胞激活中起重要作用，以及B淋巴细胞作为抗原呈递细胞的功能。作为B淋巴细胞抗原受体（BCR）信号传导的后果上调ICAM-1表达，从而用于使抗原刺激的B细胞更容易受到T细胞介导的共刺激信号。我们研究了BCR诱导的原发性B细胞和B细胞系中的ICAM-1基因表达，并发现它依赖于转录因子EGR1的BCR诱导的表达。通过BCR交联或用散晶BCR诱导的ICAM-1转录在B细胞系中不存在于其中eGR1编码基因（EGR-1）甲基化并且不表达的B细胞系。潜在的EGR1结合位点位于鼠ICAM-1基因转录开始部位的-701bp上，并通过电泳迁移率转移测定显示与鼠EGR1结合。在ICAM-1启动子的1.1 kB的背景下，该网站的突变显着消除了菲尔伯酯的转录诱导和原发性B细胞中的抗穆刺激。通过从SV40驱动的表达载体表达的EGR1表达的EGR1反式静脉曲张野生型ICAM-1启动子的能力，提出了EGR1对ICAM-1启动子的直接效应，而EGR1结合基序的EGR1突变在-701则突变BP显着损害了这种归纳。这些数据识别EGR1作为BCR刺激的B细胞功能反应中的信号中间体，特别是将BCR信号转导与ICAM-1基因的诱导。此外，BCR诱导的CD44基因诱导的类似发现（Maltzman，JS，JA Carman和JG Monroe。1996。EGR1在B淋巴细胞中刺激依赖性CD44转录调节中的作用。摩尔。细胞。BIOL。在新闻界）建议EGR1可以是用于调节体液免疫应答期间迁移和粘附分子水平的重要信号分子。

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《The Journal of Experomental Medicine》 |1996年第4期|共13页
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J S Maltzman; J A Carmen; J G Monroe;
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6. Transcriptional regulation of the Icam-1 gene in antigen receptor- and phorbol ester-stimulated B lymphocytes: role for transcription factor EGR1 [O] . 1996

机译：抗原受体和佛波酯刺激的B淋巴细胞中Icam-1基因的转录调控：转录因子EGR1的作用
7. Transcriptional regulation of the Icam-1 gene in antigen receptor- and phorbol ester-stimulated B lymphocytes: role for transcription factor EGR1 [O] . 1996

机译：抗原受体和佛波酯刺激的B淋巴细胞中Icam-1基因的转录调控：转录因子EGR1的作用

Transcriptional regulation of the Icam-1 gene in antigen receptor- and phorbol ester-stimulated B lymphocytes: role for transcription factor EGR1.

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