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肝脏急性期反应的发育调控

Developmental regulation of the hepatic acute phase response.

作者信息

Schwarzenberg S J, Potter C J, Berry S A

机构信息

Department of Pediatrics, University of Minnesota, Minneapolis 55455.

出版信息

Am J Physiol. 1991 Sep;261(3 Pt 1):C461-6. doi: 10.1152/ajpcell.1991.261.3.C461.

Abstract

For evaluation of the ontogenetic regulation of the acute phase response, inflammation was induced in Fischer rat litters at different postnatal ages. Four homologous rat hepatic serine protease inhibitor (Spi 2.1, Spi 2.2, Spi 2.3, and alpha 1-antitrypsin) mRNAs were measured in livers 24 h after injection. Animals mounted both positive and negative acute phase responses at all ages, but responses were blunted in young animals, reaching adult levels by days 7-19. alpha 1-Antitrypsin mRNA had no response, and Spi 2.2 mRNA had 50% the rise seen in adults on days 3 and 7. Spi 2.1 and 2.3 mRNAs, negative acute phase reactants, showed attenuation of adult response to inflammation in infant animals of 33% (Spi 2.1) and 40% (Spi 2.3). In hypophysectomized animals, the responses of Spi 2.2, 2.3, and alpha 1-antitrypsin mRNAs after turpentine stimulation were similar to that of normal animals, whereas Spi 2.1 mRNA did not change. In conclusion, infant animals mount a blunted response to tissue injury; multiple factors may be involved in the development of the full adult response. Immaturity of the pituitary may play a role in the suppression of Spi 2.1 mRNA's response during inflammation in infant animals. These highly evolutionary related genes will be helpful in identifying specific factors regulating gene expression in inflammation and development.

摘要

为评估急性期反应的个体发生调节,在不同出生后年龄的Fischer大鼠幼崽中诱导炎症。在注射后24小时测量肝脏中四种同源大鼠肝丝氨酸蛋白酶抑制剂(Spi 2.1、Spi 2.2、Spi 2.3和α1-抗胰蛋白酶)的mRNA。所有年龄段的动物都出现了阳性和阴性急性期反应,但幼龄动物的反应减弱,在7至19天时达到成年水平。α1-抗胰蛋白酶mRNA无反应,Spi 2.2 mRNA在第3天和第7天的升高幅度为成年动物的50%。Spi 2.1和2.3 mRNA作为阴性急性期反应物,在33%(Spi 2.1)和40%(Spi 2.3)的幼龄动物中显示出成年期对炎症反应的减弱。在垂体切除的动物中,松节油刺激后Spi 2.2、2.3和α1-抗胰蛋白酶mRNA的反应与正常动物相似,而Spi 2.1 mRNA没有变化。总之,幼龄动物对组织损伤的反应减弱;多种因素可能参与了成年期完全反应的发展。垂体不成熟可能在幼龄动物炎症期间抑制Spi 2.1 mRNA反应中起作用。这些高度进化相关的基因将有助于识别调节炎症和发育中基因表达的特定因素。

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