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Immunobiology: A CpG-loaded tumor cell vaccine induces antitumor CD4+ T cells that are effective in adoptive therapy for large and established tumors

机译:免疫生物学:加载CpG的肿瘤细胞疫苗可诱导抗肿瘤CD4 + T细胞该CD40 + T细胞可有效地对大而已确立的肿瘤进行过继治疗

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摘要

We designed a whole tumor cell vaccine by “loading” lymphoma tumor cells with CG-enriched oligodeoxynucleotide (CpG), a ligand for the Toll-like receptor 9 (TLR9). CpG-loaded tumor cells were phagocytosed, delivering both tumor antigen(s) and the immunostimulatory CpG molecule to antigen-presenting cells (APCs). These APCs then expressed increased levels of costimulatory molecules and induced T-cell immunity. TLR9 was required in the APCs but not in the CpG-loaded tumor cell. We demonstrate that T cells induced by this vaccine are effective in adoptive cellular therapy for lymphoma. T cells from vaccinated mice transferred into irradiated, syngeneic recipients protected against subsequent lymphoma challenge and, remarkably, led to regression of large and established tumors. This therapeutic effect could be transferred by CD4+ but not by CD8+ T cells. A CpG-loaded whole-cell vaccination is practical and has strong potential for translation to the clinical setting. It is currently being tested in a clinical trial of adoptive immunotherapy for mantle-cell lymphoma.
机译:我们通过将富含CG的寡脱氧核苷酸(CpG)(一种Toll样受体9(TLR9)的配体)“装载”到淋巴瘤肿瘤细胞上,从而设计了一种完整的肿瘤细胞疫苗。负载CpG的肿瘤细胞被吞噬,同时将肿瘤抗原和免疫刺激性CpG分子同时传递给抗原呈递细胞(APC)。这些APC然后表达增加水平的共刺激分子并诱导T细胞免疫。 APC中需要TLR9,而CpG加载的肿瘤细胞中不需要TLR9。我们证明了这种疫苗诱导的T细胞在淋巴瘤的过继细胞治疗中有效。来自接种疫苗的小鼠的T细胞转移到受辐照的同基因受体中,可以防止随后的淋巴瘤攻击,并显着地导致大型和成熟肿瘤的消退。这种治疗作用可以通过CD4 + 转移,而不能通过CD8 + T细胞转移。加载CpG的全细胞疫苗非常实用,具有转化为临床应用的强大潜力。目前正在对套细胞淋巴瘤进行过继免疫治疗的临床试验中对其进行测试。

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