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通过改良的蛋白质表达实现 Cu 和 Zn 同位素的再分配。

Re-partitioning of Cu and Zn isotopes by modified protein expression.

机构信息

Department of Earth Sciences, University of Bristol, Wills Memorial Building, Bristol, BS8 4EU, UK.

出版信息

Geochem Trans. 2008 Oct 10;9:11. doi: 10.1186/1467-4866-9-11.

Abstract

Cu and Zn have naturally occurring non radioactive isotopes, and their isotopic systematics in a biological context are poorly understood. In this study we used double focussing mass spectroscopy to determine the ratios for these isotopes for the first time in mouse brain. The Cu and Zn isotope ratios for four strains of wild-type mice showed no significant difference (delta 65Cu -0.12 to -0.78 permil; delta 66Zn -0.23 to -0.48 permil). We also looked at how altering the expression of a single copper binding protein, the prion protein (PrP), alters the isotope ratios. Both knockout and overexpression of PrP had no significant effect on the ratio of Cu isotopes. Mice brains expressing mutant PrP lacking the known metal binding domain have delta 65Cu isotope values of on average 0.57 permil higher than wild-type mouse brains. This implies that loss of the copper binding domain of PrP increases the level of 65Cu in the brain. delta 66Zn isotope values of the transgenic mouse brains are enriched for 66Zn to the wild-type mouse brains. Here we show for the first time that the expression of a single protein can alter the partitioning of metal isotopes in mouse brains. The results imply that the expression of the prion protein can alter cellular Cu isotope content.

摘要

铜和锌都有天然存在的非放射性同位素,而它们在生物环境中的同位素系统尚未得到充分了解。在这项研究中,我们首次使用双聚焦质谱法测定了小鼠大脑中这些同位素的比值。四种野生型小鼠的铜和锌同位素比值没有显著差异(δ65Cu 为-0.12 至-0.78 皮米;δ66Zn 为-0.23 至-0.48 皮米)。我们还研究了单一铜结合蛋白,朊病毒蛋白(PrP)的表达改变如何影响同位素比值。PrP 的敲除和过表达均对铜同位素比值没有显著影响。缺乏已知金属结合域的突变型 PrP 表达的小鼠大脑的 δ65Cu 同位素值比野生型小鼠大脑平均高 0.57 皮米。这意味着 PrP 的铜结合域的丧失会增加大脑中的 65Cu 水平。转基因小鼠大脑的 δ66Zn 同位素值相对于野生型小鼠大脑富集了 66Zn。这里我们首次表明,单个蛋白质的表达可以改变小鼠大脑中金属同位素的分配。结果表明,朊病毒蛋白的表达可以改变细胞内铜同位素的含量。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/995b/2570658/029c03d03867/1467-4866-9-11-1.jpg

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