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使用表面分子印迹的Zn/Ce-ZIF对肌氨酸进行高特异性比色检测。

Highly specific colorimetric detection of sarcosine using surface molecular imprinted Zn/Ce-ZIF.

作者信息

Liu Peng, Liu Yeping, Gai Zhexu, Yang Fei, Yang Yanzhao

机构信息

Key Laboratory for Special Functional Aggregate Materials of Education Ministry, School of Chemistry and Chemical Engineering, Shandong University, Jinan, Shandong 250100, China.

School of Pharmaceutical Sciences, Shandong University, Jinan 250012, Shandong, China.

出版信息

J Colloid Interface Sci. 2025 Mar;681:239-249. doi: 10.1016/j.jcis.2024.11.179. Epub 2024 Nov 26.

Abstract

Despite significant progress in nanozyme research and the advancement of analytical techniques, the inherent lack of specificity for target analytes often limits their utility in analysis. Integrating specific recognition capabilities into inorganic nanomaterials, independent of biological catalysts or adaptors, represents a crucial breakthrough in the field. Detecting Sarcosine (Sar) in human urine has recently emerged as a non-invasive biomarker for prostate cancer (PCa), presenting a valuable diagnostic tool. This study introduces a novel method for embedding molecular imprinting sites directly onto the surface of a Zn/Ce-based zeolitic imidazolate framework (Zn/Ce-ZIF) nanozyme, facilitating the development of a highly specific colorimetric assay for precise Sar measurement. By utilizing the lanthanide metal cerium as the catalytic element and ZIF-8 as the structural scaffold, we synthesized spherical Zn/Ce-ZIF nanozymes with exceptional oxidase-like catalytic efficiency. The efficiency of molecular imprinting experiments and the ability of molecularly imprinted polymers (MIPs) to identify target molecules were significantly enhanced by using theortical calculations to screen suitable functional monomers. The molecularly imprinted nanozyme (Zn/Ce-ZIF@MIP) initiates a colorimetric oxidation reaction of 3,3',5,5'-tetramethylbenzidine (TMB), wherein the presence of Sar facilitates selective recognition and capture by the MIP shell, modulating the colorimetric response by hindering TMB's access to the catalytic site. An intelligent color extraction detection device has been developed for the rapid perception of Sar. This colorimetric sensing platform has been validated through the detection of Sar in simulated urine samples. Overall, the application of surface molecular imprinting enhances the functionality of nanozymes in analytical fields.

摘要

尽管纳米酶研究取得了重大进展,分析技术也不断进步,但纳米酶对目标分析物固有的特异性不足常常限制了它们在分析中的应用。将特异性识别能力整合到无机纳米材料中,而不依赖生物催化剂或适配体,是该领域的一项关键突破。检测人尿中的肌氨酸(Sar)最近已成为前列腺癌(PCa)的一种非侵入性生物标志物,是一种有价值的诊断工具。本研究介绍了一种将分子印迹位点直接嵌入基于锌/铈的沸石咪唑酯骨架(Zn/Ce-ZIF)纳米酶表面的新方法,有助于开发一种用于精确测量Sar的高特异性比色测定法。通过使用镧系金属铈作为催化元素,ZIF-8作为结构支架,我们合成了具有出色类氧化酶催化效率的球形Zn/Ce-ZIF纳米酶。通过理论计算筛选合适的功能单体,显著提高了分子印迹实验的效率以及分子印迹聚合物(MIP)识别目标分子的能力。分子印迹纳米酶(Zn/Ce-ZIF@MIP)引发3,3',5,5'-四甲基联苯胺(TMB)的比色氧化反应,其中Sar的存在促进了MIP壳层的选择性识别和捕获,通过阻碍TMB进入催化位点来调节比色响应。已经开发了一种智能颜色提取检测装置用于快速检测Sar。该比色传感平台已通过在模拟尿液样本中检测Sar得到验证。总体而言,表面分子印迹的应用增强了纳米酶在分析领域的功能。

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