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A nanoparticle vaccine that targets neoantigen peptides to lymphoid tissues elicits robust antitumor T cell responses

机译:靶向淋巴组织的Neoantigen肽的纳米粒子疫苗引发鲁棒抗肿瘤T细胞应答

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Cancer vaccines using synthetic long peptides (SLP) targeting tumor antigens have been tested in the clinic but the outcomes have been unimpressive, perhaps because these peptides elicit predominantly CD4+ T cell responses. We hypothesized that enhanced delivery of peptide antigens to, and uptake in, secondary lymphoid tissues should elicit more robust CD8+ and CD4+ T cell responses and improved anti-tumor responses. Here, we have designed SLP-containing cationic lipoplexes (SLP–Lpx) that improve delivery of peptides to myeloid cells in the spleen and lymphatics. Using the G12D KRAS mutations as neoantigens, we found that vaccination of mice with naked synthetic peptides harboring the G12D mutation with CpG adjuvant stimulated mainly CD4+ T cell responses with limited tumor growth inhibition. On the other hand, immunization with SLP–Lpx stimulated both CD4+ and CD8+ T cells and suppressed tumor growth in a CD8+ T cell-dependent manner. Combination of the SLP–Lpx vaccines with a checkpoint inhibitor led to profound growth suppression of established tumors. These studies suggest that preferential targeting of peptides derived from neoantigens to the spleen via lipoplexes elicits potent CD4+ and CD8+ T cell responses that inhibit tumor growth.
机译:使用合成长肽(SLP)靶向肿瘤抗原的癌症疫苗已经在临床中进行了测试,但结果是不压迫的,也许是因为这些肽主要引发CD4 + T细胞反应。我们假设增强肽抗原的递送和摄取,次级淋巴组织应引起更强的CD8 +和CD4 + T细胞应答和改善的抗肿瘤反应。在这里,我们设计了含SLP的阳离子脂肪量(SLP-LPX),可改善果冻细胞的肽在脾脏和淋巴管中的粘液细胞。使用G12D KRAS突变作为新抗原,我们发现用含有裸体合成肽的小鼠接种与CPG佐剂的G12D突变刺激CD4 + T细胞应答,肿瘤生长抑制有限。另一方面,用SLP-LPX免疫刺激CD4 +和CD8 + T细胞并抑制CD8 + T细胞依赖性方式的肿瘤生长。 SLP-LPX疫苗与检查点抑制剂的组合导致建立肿瘤的深刻生长抑制。这些研究表明,通过Lipoplexes衍生自Neoantigens衍生自脾脏的肽的优先靶向抑制肿瘤生长的有效的CD4 +和CD8 + T细胞应答。

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