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基于炔基铂(II) 2,6-双(苯并咪唑-2-基)吡啶配合物的精氨酸诱导超分子自组装用于肝素的选择性无标记检测和胰蛋白酶活性的实时监测

Protamine-Induced Supramolecular Self-Assembly of Red-Emissive Alkynylplatinum(II) 2,6-Bis(benzimidazol-2'-yl)pyridine Complex for Selective Label-Free Sensing of Heparin and Real-Time Monitoring of Trypsin Activity.

机构信息

Institute of Molecular Functional Materials (Areas of Excellence Scheme, University Grants Committee (Hong Kong)) and Department of Chemistry , The University of Hong Kong , Pokfulam Road , Hong Kong , People's Republic of China.

出版信息

ACS Appl Mater Interfaces. 2019 Sep 4;11(35):31585-31593. doi: 10.1021/acsami.9b08653. Epub 2019 Aug 22.

Abstract

A label-free detection assay is developed based on the design and synthesis of a new anionic alkynylplatinum(II) 2,6-bis(benzimidazol-2'-yl)pyridine complex with water-soluble pendants. With the aid of electrostatic interaction and noncovalent metal-metal and π-π stacking interactions, protamine is shown to induce supramolecular self-assembly of platinum(II) complexes with drastic UV-vis absorption and red emission changes. On the basis of the strong binding affinity of protamine and heparin, the ensemble has been further employed to probe heparin by monitoring the spectroscopic changes. Other than heparin, this ensemble can also detect the activity of trypsin, which can hydrolyze protamine into fragments, leading to the deaggregation of platinum(II) complexes. By modulation of the self-assembly properties of platinum(II) complexes via real-time UV-vis absorption and emission studies, the reported assay has been demonstrated to be a sensitive and selective detection method for trypsin, as well as trypsin inhibitor screening, which is essential for drug discovery.

摘要

基于设计和合成带有水溶性支链的新型阴离子炔基铂(II)2,6-双(苯并咪唑-2'-基)吡啶配合物,开发了一种无标记检测分析方法。在静电相互作用以及非共价金属-金属和π-π堆积相互作用的辅助下,鱼精蛋白被证明能够诱导铂(II)配合物的超分子自组装,从而导致剧烈的紫外可见吸收和红色发射变化。基于鱼精蛋白和肝素之间的强结合亲和力,该配合物进一步被用于通过监测光谱变化来探测肝素。除肝素外,该配合物还可以检测胰蛋白酶的活性,因为胰蛋白酶可以将鱼精蛋白水解成片段,从而导致铂(II)配合物的解聚集。通过实时紫外可见吸收和发射研究来调节铂(II)配合物的自组装性质,该报道的分析方法已被证明是一种用于胰蛋白酶的灵敏且选择性检测方法,同时也是用于药物发现的胰蛋白酶抑制剂筛选的重要方法。

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