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多嘧啶序列结合蛋白参与响应食物摄入对白蛋白合成的调控。

Polypyrimidine tract-binding protein is involved in regulation of albumin synthesis in response to food intake.

作者信息

Kuwahata Masashi, Kuramoto Yasuko, Sawai Yukiko, Amano Saki, Tomoe Yuka, Segawa Hiroko, Tatsumi Sawako, Ito Mikiko, Kobayashi Yukiko, Kido Yasuhiro, Oka Tatsuzo, Miyamoto Ken-Ichi

机构信息

Department of Molecular Nutrition, Institute of Health Biosciences, The University of Tokushima Graduate School, Tokushima, Japan.

出版信息

J Nutr Sci Vitaminol (Tokyo). 2008 Apr;54(2):142-7. doi: 10.3177/jnsv.54.142.

Abstract

Our recent study demonstrates that polypyrimidine tract-binding protein (PTB), which is a sequence specific RNA-binding protein, attenuates albumin synthesis in a cell-free translation system. In this study, the effects of food intake on regulation of albumin synthesis through binding of PTB to albumin messenger RNA (mRNA) were investigated. Rats were divided into 1 of 3 groups: fed; fasted for 36 h; or fasted for 36 h and then refed for 24 h. No significant differences in albumin mRNA levels were found among fed, fasted and refed rats. However, a decrease in the proportion of albumin mRNA associated with polysomes was identified in fasted rats. Furthermore, UV-cross linking analysis demonstrated that levels of albumin mRNA-PTB complex were increased in liver extracts from fasted rats. No significant differences in PTB levels in liver homogenate were found among the experimental groups. However, PTB level in the cytoplasmic fraction was higher in fasted rats than in fed rats. In refed rats, PTB level in the cytoplasmic fraction returned to a level comparable to that in fed rats, but was inhibited by treatment with rapamycin, a mammalian target of rapamycin (mTOR) inhibitor. These results suggest that localization of PTB is regulated by food intake through mTOR signaling, and alterations in level of albumin mRNA-PTB complex play a role in mediating the effects of food intake on albumin synthesis in the rat liver.

摘要

我们最近的研究表明,多嘧啶序列结合蛋白(PTB)是一种序列特异性RNA结合蛋白,在无细胞翻译系统中可减弱白蛋白的合成。在本研究中,我们调查了食物摄入通过PTB与白蛋白信使核糖核酸(mRNA)结合对白蛋白合成调控的影响。将大鼠分为3组中的1组:正常进食组;禁食36小时组;或禁食36小时后再喂食24小时组。在正常进食、禁食和再喂食的大鼠中,白蛋白mRNA水平未发现显著差异。然而,在禁食大鼠中,与多核糖体相关的白蛋白mRNA比例有所下降。此外,紫外线交联分析表明,禁食大鼠肝脏提取物中白蛋白mRNA-PTB复合物的水平升高。各实验组肝脏匀浆中的PTB水平未发现显著差异。然而,禁食大鼠细胞质部分的PTB水平高于正常进食大鼠。在再喂食的大鼠中,细胞质部分的PTB水平恢复到与正常进食大鼠相当的水平,但雷帕霉素(一种哺乳动物雷帕霉素靶蛋白(mTOR)抑制剂)处理可抑制其恢复。这些结果表明,PTB的定位受食物摄入通过mTOR信号通路的调节,白蛋白mRNA-PTB复合物水平的改变在介导食物摄入对大鼠肝脏白蛋白合成的影响中起作用。

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