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- Kim, Yun Ji;
- Bang, Ji Young;
- Yu, Hye-Won;
- Lim, Younghyun;
- Lee, Jeonghyeon;
- ... Seo, Young-Jin;
- 외 2명
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Optimizing co-stimulatory signaling to enhance T cell responses is central to effective antitumor immunity. In this study, we developed single-stranded RNAs (ssRNAs) utilizing the internal ribosome entry site (IRES) of encephalomyocarditis virus (EMCV) to express OX40L, 4-1BBL, and ICOSL and evaluated their efficacy. Co-culture of splenocytes with tumor cells transfected with these ssRNAs resulted in increased cytokine production and proliferation, along with altered T helper (Th) subsets. In vivo , intramuscular delivery of ssRNAs expressing co-stimulatory molecules expanded antigen-specific CD8+ T cells. Furthermore, intratumoral delivery of these ssRNAs significantly suppressed tumor growth and induced complete tumor regression in a subset of melanoma-bearing mice. Mechanistically, ssRNAs expressing co-stimulatory molecules promoted immune cell infiltration into the tumor site and increased the cytotoxic CD8+ T cells while reducing regulatory T cells (Tregs) in secondary lymphoid organs. These findings suggest that IRES-based ssRNAs expressing co-stimulatory molecules represent a promising platform for the development of effective cancer immunotherapies.
키워드
- 제목
- IRES-based RNAs expressing co-stimulatory molecules: Promising candidates for cancer immunotherapy
- 저자
- Kim, Yun Ji; Bang, Ji Young; Yu, Hye-Won; Lim, Younghyun; Lee, Jeonghyeon; Park, Hyo-Jung; Seo, Young-Jin; Hong, So-Hee
- 발행일
- 2026-03
- 유형
- Article
- 권
- 37
- 호
- 1