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编码急性期蛋白CRP、SAA和C3的基因的转录调控。

Transcriptional regulation of genes encoding the acute-phase proteins CRP, SAA, and C3.

作者信息

Goldberger G, Bing D H, Sipe J D, Rits M, Colten H R

出版信息

J Immunol. 1987 Jun 1;138(11):3967-71.

PMID:2438331
Abstract

Inflammation or acute tissue injury results in a programmed change in the concentration of several plasma proteins. Among these proteins, two--C-reactive protein (CRP) and serum amyloid A protein (SAA)--increase up to 1000-fold after an acute-phase stimulus in humans and rabbits. To determine the mechanism for regulation of acute-phase gene expression, we examined changes in the rates of transcription and specific hepatic mRNA content for rabbit CRP, SAA, and some complement protein mRNA during an acute-phase response. Induction of a sterile inflammatory reaction with intramuscular injection of turpentine resulted in an increase in the hepatocellular content of CRP, SAA, C3, and factor B mRNA and the transcription of CRP, SAA, and C3 genes. These data suggest that the increase in CRP, SAA, and C3 serum concentrations observed during an acute-phase reaction is due to an increase in biosynthesis and is, at least in part, under transcriptional control.

摘要

炎症或急性组织损伤会导致几种血浆蛋白浓度发生程序性变化。在这些蛋白质中,两种——C反应蛋白(CRP)和血清淀粉样蛋白A(SAA)——在人类和兔子受到急性期刺激后浓度可升高至1000倍。为了确定急性期基因表达的调控机制,我们检测了兔CRP、SAA以及一些补体蛋白mRNA在急性期反应期间转录速率和肝脏特异性mRNA含量的变化。肌肉注射松节油引发无菌性炎症反应,导致肝细胞中CRP、SAA、C3和B因子mRNA含量增加,以及CRP、SAA和C3基因的转录增加。这些数据表明,在急性期反应期间观察到的CRP、SAA和C3血清浓度升高是由于生物合成增加所致,并且至少部分受转录控制。

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