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Recruitment of dendritic cells using ‘find-me’ signaling microparticles for personalized cancer immunotherapy
- Lee, J.A. ;
- Shin, J.M. ;
- Song, S.H. ;
- Kim, C.H. ;
- Son, S. ;
- Shin, S. ;
- Park, J.H.
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- Title
- Recruitment of dendritic cells using ‘find-me’ signaling microparticles for personalized cancer immunotherapy
- Issued Date
- 2022-03
- Citation
- Lee, J.A. (2022-03). Recruitment of dendritic cells using ‘find-me’ signaling microparticles for personalized cancer immunotherapy. Biomaterials, 282. doi: 10.1016/j.biomaterials.2022.121412
- Type
- Article
- Author Keywords
- Cancer antigen ; Cancer immunotherapy ; Find-me signal ; Immune checkpoint inhibitors ; Personalized therapy ; Polymeric microparticle
- Keywords
- EXPRESSION ; DEATH
- ISSN
- 0142-9612
- Abstract
-
Therapeutic cancer vaccines have attracted attention because of their potential to prime cytotoxic T cells, which are highly antigen (Ag)-specific, allowing personalized cancer immunotherapy. However, because of their low immunogenicity, cancer vaccines have been used in only a few types of cancers in clinics, primarily because of the poor Ag presentation of dendritic cells (DCs). To address these limitations of cancer vaccines, we show that ‘find-me’ signaling polymeric microparticles (F-PMs) bearing tumor lysate as an Ag can efficiently recruit DCs and facilitate antigen presentation. When subcutaneously injected into tumor-bearing mice, F-PMs significantly increased mature DCs in tumor-draining lymph nodes by eliciting adenosine triphosphate (ATP)-induced chemotaxis, resulting in high antitumor efficacy. CD8+ cytotoxic T cells were remarkably enriched in the tumor microenvironment following co-administration of an immune checkpoint inhibitor with F-PMs. We demonstrated that F-PMs elicit a robust antitumor immune response, which may provide a promising therapeutic option for cancer treatment. © 2022 Elsevier Ltd
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- Publisher
- Elsevier Ltd
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