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A bi-adjuvant nanovaccine that potentiates immunogenicity of neoantigen for combination immunotherapy of colorectal cancer

机译:一种双佐剂纳米宫,其增强了Neoantigen的免疫原符,以进行结直肠癌的联合免疫疗法

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Neoantigen vaccines have been enthusiastically pursued for personalized cancer immunotherapy while vast majority of neoantigens have no or low immunogenicity. Here, a bi-adjuvant neoantigen nanovaccine (banNV) that codelivered a peptide neoantigen (Adpgk) with two adjuvants [Toll-like receptor (TLR) 7/8 agonist R848 and TLR9 agonist CpG] was developed for potent cancer immunotherapy. Specifically, banNVs were prepared by a nanotemplated synthesis of concatemer CpG, nanocondensation with cationic polypeptides, and then physical loading with hydrophobic R848 and Adpgk. The immunogenicity of the neoantigen was profoundly potentiated by efficient codelivery of neoantigen and dual synergistic adjuvants, which is accompanied by reduced acute systemic toxicity. BanNVs sensitized immune checkpoint programmed death receptor 1 (PD-1) on T cells, therefore, a combination of banNVs with aPD-1 conspicuously induced the therapy response and led to complete regression of 70% neoantigen-specific tumors without recurrence. We conclude that banNVs are promising to optimize personalized therapeutic neoantigen vaccines for cancer immunotherapy.
机译:Neoantigen疫苗已经热衷于个性化癌症免疫疗法,而绝大多数新奥地利格没有或低免疫原虫。这里,为具有两个佐剂的肽新抗原(ADPGK)进行双佐剂Neoantigen NaNovaccine(Bannv),为有效的癌症免疫疗法开发了具有两个佐剂的肽Neoantigen(ADPGK)[Toll样受体(TLR)7/8激动剂R848和TLR9激动剂CPG]。具体地,通过散滤体CpG的纳米核化合成,用阳离子多肽的纳米常见,然后用疏水性R848和ADPGK进行物理负载来制备Bannvs。 NeoAntigen的免疫原性通过高效的新抗原和双协同佐剂的有效编码递送,伴随着减少急性的全身毒性。 Bannvs敏化免疫检查点编程死亡受体1(PD-1)在T细胞上,因此,Bannvs的组合具有APD-1的组合显着诱导治疗反应,并导致70%Neoantigen特异性肿瘤的回归而不会复发。我们得出结论,Bannvs很有希望优化用于癌症免疫疗法的个性化治疗新稻草疫苗。

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