Metallothionein is crucial for safe intracellular copper storage and cell survival at normal and supra-physiological exposure levels

被引:94
作者
Tapia, L [1 ]
González-Agüero, M [1 ]
Cisternas, MF [1 ]
Suazo, M [1 ]
Cambiazo, V [1 ]
Uauy, R [1 ]
González, M [1 ]
机构
[1] Univ Chile, INTA, Lab Bioinformat & Expres Genica, Santiago 13811, Chile
关键词
copper; efflux; iron; metal lothionein; uptake; zinc;
D O I
10.1042/BJ20031174
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
MTs (metallothioneins) increase the resistance of cells to exposure to high Cu (copper) levels. Characterization of the MT-Cu complex suggests that MT has an important role in the cellular storage and/or delivery of Cu ions to cuproenzymes. In this work we investigate how these properties contribute to Cu homoeostasis by evaluating the uptake, accumulation and efflux of Cu in wildtype and MT I/II null rat fibroblast cell lines. We also assessed changes in the expression of Cu metabolism-related genes in response to Cu exposure. At sub-physiological Cu levels (0.4 muM), the metal content was not dependent on MT; however, when extracellular Cu was increased to physiological levels (10 muM), MTs were required for the cell's ability to accumulate the metal. The subcellular localization of the accumulated metal in the cytoplasm was MT-dependent. Following supra-physiological Cu exposure (> 50 muM), NIT null cells had a decreased capacity for Cu storage and an elevated sensitivity to a minor increment in intracellular metal levels, suggesting that intracellular Cu toxicity is due not to the metal content but to the interactions of the metal with cellular components. Moreover, MT null cells failed to show increased levels of mRNAs encoding MT 1, SOD1 (superoxide dismutase 1) and Ccs1 (Cu chaperone for SOD) in response to Cu exposure. These results support a role for MT in the storage of Cu in a safe compartment and in sequestering an intracellular excess of Cu in response to supra-physiological Cu exposure. Gene expression analysis suggests the necessity of having MT as part of the signalling pathway that induces gene expression in response to Cu.
引用
收藏
页码:617 / 624
页数:8
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