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MUC1邻近系统的高灵敏度标记、可点击功能化及糖工程

Highly Sensitive Labeling, Clickable Functionalization, and Glycoengineering of the MUC1 Neighboring System.

作者信息

Wang Gang, Chen Ying, Wei Yuan, Zheng Lei, Jiao Jianwei, Guo Yuna

机构信息

Medical Science and Technology Innovation Center, Shandong First Medical University, Jinan 250117, China.

Nanjing University School of Life Sciences, Nanjing University, Nanjing 210023, China.

出版信息

JACS Au. 2024 Feb 8;4(2):828-836. doi: 10.1021/jacsau.3c00803. eCollection 2024 Feb 26.

DOI:10.1021/jacsau.3c00803
PMID:38425906
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10900198/
Abstract

This study introduces a novel wash-type affinity-primed proximity labeling (WAPL) strategy for labeling and surface engineering of the MUC1 protein neighboring system. The strategy entails the utilization of peroxidase in conjunction with a MUC1-selective aptamer, facilitating targeted binding to MUC1 and inducing covalent labeling of the protein neighboring system. This study reveals a novel finding that the WAPL strategy demonstrates superior labeling efficiency in comparison to nonwash-type affinity-primed proximity labeling, marking the first instance of such observations. The WAPL strategy provides signal amplification by converting a single recognition event into multiple covalent labeling events, thereby improving the detection sensitivity for subtle changes in MUC1. The WAPL platform employs two levels of labeling upgrades, modifying the biotin handles of the conventional labeling substrate, biotin-phenol. The first level involves a range of clickable molecules, facilitating dibenzoazacyclooctynylation, alkynylation, and -cyclooctenylation of the protein neighboring system. The second level utilizes lactose as a post-translational modification model, enabling rapid and reliable glycoengineering of the MUC1 neighboring system while remaining compatible with cell-based assays. The implementation of the WAPL strategy in protein neighboring systems has resulted in the establishment of a versatile platform that can effectively facilitate diverse monitoring and regulation techniques. This platform offers valuable insights into the regulation of relevant signaling pathways and promotes the advancement of novel therapeutic approaches, thereby bringing substantial implications for human health.

摘要

本研究介绍了一种用于标记和表面工程化MUC1蛋白邻近系统的新型洗涤型亲和引发邻近标记(WAPL)策略。该策略需要将过氧化物酶与MUC1选择性适配体结合使用,促进与MUC1的靶向结合并诱导蛋白邻近系统的共价标记。本研究揭示了一个新发现,即与非洗涤型亲和引发邻近标记相比,WAPL策略显示出更高的标记效率,这是首次有此类观察结果。WAPL策略通过将单个识别事件转化为多个共价标记事件来实现信号放大,从而提高对MUC1细微变化的检测灵敏度。WAPL平台采用了两级标记升级,对传统标记底物生物素-苯酚的生物素手柄进行修饰。第一级涉及一系列可点击分子,促进蛋白邻近系统的二苯并氮杂环辛炔化、炔基化和环辛烯化。第二级利用乳糖作为翻译后修饰模型,能够对MUC1邻近系统进行快速可靠的糖基工程,同时与基于细胞的检测兼容。WAPL策略在蛋白邻近系统中的实施导致建立了一个多功能平台,该平台可以有效地促进各种监测和调控技术。该平台为相关信号通路的调控提供了有价值的见解,并促进了新型治疗方法的发展,从而对人类健康产生重大影响。

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