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多胺是大鼠肝脏再生起始所必需的。

Polyamines are required for the initiation of rat liver regeneration.

作者信息

Alhonen Leena, Räsänen Tiina-Liisa, Sinervirta Riitta, Parkkinen Jyrki J, Korhonen Veli-Pekka, Pietilä Marko, Jänne Juhani

机构信息

A.I. Virtanen Institute for Molecular Sciences, University of Kuopio, P.O. Box 1627, FIN-70211 Kuopio, Finland.

出版信息

Biochem J. 2002 Feb 15;362(Pt 1):149-53. doi: 10.1042/0264-6021:3620149.

Abstract

A large number of studies applying inhibitors of polyamine biosynthesis have indicated that these compounds are required for animal cell proliferation. Here we show, using a transgenic rat model with activated polyamine catabolism, that a certain critical concentration of the higher polyamines spermidine and spermine is required for liver regeneration. Partial hepatectomy of transgenic rats expressing spermidine/spermine N(1)-acetyltransferase (SSAT) under the control of mouse metallothionein promoter strikingly induced the enzyme at 24 h and reduced hepatic spermidine by 80%. At that time, the weight of the liver remnant was significantly increased in syngenic rats and proliferating cell nuclear antigen (PCNA) labelling index was 20%, whereas the transgenic rats showed no liver weight gain and their PCNA-positive cells accounted for 0.5% of hepatocytes. Similarly, hepatic thymidine incorporation was markedly enhanced at this time point in syngenic, but not in transgenic, animals, whereas the rate of leucine incorporation was only marginally affected in the transgenic animals. At 3 days after operation, the spermidine pool in transgenic livers had increased to the pre-operative level, the remnant weight was significantly elevated and hepatic PCNA labelling index increased to 5%. N(1),N(11)-Diethylnorspermine, a powerful inducer of SSAT, inhibited liver weight gain and proliferative activity in both syngenic and transgenic rats. We found an extremely close correlation between hepatic spermidine, and less close between spermine, concentrations and PCNA labelling index during early liver regeneration. These results indicate that spermidine and/or spermine, but apparently not putrescine, are required for liver regeneration, yet at concentrations smaller than those normally found after partial hepatectomy.

摘要

大量应用多胺生物合成抑制剂的研究表明,这些化合物是动物细胞增殖所必需的。在此,我们利用一种具有激活的多胺分解代谢的转基因大鼠模型表明,肝脏再生需要一定临界浓度的高级多胺亚精胺和精胺。在小鼠金属硫蛋白启动子控制下表达亚精胺/精胺N(1)-乙酰转移酶(SSAT)的转基因大鼠,部分肝切除术后24小时该酶显著诱导,肝脏亚精胺减少80%。此时,同基因大鼠的肝残余重量显著增加,增殖细胞核抗原(PCNA)标记指数为20%,而转基因大鼠肝脏重量未增加,其PCNA阳性细胞占肝细胞的0.5%。同样,在这个时间点,同基因动物的肝脏胸腺嘧啶掺入显著增强,而转基因动物则没有,而亮氨酸掺入率在转基因动物中仅受到轻微影响。术后3天,转基因肝脏中的亚精胺池已增加到术前水平,残余重量显著升高,肝脏PCNA标记指数增加到5%。N(1),N(11)-二乙基亚精胺,一种强大的SSAT诱导剂,抑制同基因和转基因大鼠的肝脏重量增加和增殖活性。我们发现在早期肝脏再生过程中,肝脏亚精胺浓度与PCNA标记指数之间存在极其密切的相关性,而精胺浓度与PCNA标记指数之间的相关性较弱。这些结果表明,肝脏再生需要亚精胺和/或精胺,但显然不是腐胺,且所需浓度低于部分肝切除术后通常发现的浓度。

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