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急性期反应中的翻译调控。铁调素对白介素-1的合成反应。

Translational control during the acute phase response. Ferritin synthesis in response to interleukin-1.

作者信息

Rogers J T, Bridges K R, Durmowicz G P, Glass J, Auron P E, Munro H N

机构信息

Division of Hematology, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

J Biol Chem. 1990 Aug 25;265(24):14572-8.

PMID:1696948
Abstract

Interleukin-1 (IL-1 beta) increases the synthesis of both heavy and light (L)-ferritin subunits when added to human hepatoma cells (HepG2) grown in culture. RNase protection and Northern blot analysis with L-ferritin probes revealed that no changes in L-ferritin mRNA levels occur after cytokine stimulation. However, the induction coincides with an increased association of the L-subunit mRNA with polyribosomes. Since the recruitment of stored ferritin mRNA onto polyribosomes is seen when iron enters the cell, the effect of IL-1 beta on iron uptake was tested and was found to be unaffected by the lymphokine. Neither transferrin receptor mRNA levels nor the number of receptors displayed on the cell surface was affected by IL-1 beta. However, the action of the cytokine on ferritin translation is inhibited by the action of the intracellular iron chelator deferoxamine. These data indicate that IL-1 beta induces ferritin gene expression by translational control of its mRNA. The pathway of induction is different from iron-dependent ferritin gene expression whereas regulation requires the background presence of cellular iron.

摘要

白细胞介素-1(IL-1β)添加到培养的人肝癌细胞(HepG2)中时,会增加重链和轻链(L)铁蛋白亚基的合成。用L-铁蛋白探针进行的核糖核酸酶保护和Northern印迹分析表明,细胞因子刺激后L-铁蛋白mRNA水平没有变化。然而,这种诱导与L-亚基mRNA与多核糖体的结合增加相吻合。由于当铁进入细胞时会观察到储存的铁蛋白mRNA募集到多核糖体上,因此测试了IL-1β对铁摄取的影响,发现其不受淋巴因子的影响。IL-1β既不影响转铁蛋白受体mRNA水平,也不影响细胞表面显示的受体数量。然而,细胞内铁螯合剂去铁胺的作用会抑制细胞因子对铁蛋白翻译的作用。这些数据表明,IL-1β通过对其mRNA的翻译控制来诱导铁蛋白基因表达。诱导途径不同于铁依赖性铁蛋白基因表达,而调节需要细胞内铁的背景存在。

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