Tumor‐Associated Myeloid Cells Selective Delivery of a Therapeutic Tumor Nano‐Vaccine for Overcoming Immune Barriers for Effective and Long‐Term Cancer Immunotherapy

Author:

Wang Chufan1,Zhao Jinglian1,Duan Yufei1,Lin Liping2,Zhang Qiang1,Zheng Haiping3,Shan Wenjun4,Wang Xiumin2,Ren Lei15ORCID

Affiliation:

1. Key Laboratory of Biomedical Engineering of Fujian Province University/Research Center of Biomedical Engineering of Xiamen Department of Biomaterials College of Materials Xiamen University Xiamen 361005 P. R. China

2. School of Pharmaceutical Sciences Xiamen University Xiamen 361102 P. R. China

3. School of Medicine Xiamen University Xiamen 361102 P. R. China

4. Department of Pharmacology College of Pharmacy Army Medical University (Third Military Medical University) Chongqing 400038 P.R. China

5. State Key Lab of Physical Chemistry of Solid Surfaces Xiamen University Xiamen 361005 P. R. China

Abstract

AbstractTherapeutic cancer vaccines have the potential to induce regression of established tumors, eradicate microscopic residual lesions, and prevent metastasis and recurrence, but their efficacy is limited by the low antigenicity of soluble antigens and the immunosuppressive tumor‐associated macrophages (TAMs) that promote tumor growth. In this study, a novel strategy is reported for overcoming these defenses: a dual‐targeting nano‐vaccine (NV) based on hepatitis B core antigen (HBcAg) derived virus‐like particles (VLPs), N‐M2T‐gp100 HBc NV, equipped with both SIGNR+ dendritic cells (DCs)/TAMs‐targeting ability and high‐density display of tumor‐associated antigen (TAA). N‐M2T‐gp100 HBc NVs‐based immunotherapy has demonstrated an optimal interaction between tumor‐associated antigens (TAAs) and the immune composition of the tumor microenvironment. In a melanoma model, N‐M2T‐gp100 HBc VLPs significantly reducing in situ and abscopal tumor growth, and provide long‐term immune protection. This remarkable anti‐tumor effect is achieved by efficiently boosting of T cells and repolarizing of M2‐like TAMs. This work opens exciting avenues for the development of personalized tumor vaccines targeting not just melanoma but potentially a broad range of cancer types based on functionalized VLPs.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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