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脂肪酸合酶基因表达的调控:一种减少脂肪堆积的方法。

Regulation of fatty acid synthase gene expression: an approach for reducing fat accumulation.

作者信息

Clarke S D

机构信息

Department of Food Science and Human Nutrition, Colorado State University, Fort Collins 80523.

出版信息

J Anim Sci. 1993 Jul;71(7):1957-65. doi: 10.2527/1993.7171957x.

DOI:10.2527/1993.7171957x
PMID:8349524
Abstract

Fatty acid synthase (FAS) catalyzes the last step in the fatty acid biosynthetic pathway. The tissue concentration of FAS, which is affected by a number of hormonal and dietary factors, is a key determinant for the maximal capacity of a tissue to synthesize fatty acids by the de novo pathway. The complete nucleotide sequence of the avian and rat FAS transcripts has been cloned. In addition, a 1.5-kb cDNA that represents the thioesterase domain of the pig FAS protein plus the entire 3'-untranslated region of the transcript was isolated from a porcine liver cDNA library. Using these FAS cDNA tools, FAS mRNA transcripts have been found in most tissues, including adipose, liver, lung, brain, kidney, and small intestine. Moreover, the abundance of FAS mRNA in a tissue determines the rate of FAS protein synthesis, and ultimately the tissue content of FAS protein. In the liver, the rate of FAS gene transcription dictates the level of FAS mRNA, whereas the FAS mRNA content of adipose tissue seems to be determined by factors that affect gene transcription and mRNA stability. Adaptive changes in the abundance of FAS mRNA seem to occur primarily in hepatic and adipose tissues, whereas FAS expression in other tissue types is resistant to nutritional and hormonal manipulations. This review presents the concept that the tissue-specific adaptation in FAS gene expression can be exploited to develop a tissue-specific inhibitor of FAS gene expression and, hence, reduce the tissue capacity for fat accretion through the de novo biosynthetic pathway.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

脂肪酸合酶(FAS)催化脂肪酸生物合成途径的最后一步。FAS的组织浓度受多种激素和饮食因素影响,是组织通过从头合成途径合成脂肪酸最大能力的关键决定因素。禽类和大鼠FAS转录本的完整核苷酸序列已被克隆。此外,从猪肝cDNA文库中分离出一个1.5kb的cDNA,它代表猪FAS蛋白的硫酯酶结构域加上转录本的整个3'非翻译区。利用这些FAS cDNA工具,已在大多数组织中发现FAS mRNA转录本,包括脂肪、肝脏、肺、脑、肾和小肠。此外,组织中FAS mRNA的丰度决定FAS蛋白的合成速率,并最终决定FAS蛋白的组织含量。在肝脏中,FAS基因转录速率决定FAS mRNA水平,而脂肪组织中FAS mRNA含量似乎由影响基因转录和mRNA稳定性的因素决定。FAS mRNA丰度的适应性变化似乎主要发生在肝脏和脂肪组织中,而其他组织类型中FAS的表达对营养和激素操作具有抗性。本综述提出了这样一种概念,即可以利用FAS基因表达的组织特异性适应性来开发FAS基因表达的组织特异性抑制剂,从而通过从头合成途径降低组织脂肪蓄积的能力。(摘要截短于250字)

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