Enhancing adoptive T-cell therapy with fucoidan-based IL-2 delivery microcapsules

Authors
Jeon, Eun YoungChoi, Da-somChoi, SeunghyunWon, Ju-youngJo, YunjuKim, Hye-binJung, YoungmeeShin, Sang ChulMin, HophilChoi, Hae WoongLee, Myeong SupPark, YoonChung, Justin J.Jin, Hyung-seung
Issue Date
2023-01
Publisher
Wiley | American Institute of Chemical Engineers; Society for Biological Engineering
Citation
Bioengineering & Translational Medicine, v.8, no.1
Abstract
Adoptive cell therapy (ACT) with antigen-specific T cells is a promising treatment approach for solid cancers. Interleukin-2 (IL-2) has been utilized in boosting the efficacy of ACT. However, the clinical applications of IL-2 in combination with ACT is greatly limited by short exposure and high toxicities. Herein, a complex coacervate was designed to intratumorally deliver IL-2 in a sustained manner and protect against proteolysis. The complex coacervate consisted of fucoidan, a specific IL-2 binding glycosaminoglycan, and poly-l-lysine, a cationic counterpart (FPC2). IL-2-laden FPC2 exhibited a preferential bioactivity in ex vivo expansion of CD8(+)T cells over Treg cells. Additionally, FPC2 was embedded in pH modulating injectable gel (FPC2-IG) to endure the acidic tumor microenvironment. A single intratumoral administration of FPC2-IG-IL-2 increased expansion of tumor-infiltrating cytotoxic lymphocytes and reduced frequencies of myeloid populations. Notably, the activation and persistency of tumor-reactive T cells were observed only in the tumor site, not in the spleen, confirming a localized effect of FPC2-IG-IL-2. The immune-favorable tumor microenvironment induced by FPC2-IG-IL-2 enabled adoptively transferred TCR-engineered T cells to effectively eradicate tumors. FPC2-IG delivery system is a promising strategy for T-cell-based immunotherapies.
Keywords
CANCER; IMMUNOTHERAPY; HEPARIN; BINDING; adoptive T-cell therapy; complex coacervate; fucoidan; immunotherapy; interleukin-2
ISSN
2380-6761
URI
https://pubs.kist.re.kr/handle/201004/114192
DOI
10.1002/btm2.10362
Appears in Collections:
KIST Article > 2023
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