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连续用铜(II)孵育的大鼠和小鼠肝细胞中的胞质铜结合蛋白。

Cytosolic copper-binding proteins in rat and mouse hepatocytes incubated continuously with Cu(II).

作者信息

Palida F A, Mas A, Arola L, Bethin K, Lonergan P A, Ettinger M J

机构信息

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

出版信息

Biochem J. 1990 Jun 1;268(2):359-66. doi: 10.1042/bj2680359.

DOI:10.1042/bj2680359
PMID:2363678
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1131440/
Abstract

The proteins that bind copper when it first enters cells are likely to play roles in its intracellular distribution and utilization. When hepatocytes were incubated with 64Cu(II), the time-dependence of the subcellular distribution of 64Cu was consistent with one or more cytosolic proteins distributing copper to the mitochondrial and nuclear fractions. Cytosolic copper was reproducibly distributed among four protein fractions from Sephadex G-150 columns at the earliest time (1 min) and at the lowest concentration used [2 microM-64Cu(II)] with both rat and mouse hepatocytes. Copper binding to proteins in these functions was sensitive to copper metabolic status. Hepatocytes from nutritionally copper-deficient rats or neonatal (9-30 days old) developing rats showed an inverse correlation between copper binding to metallothionein and copper binding to proteins in fraction I (approximately 88 kDa apparent) and fraction II (approximately 38 kDa apparent). The distribution of cytosolic 64Cu from the brindled-mouse model of Menkes disease indicated decreased binding by a protein in fraction I. Brindled-mouse hepatocytes also contain decreased levels of a approximately 55 kDa protein or subunit, which most likely represents a liver-specific secondary response to the primary defect. The results are consistent with one or more copper-binding proteins in fractions I and II having significant functions in intracellular copper metabolism.

摘要

铜刚进入细胞时与之结合的蛋白质可能在其细胞内分布和利用过程中发挥作用。当肝细胞与64Cu(II)一起孵育时,64Cu亚细胞分布的时间依赖性与一种或多种胞质蛋白将铜分配到线粒体和核部分相一致。在最早的时间点(1分钟)以及使用的最低浓度[2 microM - 64Cu(II)]下,大鼠和小鼠肝细胞的胞质铜可重复地分布在Sephadex G - 150柱的四个蛋白组分中。这些功能中蛋白质与铜的结合对铜代谢状态敏感。营养性铜缺乏大鼠或新生(9 - 30日龄)发育中大鼠的肝细胞显示,铜与金属硫蛋白的结合以及铜与组分I(表观分子量约88 kDa)和组分II(表观分子量约38 kDa)中蛋白质的结合呈负相关。门克斯病的斑驳小鼠模型中胞质64Cu的分布表明组分I中的一种蛋白质结合减少。斑驳小鼠肝细胞中一种约55 kDa的蛋白质或亚基水平也降低,这很可能代表肝脏对原发性缺陷的特异性继发性反应。结果表明,组分I和II中的一种或多种铜结合蛋白在细胞内铜代谢中具有重要功能。

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1
Cytosolic copper-binding proteins in rat and mouse hepatocytes incubated continuously with Cu(II).连续用铜(II)孵育的大鼠和小鼠肝细胞中的胞质铜结合蛋白。
Biochem J. 1990 Jun 1;268(2):359-66. doi: 10.1042/bj2680359.
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本文引用的文献

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Protein measurement with the Folin phenol reagent.使用福林酚试剂进行蛋白质测定。
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A sex-linked recessive disorder with retardation of growth, peculiar hair, and focal cerebral and cerebellar degeneration.一种伴性隐性疾病,伴有生长发育迟缓、特殊毛发以及局灶性脑和小脑变性。
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Metabolism of zinc and copper in the neonate: accumulation and function of (Zn, Cu)-metallothionein in the liver of the newborn rat.新生儿锌和铜的代谢:新生大鼠肝脏中(锌,铜)-金属硫蛋白的积累与功能
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Comparison of copper metabolism between brindled mice and dietary copper-deficient mice using 67Cu.使用67Cu对花斑小鼠和膳食铜缺乏小鼠的铜代谢进行比较。
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Copper transport kinetics by isolated rat hepatocytes.分离的大鼠肝细胞的铜转运动力学
Am J Physiol. 1983 Feb;244(2):G183-91. doi: 10.1152/ajpgi.1983.244.2.G183.
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Chromosomal location of human metallothionein genes: implications for Menkes' disease.人类金属硫蛋白基因的染色体定位:对门克斯病的影响。
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Kinetics of Cu(II) transport and accumulation by hepatocytes from copper-deficient mice and the brindled mouse model of Menkes disease.来自缺铜小鼠和门克斯病的斑驳小鼠模型的肝细胞对铜(II)的转运和积累动力学。
J Biol Chem. 1983 Nov 25;258(22):13621-6.
9
The metallothionein-I gene maps to mouse chromosome 8: implications for human Menkes' disease.金属硫蛋白-I基因定位于小鼠8号染色体:对人类门克斯病的意义。
Hum Genet. 1983;64(1):61-4. doi: 10.1007/BF00289481.
10
Metabolism of radiocopper (Cu64) in the rat.大鼠体内放射性铜(Cu64)的代谢
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