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Measurement of Interpeptidic Cu Exchange Rate Constants of Cu-Amyloid-β Complexes to Small Peptide Motifs by Tryptophan Fluorescence Quenching.利用色氨酸荧光猝灭法测量 Cu-淀粉样β 复合物与小肽基序之间的肽间 Cu 交换速率常数。
Inorg Chem. 2021 Jun 7;60(11):7650-7659. doi: 10.1021/acs.inorgchem.0c03555. Epub 2021 May 13.
2
Elucidation of a Copper Binding Site in Proinsulin C-peptide and Its Implications for Metal-Modulated Activity.胰岛素原C肽中铜结合位点的解析及其对金属调节活性的影响。
Inorg Chem. 2020 Jul 6;59(13):9339-9349. doi: 10.1021/acs.inorgchem.0c01212. Epub 2020 Jun 8.
3
A Pentapeptide with Tyrosine Moiety as Fluorescent Chemosensor for Selective Nanomolar-Level Detection of Copper(II) Ions.具有酪氨酸部分的五肽作为荧光化学传感器,用于选择性纳摩尔级检测铜(II)离子。
Int J Mol Sci. 2020 Jan 23;21(3):743. doi: 10.3390/ijms21030743.
4
Analysis of Metal Effects on C-Peptide Structure and Internalization.金属对 C 肽结构和内化的影响分析。
Chembiochem. 2019 Oct 1;20(19):2447-2453. doi: 10.1002/cbic.201900172. Epub 2019 May 9.
5
Copper(II) complexation by fragment of central part of FBP28 protein from Mus musculus.铜(II)与来自小家鼠的 FBP28 蛋白中心片段的络合。
Biophys Chem. 2018 Oct;241:55-60. doi: 10.1016/j.bpc.2018.08.002. Epub 2018 Aug 7.
6
Study of the Direct Red 81 Dye/Copper(II)-Phenanthroline System.直接红 81 染料/铜(II)-菲咯啉体系的研究。
Molecules. 2018 Jan 25;23(2):242. doi: 10.3390/molecules23020242.
7
Molar absorption coefficients and stability constants of Zincon metal complexes for determination of metal ions and bioinorganic applications.用于金属离子测定和生物无机应用的锌试剂金属配合物的摩尔吸收系数和稳定常数。
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8
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Biophys Chem. 2016 Sep;216:44-50. doi: 10.1016/j.bpc.2016.06.006. Epub 2016 Jul 2.
9
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定量研究在有发色团和无发色团存在的情况下,Cu(II)与肽残基之间的结合相互作用。

Quantifying the Binding Interactions Between Cu(II) and Peptide Residues in the Presence and Absence of Chromophores.

机构信息

Department of Chemistry, University of San Francisco.

Department of Chemistry, University of California, Davis.

出版信息

J Vis Exp. 2022 Apr 5(182). doi: 10.3791/63668.

DOI:10.3791/63668
PMID:35467664
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10405695/
Abstract

Copper(II) is an essential metal in biological systems, conferring unique chemical properties to the biomolecules with which it interacts. It has been reported to directly bind to a variety of peptides and play both necessary and pathological roles ranging from mediating structure to electron transfer properties to imparting catalytic function. Quantifying the binding affinity and thermodynamics of these Cu(II)-peptide complexes in vitro provides insight into the thermodynamic driving force of binding, potential competitions between different metal ions for the peptide or between different peptides for Cu(II), and the prevalence of the Cu(II)-peptide complex in vivo. However, quantifying the binding thermodynamics can be challenging due to a myriad of factors, including accounting for all competing equilibria within a titration experiment, especially in cases where there are a lack of discrete spectroscopic handles representing the peptide, the d-block metal ion, and their interactions. Here, a robust set of experiments is provided for the accurate quantification of Cu(II)-peptide thermodynamics. This article focuses on the use of electronic absorption spectroscopy in the presence and absence of chromophoric ligands to provide the needed spectroscopic handle on Cu(II) and the use of label-free isothermal titration calorimetry. In both experimental techniques, a process is described to account for all competing equilibria. While the focus of this article is on Cu(II), the described set of experiments can apply beyond Cu(II)-peptide interactions, and provide a framework for accurate quantification of other metal-peptide systems under physiologically relevant conditions.

摘要

铜(II)是生物系统中必需的金属,赋予与之相互作用的生物分子独特的化学性质。据报道,它可以直接与各种肽结合,并发挥从介导结构到电子转移性质再到赋予催化功能等多种必需和病理作用。在体外定量这些 Cu(II)-肽复合物的结合亲和力和热力学性质,可以深入了解结合的热力学驱动力、不同金属离子与肽之间或不同肽与 Cu(II)之间的潜在竞争,以及 Cu(II)-肽复合物在体内的普遍存在。然而,由于多种因素的影响,定量测定结合热力学可能具有挑战性,包括在滴定实验中考虑所有竞争平衡,特别是在缺乏离散光谱探针代表肽、d 区金属离子及其相互作用的情况下。本文提供了一套可靠的实验方法,用于准确测定 Cu(II)-肽的热力学性质。本文重点介绍了在存在和不存在生色配体的情况下使用电子吸收光谱来提供 Cu(II)所需的光谱探针,并使用无标记等温滴定量热法。在这两种实验技术中,都描述了一种方法来考虑所有竞争平衡。虽然本文的重点是 Cu(II),但所描述的实验集可应用于超出 Cu(II)-肽相互作用的范围,并为在生理相关条件下准确测定其他金属-肽系统提供了框架。