色谱 ›› 2026, Vol. 44 ›› Issue (1): 30-42.DOI: 10.3724/SP.J.1123.2025.06028

• 专论与综述 • 上一篇    下一篇

靶向生物膜的分子印迹策略与进展

袁雪婷, 王亮, 陈鲁茜, 胡良海*()   

  1. 吉林大学生命科学学院,超分子结构与材料全国重点实验室,超分子化学生物学研究中心,吉林 长春 130023
  • 收稿日期:2025-06-24 出版日期:2026-01-08 发布日期:2026-01-14
  • 通讯作者: * E-mail:lianghaihu@jlu.edu.cn.
  • 作者简介:第一联系人:#共同第一作者
  • 基金资助:
    国家自然科学基金(22374056)

Molecular imprinting strategies and advances targeting biomembranes

YUAN Xueting, WANG Liang, CHEN Luxi, HU Lianghai*()   

  1. Center for Supramolecular Chemical Biology,State Key Laboratory of Supramolecular Structure and Materials,School of Life Sciences,Jilin University,Changchun 130023,China
  • Received:2025-06-24 Online:2026-01-08 Published:2026-01-14
  • Supported by:
    National Natural Science Foundation of China(22374056)

摘要:

生物膜作为细胞内外环境之间的选择性屏障和沟通桥梁,在信号转导、能量传递和物质交换中发挥着重要作用。生物膜由脂质、蛋白质、糖类和其他成分组成,是细胞识别和通讯的枢纽。生物膜介导的特异性识别和结合,在疾病的早期诊断、药物靶向递送、环境监测等诸多方面具有潜在的应用价值。分子印迹聚合物(molecularly imprinted polymer,MIP)作为一种人工抗体,具有成本低、稳定性高和可重复使用等优点,已经成为特异性识别和结合生物膜上生物分子的有力工具。本文概述了针对生物膜上脂质、蛋白和糖分子印迹聚合物的最新进展,并深入探讨了MIP在生物医学领域中的应用。MIP作为高效的分子识别工具,能够实现对疾病生物标志物的高灵敏度和选择性检测;作为药物载体,MIP通过识别特定的疾病标志物,实现了精准的药物靶向递送;在细胞成像方面,MIP用于标记细胞表面的各类生物分子,丰富了成像的分子类型;此外,MIP还可构建传感器,用于检测生物样品中的目标分子。同时,文章也总结了当前MIP面临的主要挑战,包括合成步骤的复杂性、模板去除的不完全性、规模化生产的困难、性能的不足以及糖类模板制备的难题。为应对这些挑战,文中展望了使用虚拟模板或替代模板、整合新兴技术等可行性方案,并深入探讨了MIP应用的生物相容性问题以及应用转化的制约因素,旨在为实现MIP的实际转化应用提供合理的策略。

关键词: 生物膜, 分子印迹聚合物, 细胞外囊泡, 生物医学应用, 综述

Abstract:

Biomembranes are selective barriers and communication interfaces between intracellular and extracellular environments. They are crucial for signal transduction, energy transfer, and material exchange. Composed of lipids, proteins, glycans, and other components, biomembranes are central platforms for cell recognition and communication. Their specific recognition and binding abilities show great potential in early disease diagnosis, targeted drug delivery, environmental monitoring, and more. Molecularly imprinted polymer (MIP) has emerged as a robust tool for recognizing and binding biomolecules on biomembranes. This article summarizes recent technological advancements in MIP for biomembrane-associated lipids, proteins, and glycans. Lipids are a key part of biomembranes, crucial for maintaining membrane fluidity and stability. In lipid imprinting, lipid bilayers serve as templates. Functional monomers interact with lipid molecules and, upon polymerization, form a polymeric shell on the bilayer. Template removal leaves behind complementary binding sites. This strategy has been exploited to fabricate lipid-imprinted nanoparticles for drug delivery. These nanoparticles selectively recognize lipid components on cell membranes, thereby enabling targeted drug delivery. Proteins constitute another critical class of biomembrane components and execute diverse functions. Protein-imprinted MIPs selectively recognize membrane proteins such as cell-surface receptors, bacterial outer-membrane proteins, and viral capsid proteins. This enables precise identification and binding of specific proteins, which is useful in disease diagnosis and drug development. MIP can detect specific membrane protein biomarkers on cancer cells, allowing for early cancer detection and monitoring. Glycans also play a key role in biomembranes, particularly in cell recognition and immune responses. Carbohydrate-imprinted MIPs recognize specific glycan structures for use in disease diagnosis and therapy. Cancer cells have different glycan structures on their membranes compared to normal cells. These abnormal glycans serve as biomarkers for early cancer detection and monitoring. The article also emphasizes the potential of MIP in various applications. In disease diagnosis, MIP can develop biosensors for fast and accurate detection of disease biomarkers, enabling early treatment. In drug delivery, MIP can create targeted systems that deliver drugs directly to diseased cells, minimizing off-target effects and enhancing therapeutic efficacy. In cell imaging, MIP can specifically label cells or biomolecules, providing detailed images of cellular processes and aiding in understanding disease mechanisms. In biosensing, MIP can serve as efficient recognition elements to construct biosensors for detecting specific biomarkers in biological samples. The specific binding sites formed by molecular imprinting technology enable MIP-based biosensors to detect target molecules with high sensitivity and selectivity, providing a powerful tool for early disease diagnosis and real-time monitoring. However, the development of MIP still faces challenges, including complex synthetic procedures, incomplete template removal, limited scalability, and the need for performance optimization. The synthesis process is complex, requiring precise control of parameters like functional monomers, cross-linkers, and initiators. Incomplete template removal compromises binding affinity and selectivity. Scaling-up while maintaining batch-to-batch reproducibility is challenging, and the binding capacity, selectivity, and stability of MIPs must be optimized for each application. For glycan imprinting, monosaccharide templates have low specificity, glycan chain templates are difficult to synthesize and purify, and there is a lack of efficient O-glycan cleavage tools. To break through the bottleneck, the study improves template removal efficiency, synthetic optimization and structural controllability through controllable free radical/photo-initiated polymerization, magnetic material integration, microfluidics, artificial intelligence, machine learning and 3D printing; meanwhile, virtual templates, glycopeptide substitution templates, and solid-phase imprinting strategies are used to solve the scarcity of glycan templates. In addition, optimization of biocompatible materials, surface modification to reduce toxicity, and combination with computer simulation and automated preparation can accelerate clinical translation. In conclusion, MIP technology is highly promising for biomembrane research with broad applications in disease diagnosis, drug delivery, cell imaging, and extracellular vesicle enrichment. With continued development and optimization, MIP are expected to play an increasingly important role in biomedical and life sciences, offering more powerful tools and solutions for disease diagnosis, treatment, and monitoring.

Key words: biomembrane, molecularly imprinted polymer (MIP), extracellular vesicle (EV), biomedical applications, review

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