Novel Personalized Cancer Vaccine Using Tumor Extracellular Vesicles with Attenuated Tumorigenicity and Enhanced Immunogenicity

Author:

Han Jihoon12,Kim Seohyun123,Hwang Yeong Ha12,Kim Seong A12,Lee Yeji12,Kim Jihong12,Cho Seongeon12,Woo Jiwan4,Jeong Cherlhyun25,Kwon Minsu6,Nam Gi‐Hoon37,Kim In‐San12ORCID

Affiliation:

1. KU‐KIST Graduate School of Converging Science and Technology Korea University Seoul 02841 Republic of Korea

2. Chemical and Biomedical Integrative Research Center Korea Institute of Science and Technology (KIST) Seoul 02792 Republic of Korea

3. Department of Research and Development ShiftBio Seoul 02751 Republic of Korea

4. Research Animal Resource Center Korea Institute of Science and Technology (KIST) Seoul 02792 Republic of Korea

5. KHU‐KIST Department of Converging Science and Technology Kyung Hee University Seoul 02447 Republic of Korea

6. Department of Otolaryngology Asan Medical Center University of Ulsan College of Medicine Seoul 05505 Republic of Korea

7. Department of Biochemistry and Molecular Biology Korea University College of Medicine Seoul 02841 Republic of Korea

Abstract

AbstractCancer vaccines offer a promising avenue in cancer immunotherapy by inducing systemic, tumor‐specific immune responses. Tumor extracellular vesicles (TEVs) are nanoparticles naturally laden with tumor antigens, making them appealing for vaccine development. However, their inherent malignant properties from the original tumor cells limit their direct therapeutic use. This study introduces a novel approach to repurpose TEVs as potent personalized cancer vaccines. The study shows that inhibition of both YAP and autophagy not only diminishes the malignancy‐associated traits of TEVs but also enhances their immunogenic attributes by enriching their load of tumor antigens and adjuvants. These revamped TEVs, termed attenuated yet immunogenically potentiated TEVs (AI‐TEVs), showcase potential in inhibiting tumor growth, both as a preventive measure and a possible treatment for recurrent cancers. They prompt a tumor‐specific and enduring immune memory. In addition, by showing that AI‐TEVs can counteract cancer growth in a personalized vaccine approach, a potential strategy is presented for developing postoperative cancer immunotherapy that's enduring and tailored to individual patients.

Funder

National Research Foundation of Korea

Publisher

Wiley

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