Promoting the Recruitment, Engagement, and Reinvigoration of Effector T Cells via an Injectable Hydrogel with a Supramolecular Binding Capability for Cancer Immunotherapy

Author:

Zhu Yueqiang12,Jin Liangjie12,Chen Junbin1,Su Miao1,Sun Tianmeng3,Yang Xianzhu124ORCID

Affiliation:

1. School of Biomedical Sciences and Engineering South China University of Technology Guangzhou International Campus Guangzhou Guangdong 511442 P. R. China

2. Guangdong Provincial Key Laboratory of Biomedical Engineering South China University of Technology Guangzhou Guangdong 510006 P. R. China

3. Key Laboratory of Organ Regeneration and Transplantation of Ministry of Education Institute of Immunology The First Hospital Jilin University Changchun 130061 China

4. National Engineering Research Center for Tissue Restoration and Reconstruction and Key Laboratory of Biomedical Materials and Engineering of the Ministry of Education South China University of Technology Guangzhou Guangdong 510006 P. R. China

Abstract

AbstractT cells play a basic and key role in immunotherapy against solid tumors, and efficiently recruiting them into neoplastic foci and sustaining long‐term effector function are consistent goals that remain a critical challenge. Here, an injectable alginate‐based hydrogel with abundant β‐cyclodextrin (ALG‐βCD) sites is developed and intratumorally injected to recruit CCR9+CD8+ T cells (a subset of T cells with robust antitumor activity) via the trapped chemokine CCL25. In the meantime, an intravenously injected adamantane‐decorated anti‐PD1 antibody (Ad‐aPD1) would hitchhike on recruited CCR9+CD8+ T cells to achieve the improved intratumoral accumulation of Ad‐aPD1. Moreover, the Ad‐PD1 and Ad‐PDL1 antibodies are immobilized in the ALG‐βCD hydrogel through supramolecular host–guest interactions of Ad and βCD, which facilitate engagement between CD8+ T cells and tumor cells and reinvigorate CD8+ T cells to avoid exhaustion. Based on this treatment strategy, T cell‐mediated anticancer activity is promoted at multiple levels, eventually achieving superior antitumor efficacy in both orthotopic and postsurgical B16‐F10 tumor models.

Funder

National Key Research and Development Program of China

National Natural Science Foundation of China

Publisher

Wiley

Subject

Mechanical Engineering,Mechanics of Materials,General Materials Science

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