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促红细胞生成素诱导Friend病毒感染的红系细胞成熟过程中的转铁蛋白受体数量、合成及内吞作用

Transferrin receptor number, synthesis, and endocytosis during erythropoietin-induced maturation of Friend virus-infected erythroid cells.

作者信息

Sawyer S T, Krantz S B

出版信息

J Biol Chem. 1986 Jul 15;261(20):9187-95.

PMID:3013876
Abstract

Erythropoietin (EP) responsive Friend virus-infected erythroid cells had 200,000 steady-state binding sites for transferrin at 37 degrees C when isolated from the spleens of Friend virus-infected mice. Upon culture of these cells with EP, the synthesis of transferrin receptors increased 4- to 7-fold and the number of transferrin-binding sites per cell doubled after 24 h. However, the rate of uptake of 59Fe from transferrin remained constant at approximately 35,000 atoms of 59Fe per minute per cell during this period in culture. The amount of 125I-transferrin internalized during the steady-state binding did not change during this culture period while the transferrin bound to the surface increased 3-fold. At all stages of erythroid maturation, the maximum rate of endocytosis was determined to be 18,000 molecules of transferrin per minute per cell, and the interval that 125I-transferrin remains in the interior of the cell was calculated to be 6.9 min. After 48 h of culture with EP, the number of steady-state transferrin-binding sites was reduced in part due to the sequestration of surface receptors within the cell. The uptake of iron from transferrin was limited by the level of endocytosis of transferrin during the initial phase of culture and the number of transferrin receptors at the cell surface during the latter stages of erythroid maturation of these cells.

摘要

当从感染了弗氏病毒的小鼠脾脏中分离时,促红细胞生成素(EP)反应性弗氏病毒感染的红系细胞在37℃时具有200,000个转铁蛋白的稳态结合位点。用EP培养这些细胞后,转铁蛋白受体的合成增加了4至7倍,并且在24小时后每个细胞的转铁蛋白结合位点数量增加了一倍。然而,在此培养期间,每细胞每分钟从转铁蛋白摄取59Fe的速率保持恒定,约为35,000个59Fe原子。在稳态结合期间内化的125I-转铁蛋白的量在该培养期间没有变化,而结合到表面的转铁蛋白增加了3倍。在红系成熟的所有阶段,确定内吞作用的最大速率为每细胞每分钟18,000个转铁蛋白分子,并且计算出125I-转铁蛋白保留在细胞内部的时间间隔为6.9分钟。用EP培养48小时后,稳态转铁蛋白结合位点的数量减少,部分原因是细胞内表面受体的隔离。在培养的初始阶段,从转铁蛋白摄取铁受到转铁蛋白内吞作用水平的限制,而在这些细胞红系成熟的后期阶段,受到细胞表面转铁蛋白受体数量的限制。

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