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Evaluation of pH-sensitive fusogenic polymer-modified liposomes co-loadedwith antigen and α-galactosylceramide as an anti-tumor vaccine

机译:共载pH敏感的融合聚合物修饰脂质体的评估用抗原和α-半乳糖苷神经酰胺作为抗肿瘤疫苗

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摘要

pH-Sensitive fusogenic polymer-modified (pH-sensitive) liposomes co-loaded with tumor model antigen, ovalbumin (OVA), and adjuvant, α-galactosylceramide (α-GalCer) were fabricated and administered subcutaneously into mice. The ability of pH-sensitive liposomes containing OVA and α-GalCer to stimulate cellular and humoral immune responses in vivo was compared with OVA-encapsulating pH-sensitive liposomes as well as with OVA alone. After immunization, significant OVA-specific antibodies were detected in the serum. When sera were analyzed for isotype distribution, antigen-specific IgG1 antibody responses were noted in mice immunized with OVA alone, whereas immunization with OVA-containing pH-sensitive liposomes and with pH-sensitive liposomes containing OVA and α-GalCer resulted in the induction of OVA-specific IgG1 and IgG2b antibody responses. Moreover, more substantial production of IFN-γ and IL-4 was demonstrated in spleen cells from mice immunized with pH-sensitive liposomes having OVA and α-GalCer than OVA-containing pH-sensitive liposomes in vitro. Spleen cells from the immunized mice showed strong cytotoxic activity against E.G7-OVA tumor cells. In addition, prophylactic vaccination efficacy against tumor formation was evaluated. In all mice immunized with pH-sensitive liposomes having OVA and α-GalCer, immunization provided substantial protection from tumor formation. The therapeutic efficacy of pH-sensitiveliposomes containing OVA and α-GalCer against already established E.G7-OVA tumors was alsoinvestigated. Tumor growth was reduced significantly in all mice treated with pH-sensitiveliposomes having OVA and α-GalCer. The provided evidence on the advantage of antigen andα-GalCer co-encapsulation into pH-sensitive liposomes should be considered in the designof future cancer vaccines for prophylactic and therapeutic purposes.
机译:与肿瘤模型抗原,卵清蛋白(OVA)和佐剂α-半乳糖苷神经酰胺(α-GalCer)共同负载的pH敏感的融合型聚合物修饰的(pH敏感)脂质体被制成并皮下注射给小鼠。将包含OVA和α-GalCer的pH敏感脂质体在体内刺激细胞和体液免疫反应的能力与封装OVA的pH敏感脂质体以及单独使用OVA进行了比较。免疫后,在血清中检测到明显的OVA特异性抗体。当分析血清的同种型分布时,在单独用OVA免疫的小鼠中观察到抗原特异性IgG1抗体反应,而用含OVA的pH敏感脂质体和包含OVA和α-GalCer的pH敏感脂质体免疫则诱导OVA特异性IgG1和IgG2b抗体反应。此外,在体外用含有OVA和α-GalCer的pH敏感脂质体免疫的小鼠脾脏细胞中,IFN-γ和IL-4的产生要比含OVA的pH敏感脂质体产生的IFN-γ和IL-4更多。来自经免疫小鼠的脾细胞显示出针对E.G7-OVA肿瘤细胞的强细胞毒性活性。另外,评估了针对肿瘤形成的预防性疫苗接种功效。在用具有OVA和α-GalCer的pH敏感脂质体免疫的所有小鼠中,免疫均提供了对肿瘤形成的实质性保护。 pH敏感的治疗功效含有OVA和α-GalCer的脂质体还可以抵抗已经建立的E.G7-OVA肿瘤调查。用pH敏感剂治疗的所有小鼠的肿瘤生长均显着降低具有OVA和α-GalCer的脂质体。提供的证据表明抗原和在设计中应考虑将α-GalCer共包裹到pH敏感脂质体中用于预防和治疗目的的未来癌症疫苗。

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