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- Kim, Jeong Yeon;
- An, Jinhyeon;
- Kim, Soyeon;
- Jo, Hye-Yeong;
- Lee, Eun Ji;
- ... Lee, Se-Hoon;
- 외 8명
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0초록
B cell involvement in neoantigen-driven antitumor immunity remains largely unexplored because of challenges in predicting B cell responses. Here, we developed a method to identify B cell epitopes by characterizing >437,000 peptides tested for IgG binding and >370 million B cell receptor (BCR) clones. Our single-cell BCR sequencing of pre- and post-severe acute respiratory syndrome coronavirus 2 vaccination validates the performance of this method. Mouse vaccination experiments demonstrate that B cell neoepitopes enhance immune responses, driving BCR expansion and tumor regression. Genomic analysis of >8000 The Cancer Genome Atlas (TCGA) samples reveals an inverse correlation between predicted B cell reactivity and mutation allele frequencies, indicating B cell-mediated neoantigen elimination. Applying our multiomics model to checkpoint blockade responses in 2074 patients highlights the clinical relevance of B cell neoepitope prediction. A meta-analysis of 11 personalized vaccine trials involving 1739 neoantigens suggests that incorporating B cell neoepitopes may improve vaccination efficacy. These results underscore the significance of B cell-reactive neoantigens in antitumor immunity.
키워드
- 제목
- B cell-reactive neoantigens boost antitumor immunity
- 저자
- Kim, Jeong Yeon; An, Jinhyeon; Kim, Soyeon; Jo, Hye-Yeong; Lee, Eun Ji; Kim, Minju; Cha, Hongui; Lee, Se-Hoon; Park, Hyun-Young; Kim, Sang Cheol; Cho, Dae-Yeon; Shin, Inkyung; Chang, Suhwan; Choi, Jung Kyoon
- 발행일
- 2025-12-03
- 유형
- Article
- 저널명
- Science advances
- 권
- 11
- 호
- 49
- 페이지
- eadx8303