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探究拓扑效应对蛋白生物缀合物稳定性增强和治疗性能的影响:蝌蚪、大环与 8 字形。

Probing the Topological Effects on Stability Enhancement and Therapeutic Performance of Protein Bioconjugates: Tadpole, Macrocycle versus Figure-of-Eight.

机构信息

Beijing National Laboratory for Molecular Sciences, Key Laboratory of Polymer Chemistry & Physics of Ministry of Education, Center for Soft Matter Science and Engineering, College of Chemistry and Molecular Engineering, Peking University, Beijing, 100871, P. R. China.

出版信息

Adv Healthc Mater. 2024 Nov;13(29):e2400466. doi: 10.1002/adhm.202400466. Epub 2024 Aug 1.

DOI:10.1002/adhm.202400466
PMID:39091049
Abstract

Chemical topology provides a unique dimension for making therapeutic protein bioconjugates with native structure and intact function, yet the effects of topology remain elusive. Herein, the design, synthesis, and characterization of therapeutic protein bioconjugates in three topologies (i.e., tadpole, macrocycle, and figure-of-eight), are reported. The interferon α2b (IFN) and albumin binding domain (ABD) are selected as the model proteins for bioconjugation and proof-of-concept. The biosynthesis of these topological isoforms is accomplished via direct expression in cells using SpyTag-SpyCatcher chemistry and/or split-intein-mediated ligation for topology diversification. The corresponding topologies are proven with combined techniques of LC-MS, SDS-PAGE, and controlled proteolytic digestion. While the properties of these topological isoforms are similar in most cases, the figure-of-eight-shaped bioconjugate, f8-IFN-ABD, exhibits the best thermal stability and anti-aggregation properties along with prolonged half-life and enhanced tumor retention relative to the tadpole-shaped control, tadp-IFN-ABD, and the macrocyclic control, c-IFN-ABD, showcasing considerable topological effects. The work expands the topological diversity of proteins and demonstrates the potential advantages of leveraging chemical topology for functional benefits beyond multi-function integration in protein therapeutics.

摘要

化学拓扑学为保持治疗性蛋白生物缀合物的天然结构和完整功能提供了一个独特的维度,但拓扑结构的影响仍难以捉摸。本文报道了三种拓扑结构(蝌蚪型、大环型和 8 字形)的治疗性蛋白生物缀合物的设计、合成和表征。选择干扰素 α2b(IFN)和白蛋白结合结构域(ABD)作为生物缀合和概念验证的模型蛋白。这些拓扑异构型的生物合成是通过使用 SpyTag-SpyCatcher 化学和/或分裂内含肽介导的连接在细胞中直接表达来实现的,用于拓扑多样化。使用 LC-MS、SDS-PAGE 和受控蛋白水解消化的组合技术证明了相应的拓扑结构。虽然这些拓扑异构型在大多数情况下具有相似的性质,但 8 字形生物缀合物 f8-IFN-ABD 与蝌蚪形对照 tadp-IFN-ABD 和大环对照 c-IFN-ABD 相比,表现出最佳的热稳定性和抗聚集特性,半衰期延长,肿瘤滞留增强,展示了相当大的拓扑效应。这项工作扩展了蛋白质的拓扑多样性,并证明了利用化学拓扑学在蛋白质治疗中除多功能集成之外,获得功能优势的潜力。

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