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在大鼠急性期反应期间尿素合成的调节。

Regulation of urea synthesis during the acute-phase response in rats.

机构信息

Department of Hepatology and Gastroenterology, Aarhus University Hospital, 44 Norrebrogade, DK-8000 Aarhus, Denmark.

出版信息

Am J Physiol Gastrointest Liver Physiol. 2013 Apr 1;304(7):G680-6. doi: 10.1152/ajpgi.00416.2012. Epub 2013 Feb 7.

Abstract

The acute-phase response is a catabolic event involving increased waste of amino-nitrogen (N) via hepatic urea synthesis, despite an increased need for amino-N incorporation into acute-phase proteins. This study aimed to clarify the regulation of N elimination via urea during different phases of the tumor necrosis factor-α (TNF-α)-induced acute-phase response in rats. We used four methods to study the regulation of urea synthesis: We examined urea cycle enzyme mRNA levels in liver tissue, the hepatocyte urea cycle enzyme proteins, the in vivo capacity of urea-N synthesis (CUNS), and known humoral regulators of CUNS at 1, 3, 24, and 72 h after TNF-α injection (25 μg/kg iv rrTNF-α) in rats. Serum acute-phase proteins and their liver mRNA levels were also measured. The urea cycle enzyme mRNA levels acutely decreased and then gradually normalized, whereas the urea cycle enzyme proteins remained essentially unchanged over time. The CUNS rose after 3 h and then normalized. The acute-phase response was fully activated at 24 h with markedly increased serum levels of the acute-phase proteins. TNF-α acutely upregulated the CUNS. Later, despite the fully established 24-h acute-phase response and the decreased activity of the urea cycle enzyme genes, there was no change in the urea cycle enzyme proteins or the CUNS. Thus in no phase after the initiation of the acute-phase response was in vivo urea synthesis orchestrated in combination with acute-phase protein synthesis so as to limit N waste.

摘要

急性期反应是一种分解代谢事件,涉及通过肝脏尿素合成增加氨基酸氮(N)的浪费,尽管需要将氨基酸 N 掺入急性期蛋白中。本研究旨在阐明在 TNF-α(肿瘤坏死因子-α)诱导的大鼠急性期反应的不同阶段,通过尿素来调节 N 消除。我们使用四种方法研究尿素合成的调节:我们检查了肝组织中的尿素循环酶 mRNA 水平、肝细胞尿素循环酶蛋白、尿素-N 合成的体内能力(CUNS),以及在 TNF-α(25 μg/kg iv rrTNF-α)注射后 1、3、24 和 72 小时时已知的 CUNS 的体液调节剂,在大鼠中。还测量了血清急性期蛋白及其肝 mRNA 水平。尿素循环酶 mRNA 水平急性下降,然后逐渐正常化,而尿素循环酶蛋白随时间基本不变。CUNS 在 3 小时后上升,然后正常化。在 24 小时时,急性期反应完全激活,血清急性期蛋白水平明显升高。TNF-α 急性上调 CUNS。后来,尽管完全建立了 24 小时的急性期反应,并且尿素循环酶基因的活性降低,但尿素循环酶蛋白或 CUNS 没有变化。因此,在急性期反应开始后的任何阶段,体内尿素合成都没有与急性期蛋白合成协调,以限制 N 浪费。

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