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Circulating nano-particulate TLR9 agonist scouts out tumor microenvironment to release immunogenic dead tumor cells

机译:循环的纳米颗粒TLR9激动剂可探测出肿瘤微环境从而释放出具有免疫原性的死亡肿瘤细胞

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摘要

Recent evidence suggest that a β-glucan derived from mushroom Schizophyllan(SPG) complexed with a humanized TLR9 agonistic CpG DNA, K3 (K3-SPG) is a promising vaccine adjuvant that induces robust CD8 T cell responses to co-administered antigen. However, it has not been investigated whether K3-SPG alone can act as an anti-cancer immunotherapeutic agent or not. Here, we demonstrate that intravenous injection of K3-SPG, but not CpG alone, is accumulated in the tumor microenvironment and triggered immunogenic cell death (ICD) of tumor cells by local induction of type-I interferon (IFN) as well as IL-12. Resultant innate immune activation as well as subsequent tumor-specific CD8 T cell responses were contributed the tumor growth suppression. This anti-tumor effect of K3-SPG monotherapy was also confirmed by using various tumor models including pancreatic cancer peritoneal dissemination model. Taken together, nano-particulate TLR9 agonist injected intravenously can scout out tumor microenvironment to provoke local innate immune activation and release dead tumor cells into circulation that may induce broader and protective tumor antigen-specific CD8 T cells.
机译:最近的证据表明,与人源化TLR9激动性CpG DNA,K3(K3-SPG)复合的蘑菇裂褶多糖(SPG)衍生的β-葡聚糖是一种有前途的疫苗佐剂,可诱导对共同施用的抗原产生强烈的CD8 T细胞应答。然而,尚未研究单独的K3-SPG是否可以充当抗癌免疫治疗剂。在这里,我们证明,静脉注射K3-SPG而不是单独的CpG会在肿瘤微环境中积累,并通过局部诱导I型干扰素(IFN)和IL-来触发肿瘤细胞的免疫原性细胞死亡(ICD)。 12最终的先天免疫激活以及随后的肿瘤特异性CD8 T细胞应答有助于抑制肿瘤生长。通过使用各种肿瘤模型,包括胰腺癌腹膜扩散模型,也证实了K3-SPG单一疗法的这种抗肿瘤作用。综上所述,静脉内注射的纳米颗粒TLR9激动剂可以侦查肿瘤微环境,以激发局部先天免疫活化,并将死的肿瘤细胞释放到循环中,从而可以诱导更广泛的保护性肿瘤抗原特异性CD8 T细胞。

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