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一种用于测定血清中不稳定铜(II)离子的荧光测定法。

A fluorometric assay to determine labile copper(II) ions in serum.

机构信息

Department of Food Chemistry and Toxicology, Technische Universität Berlin, Straße des 17. Juni 135, 10623, Berlin, Germany.

TraceAge-DFG Research Unit on Interactions of Essential Trace Elements in Healthy and Diseased Elderly, Potsdam-Berlin-Jena, Germany.

出版信息

Sci Rep. 2023 Aug 7;13(1):12807. doi: 10.1038/s41598-023-39841-9.

Abstract

Labile copper(II) ions (Cu) in serum are considered to be readily available for cellular uptake and to constitute the biologically active Cu species in the blood. It might also be suitable to reflect copper dyshomeostasis during diseases such as Wilson's disease (WD) or neurological disorders. So far, no direct quantification method has been described to determine this small Cu subset. This study introduces a fluorometric high throughput assay using the novel Cu binding fluoresceine-peptide sensor FP4 (Kd of the Cu-FP4-complex 0.38 pM) to determine labile Cu in human and rat serum. Using 96 human serum samples, labile Cuwas measured to be 0.14 ± 0.05 pM, showing no correlation with age or other serum trace elements. No sex-specific differences in labile Cu concentrations were noted, in contrast to the total copper levels in serum. Analysis of the effect of drug therapy on labile Cu in the sera of 19 patients with WD showed a significant decrease in labile Cu following copper chelation therapy, suggesting that labile Cu may be a specific marker of disease status and that the assay could be suitable for monitoring treatment progress.

摘要

血清中的不稳定铜(II)离子(Cu)被认为易于被细胞摄取,并构成血液中具有生物活性的 Cu 物质。它也可能适合反映威尔逊病(WD)或神经紊乱等疾病期间的铜代谢紊乱。到目前为止,还没有描述直接定量测定这个小 Cu 子集的方法。本研究介绍了一种使用新型 Cu 结合荧光素肽传感器 FP4 的荧光高通量测定法(Cu-FP4 配合物的 Kd 为 0.38 pM),用于测定人血清和大鼠血清中的不稳定 Cu。使用 96 个人血清样本,测得不稳定 Cu 为 0.14±0.05 pM,与年龄或其他血清微量元素无相关性。与血清中的总铜水平相反,未观察到不稳定 Cu 浓度的性别特异性差异。对 19 例 WD 患者血清中药物治疗对不稳定 Cu 的影响分析表明,铜螯合治疗后不稳定 Cu 显著下降,提示不稳定 Cu 可能是疾病状态的特定标志物,该测定方法可能适合监测治疗进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7a2b/10406877/1ad17ffc8a93/41598_2023_39841_Fig1_HTML.jpg

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