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人类白细胞介素1β前体基因的转录调控

Transcriptional regulation of the human prointerleukin 1 beta gene.

作者信息

Fenton M J, Clark B D, Collins K L, Webb A C, Rich A, Auron P E

出版信息

J Immunol. 1987 Jun 1;138(11):3972-9.

PMID:3495577
Abstract

Interleukin 1 (IL 1) is a protein produced by monocytes in response to certain antigens which produces a wide variety of cellular responses in various tissues. We have studied the regulation of the human proIL-1 beta gene in THP-1 human monocytic leukemia cells. Lipopolysaccharide (LPS) induction of this gene results in an immediate and transient increase of message that rapidly falls to a low, but constant, level within 6 hr. This decrease results from a specific repression of transcription by 2 hr after stimulation. Cycloheximide inhibition of new protein synthesis causes a superinduction of IL 1 message, but does not alter the initial kinetics of message production. This presumably delays the synthesis of a labile transcriptional repressor protein and implies that the proIL-1 beta gene is under the control of both a transcriptional activator and a newly synthesized transcriptional repressor. The transient increase in mRNA production and the sustained low-level synthesis beyond the initial transient response suggest that the IL 1 protein itself may act intracellularly in a manner analogous to that described for several proto-oncogenes and cellular competence factors.

摘要

白细胞介素1(IL - 1)是单核细胞在接触某些抗原后产生的一种蛋白质,它能在多种组织中引发多种细胞反应。我们研究了人原IL - 1β基因在THP - 1人单核细胞白血病细胞中的调控情况。脂多糖(LPS)对该基因的诱导会导致信使RNA立即短暂增加,6小时内迅速降至低水平但稳定的状态。这种下降是由于刺激后2小时转录受到特异性抑制所致。放线菌酮抑制新蛋白质合成会导致IL - 1信使RNA超诱导,但不会改变信使RNA产生的初始动力学。这可能延迟了不稳定转录抑制蛋白的合成,意味着原IL - 1β基因受转录激活因子和新合成的转录抑制因子共同控制。信使RNA产生的短暂增加以及初始短暂反应后持续的低水平合成表明,IL - 1蛋白本身可能在细胞内以类似于几种原癌基因和细胞感受态因子的方式发挥作用。

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