Intratumoral delivery of the chitin-derived C100 adjuvant promotes robust STING, IFNAR, and CD8+ T cell-dependent anti-tumor immunity

被引:0
|
作者
Turley, Joanna L. [1 ]
Ward, Ross W. [1 ]
Huete-Carrasco, Jorge [1 ]
Munoz-Wolf, Natalia [1 ]
Roche, Kate [1 ]
Jin, Lei [2 ]
Bowie, Andrew [3 ]
Andersson, Mats [4 ]
Lavelle, Ed C. [1 ,5 ,6 ]
机构
[1] Trinity Coll Dublin, Trinity Biomed Sci Inst, Sch Biochem & Immunol, Adjuvant Res Grp, Dublin D02 R590 2, Ireland
[2] Univ Florida, Dept Med, Div Pulm Crit Care & Sleep Med, Gainesville, FL USA
[3] Trinity Coll Dublin, Trinity Biomed Sci Inst TBSI, Sch Biochem & Immunol, Dublin D02 R590, Ireland
[4] RISE Res Inst Sweden, Div Biosci & Mat, Forskargatan 18, S-15136 Sodertalje, Sweden
[5] Trinity Coll Dublin, Ctr Res Adapt Nanostruct & Nanodevices CRANN, Dublin D02 PN40 2, Ireland
[6] Trinity Coll Dublin, Adv Mat Bioengn Res Ctr AMBER, Dublin D02 PN40 2, Ireland
关键词
NF-KAPPA-B; DENDRITIC CELLS; I INTERFERON; TUMOR; ACTIVATION; MATURATION; REJECTION; ENHANCE; SIGNALS; MOUSE;
D O I
10.1016/j.xcrm.2024.101560
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Stimulator of IFN genes (STING) is a promising target for adjuvants utilized in in situ cancer vaccination approaches. However, key barriers remain for clinical translation, including low cellular uptake and accessibility, STING variability necessitating personalized STING agonists, and interferon (IFN)-independent signals that can promote tumor growth. Here, we identify C100, a highly deacetylated chitin -derived polymer (HDCP), as an attractive alternative to conventional STING agonists. C100 promotes potent anti -tumor immune responses, outperforming less deacetylated HDCPs, with therapeutic efficacy dependent on STING and IFN alpha/beta receptor (IFNAR) signaling and CD8 + T cell mediators. Additionally, C100 injection synergizes with systemic checkpoint blockade targeting PD -1. Mechanistically, C100 triggers mitochondrial stress and DNA damage to exclusively activate the IFN arm of the cGAS-STING signaling pathway and elicit sustained IFNAR signaling. Altogether, these results reveal an effective STING- and IFNAR-dependent adjuvant for in situ cancer vaccines with a defined mechanism and distinct properties that overcome common limitations of existing STING therapeutics.
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收藏
页数:20
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