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胰高血糖素和三碘甲状腺原氨酸对肝脏信使核糖核酸S14水平的相反作用以及这些作用对昼夜节律因子的依赖性。

Opposing effects of glucagon and triiodothyronine on the hepatic levels of messenger ribonucleic acid S14 and the dependence of such effects on circadian factors.

作者信息

Kinlaw W B, Schwartz H L, Towle H C, Oppenheimer J H

出版信息

J Clin Invest. 1986 Oct;78(4):1091-6. doi: 10.1172/JCI112665.

Abstract

We have studied the effect of glucagon on the expression of a triiodothyronine (T3) and carbohydrate-inducible mRNA sequence (mRNA-S14) in rat liver that undergoes a threefold diurnal variation (peak, 2200 h; nadir, 0800 h). Glucagon injection into euthyroid rats (25 micrograms/100 g body wt i.p., three doses at 15-min intervals) during the nocturnal plateau of mRNA-S14 caused a monoexponential disappearance of this sequence (t1/2, 90 min) accompanied by a 90% reduction in the transcriptional rate in a nuclear run-off assay, indicative of a near total reduction of synthesis. This effect was markedly attenuated in rats treated with T3 (200 micrograms/100 g body wt i.p.) 24 h before glucagon injection. When T3 was given 15 min after glucagon, the glucagon-initiated decline in mRNA-S14 was reversed within 90 min, suggesting a rapid interaction between the two hormones in the evening. Curiously, administration of T3 alone at this hour did not affect a significant increase in mRNA-S14. At 0800 h, however, T3 caused the expected brisk induction of this sequence, whereas glucagon was without effect. In essence, glucagon affected mRNA-S14 synthesis only in the evening, while T3 increased levels of this sequence above the baseline only in the morning. T3, however, reversed the effect of prior glucagon injection at night. The observed alterations in hormonal responsivity could underly the diurnal variation of mRNA-S14 expression. Moreover, the data suggest the hypothesis that T3 may act on S14 gene expression by antagonizing factors that inhibit its transcription.

摘要

我们研究了胰高血糖素对大鼠肝脏中三碘甲状腺原氨酸(T3)和碳水化合物诱导型mRNA序列(mRNA-S14)表达的影响,该序列呈现出三倍的昼夜变化(峰值在22:00;谷值在08:00)。在mRNA-S14的夜间平台期,向甲状腺功能正常的大鼠腹腔注射胰高血糖素(25微克/100克体重,每15分钟注射一次,共三次),导致该序列呈单指数消失(半衰期为90分钟),同时在核转录分析中转录速率降低90%,这表明合成几乎完全减少。在用T3(200微克/100克体重,腹腔注射)处理24小时后的大鼠中,这种作用明显减弱。当在胰高血糖素注射后15分钟给予T3时,胰高血糖素引发的mRNA-S14下降在90分钟内逆转,这表明两种激素在傍晚时迅速相互作用。奇怪的是,在这个时间单独给予T3并没有显著影响mRNA-S14的增加。然而,在08:00时,T3导致了该序列预期的快速诱导,而胰高血糖素则没有作用。本质上,胰高血糖素仅在傍晚影响mRNA-S14的合成,而T3仅在早晨使该序列水平高于基线。然而,T3逆转了夜间先前注射胰高血糖素的作用。观察到的激素反应性改变可能是mRNA-S14表达昼夜变化的基础。此外,数据提出了一个假设,即T3可能通过拮抗抑制其转录的因子来作用于S14基因表达。

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