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转铁蛋白与贝尔格莱德大鼠网织红细胞中的转铁蛋白循环

Transferrin and the transferrin cycle in Belgrade rat reticulocytes.

作者信息

Garrick M D, Gniecko K, Liu Y, Cohan D S, Garrick L M

机构信息

Department of Biochemistry, State University of New York, Buffalo 14214.

出版信息

J Biol Chem. 1993 Jul 15;268(20):14867-74.

PMID:8325865
Abstract

Belgrade rats have an autosomal recessive anemia with hypochromia and microcytosis. Iron uptake into reticulocytes is approximately 20% of normal, but transferrin uptake is unimpaired. We have systematically compared the transferrin cycle in Belgrade versus normal reticulocytes to locate the defect more precisely. Belgrade transferrin was functionally normal as purified transferrin or whole plasma. Transferrin affinity of Belgrade receptors was indistinguishable from normal, but Belgrade reticulocytes had twice as many receptors. Belgrade transferrin endocytosis was 1.5 times faster than normal, whereas exocytosis is about twice as fast. Initially Belgrade reticulocytes internalize iron at an unimpaired rate, but they lag behind normal by 5 min. During reincubation, they release 25-33% of iron taken up during a 30-min preincubation, whereas normal cells do not lose a detectable fraction. Unexpectedly, transferrin cycle time was unchanged. Hence another kinetic step of the cycle is slower, compensating for increases in Belgrade endocytosis and exocytosis. After one cycle, Belgrade reticulocytes retain only half of the iron that entered, but over 90% of iron entering normal cells remains within. Iron unloading is ineffective inside the Belgrade vesicle; 85% of iron that entered on transferrin returned to the medium after exocytosis, whereas only 45% of iron entering normal reticulocytes exits. Ineffective utilization of iron in or near Belgrade endosomes accounts for the Belgrade defect.

摘要

贝尔格莱德大鼠患有常染色体隐性贫血,伴有低色素血症和小红细胞症。网织红细胞对铁的摄取约为正常水平的20%,但转铁蛋白摄取未受损害。我们系统地比较了贝尔格莱德大鼠与正常网织红细胞的转铁蛋白循环,以更精确地定位缺陷所在。贝尔格莱德大鼠的转铁蛋白作为纯化的转铁蛋白或全血浆,功能正常。贝尔格莱德大鼠受体的转铁蛋白亲和力与正常情况无异,但贝尔格莱德大鼠的网织红细胞受体数量是正常的两倍。贝尔格莱德大鼠转铁蛋白的内吞作用比正常情况快1.5倍,而外排作用约快两倍。最初,贝尔格莱德大鼠的网织红细胞以正常速率摄取铁,但比正常情况滞后5分钟。在再次孵育期间,它们释放出在30分钟预孵育期间摄取铁的25%-33%,而正常细胞不会损失可检测到的部分。出乎意料的是,转铁蛋白循环时间没有变化。因此,循环的另一个动力学步骤较慢,补偿了贝尔格莱德大鼠内吞作用和外排作用的增加。经过一个循环后,贝尔格莱德大鼠的网织红细胞仅保留进入铁的一半,但进入正常细胞的铁超过90%仍留在细胞内。在贝尔格莱德大鼠的囊泡内铁卸载无效;转铁蛋白携带进入的铁,85%在胞吐作用后返回培养基,而进入正常网织红细胞的铁只有45%排出。贝尔格莱德大鼠内体或其附近铁利用无效导致了贝尔格莱德大鼠的缺陷。

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