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用于级联酶循环放大耦合免疫分析的分级多孔沸石咪唑酯骨架的配位驱动模板合成

Coordination-Driven Templated Synthesis of Hierarchically Porous Zeolitic Imidazolate Frameworks for Cascade Enzyme Cycle Amplification Coupled Immunoassay.

作者信息

Xia Fan, Yang Jian, Chen Jingwen, Liu Ximeng, Ma Zhefan, Gu Jinlou

机构信息

Key Laboratory for Ultrafine Materials of Ministry of Education, School of Materials Science and Engineering, East China University of Science and Technology, Shanghai 200237, China.

出版信息

ACS Appl Mater Interfaces. 2024 Aug 7;16(31):40602-40610. doi: 10.1021/acsami.4c06788. Epub 2024 Jul 23.

DOI:10.1021/acsami.4c06788
PMID:39042822
Abstract

Although hierarchically porous zeolitic imidazolate frameworks (HPZIFs) not only inherit the intrinsic architectural and chemical stabilities of their microporous counterparts but also afford open space for the efficient mass diffusion of the macromolecules involved, their rational design and construction are still challenging. Herein, HPZIFs with tailorable pore sizes ranging from 18 to 54 nm were successfully fabricated by using a newly developed soft-template-directed strategy. Our success rooted in the fact that the screened PS-PVP-PEO triblock copolymer could effectively coordinate with the metal precursor for the directed crystallization of ZIFs along surfactant assemblies. The advantages of continuous large pores and open structures in such HPZIFs were fully taken into account to serve as a bioreactor for the efficient immunoassay. The expanded large pores provided not only a significantly vast surface area to enhance the density of capture antibodies but also enough space for accommodating multiple conjugated biomolecules in one pore channel. In combination with a cascade enzyme cycle amplification strategy, a model biomarker of prostate-specific antigen (PSA) at the femtomolar level was checked with a limit of detection of 92 fM using the developed immunosensor. Specific screening on patients with prostate cancer or even benign prostatic hyperplasia was exemplified through accurately quantifying small changes of PSA concentration in clinical serum samples, prefiguring the great potential of the developed HPZIF-8 immunosensor platform for the early monitoring and diagnostics of diseases.

摘要

尽管分级多孔沸石咪唑酯骨架材料(HPZIFs)不仅继承了其微孔对应物的固有结构和化学稳定性,还为所涉及的大分子的高效质量扩散提供了开放空间,但其合理设计和构建仍然具有挑战性。在此,通过使用新开发的软模板导向策略成功制备了孔径范围为18至54纳米的可定制HPZIFs。我们的成功源于这样一个事实,即筛选出的PS-PVP-PEO三嵌段共聚物可以与金属前驱体有效配位,以沿着表面活性剂组装体引导ZIFs的结晶。充分考虑了此类HPZIFs中连续大孔和开放结构的优势,将其用作高效免疫分析的生物反应器。扩展的大孔不仅提供了显著大的表面积以提高捕获抗体的密度,还为在一个孔道中容纳多个共轭生物分子提供了足够的空间。结合级联酶循环放大策略,使用所开发的免疫传感器检测到飞摩尔水平的前列腺特异性抗原(PSA)模型生物标志物,检测限为92 fM。通过准确量化临床血清样本中PSA浓度的微小变化,举例说明了对前列腺癌甚至良性前列腺增生患者的特异性筛查,预示了所开发的HPZIF-8免疫传感器平台在疾病早期监测和诊断方面的巨大潜力。

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