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炎症期间铜蓝蛋白基因表达的转录调控

Transcriptional regulation of ceruloplasmin gene expression during inflammation.

作者信息

Gitlin J D

机构信息

Edward Mallinckrodt Department of Pediatrics, Washington University School of Medicine, St. Louis, Missouri 63110.

出版信息

J Biol Chem. 1988 May 5;263(13):6281-7.

PMID:3360784
Abstract

Mixed sequence oligonucleotides were used to isolate a series of acute-phase human liver cDNA clones corresponding to the serum alpha 2-globulin ceruloplasmin. These clones were characterized, sequenced, and used to analyze changes in hepatic ceruloplasmin mRNA content during inflammation. In all species examined, hepatic ceruloplasmin mRNA content increased approximately 6-10-fold over control values within 24 h following the induction of inflammation. The mechanisms leading to this increase in hepatic ceruloplasmin mRNA content were studied following turpentine-induced inflammation in Syrian hamsters. Nuclear run-on assays demonstrated an increase in the relative rate of transcription of the ceruloplasmin gene within 3 h following induction, reaching maximum values by 18 h. Hepatic ceruloplasmin mRNA content increased 2-fold within 12 h following induction, reached maximum values by 24 h, and returned to control within 72 h. In contrast, serum ceruloplasmin concentration did not increase until 36 h, reached maximal levels by 120 h, and remained elevated for the course of the study. These data indicate that inflammation leads to a rapid increase in hepatic ceruloplasmin mRNA content. This increase is largely the result of increased ceruloplasmin gene transcription, but comparison of the relative rate of transcription and mRNA accumulation suggests that changes in ceruloplasmin mRNA turnover are also involved. In addition, translational and/or post-translational mechanisms must account for the observed changes in serum ceruloplasmin concentration seen during inflammation.

摘要

混合序列寡核苷酸被用于分离一系列与血清α2球蛋白铜蓝蛋白相对应的急性期人肝脏cDNA克隆。对这些克隆进行了表征、测序,并用于分析炎症期间肝脏铜蓝蛋白mRNA含量的变化。在所有检测的物种中,炎症诱导后24小时内,肝脏铜蓝蛋白mRNA含量比对照值增加了约6 - 10倍。在叙利亚仓鼠中,通过松节油诱导炎症后,研究了导致肝脏铜蓝蛋白mRNA含量增加的机制。核转录分析表明,诱导后3小时内铜蓝蛋白基因的相对转录速率增加,18小时达到最大值。诱导后12小时内肝脏铜蓝蛋白mRNA含量增加2倍,24小时达到最大值,并在72小时内恢复到对照水平。相比之下,血清铜蓝蛋白浓度直到36小时才增加,120小时达到最高水平,并在研究过程中一直保持升高。这些数据表明,炎症导致肝脏铜蓝蛋白mRNA含量迅速增加。这种增加主要是铜蓝蛋白基因转录增加的结果,但转录相对速率和mRNA积累的比较表明,铜蓝蛋白mRNA周转的变化也参与其中。此外,翻译和/或翻译后机制必须解释炎症期间观察到的血清铜蓝蛋白浓度变化。

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