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铁蛋白在成熟正常人类红系前体细胞中的表达。

Ferritin expression in maturing normal human erythroid precursors.

作者信息

Vaisman B, Meyron-Holtz E G, Fibach E, Krichevsky A M, Konijn A M

机构信息

Department of Human Nutrition and Metabolism, The Hebrew University, Faculty of Medicine, Jerusalem, Israel.

出版信息

Br J Haematol. 2000 Aug;110(2):394-401. doi: 10.1046/j.1365-2141.2000.02167.x.

Abstract

We studied the expression of H- and L-ferritin subunits at sequential stages of maturation of normal human erythroid precursors. The erythroid cells developed in liquid culture and were purified immunomagnetically before analysis. It was found that the content of both ferritin subunits decreased exponentially with maturation: the decrease was rapid when cellular haemoglobin was low, and it slowed down when the haemoglobin was increased. This mode of decline was especially pronounced for the L-subunits. The H-/L-subunit ratio did not change significantly during the investigated period. The synthesis of both subunits was equal at each given developmental stage, and declined significantly with maturation. However, this decline was just slightly faster than that of total protein synthesis. The data indicated that the degradation of H- and L-ferritin also declined as maturation proceeded. No decrease was observed in mRNA levels of either ferritin subunit. Thus, the ferritin content and turnover were maximal at the beginning of haemoglobin accumulation and diminished later. As the rate of ferritin turnover determines the rate of incorporation and release of its iron, the results presented suggest that ferritin mediates cellular iron transport and donates iron for haem synthesis, mainly at the beginning of haemoglobin accumulation. The synthesis of both ferritin subunits is regulated during erythroid maturation at the post-transcriptional level.

摘要

我们研究了正常人红细胞前体成熟的连续阶段中H-和L-铁蛋白亚基的表达。红细胞在液体培养中发育,并在分析前通过免疫磁珠法进行纯化。结果发现,随着成熟过程,两种铁蛋白亚基的含量均呈指数下降:当细胞血红蛋白含量较低时下降迅速,而当血红蛋白含量升高时下降减缓。这种下降模式在L-亚基中尤为明显。在研究期间,H-/L-亚基比值没有显著变化。在每个特定的发育阶段,两种亚基的合成量相等,并随着成熟而显著下降。然而,这种下降仅略快于总蛋白合成的下降。数据表明,随着成熟过程的进行,H-和L-铁蛋白的降解也在下降。未观察到任何一种铁蛋白亚基的mRNA水平降低。因此,铁蛋白含量和周转率在血红蛋白积累开始时最高,随后降低。由于铁蛋白周转率决定了其铁的掺入和释放速率,所呈现的结果表明,铁蛋白主要在血红蛋白积累开始时介导细胞铁转运并为血红素合成提供铁。两种铁蛋白亚基的合成在红细胞成熟过程中在转录后水平受到调控。

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