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首页> 外文期刊>Clinical & developmental immunology. >Archaeosome Adjuvant Overcomes Tolerance to Tumor-Associated Melanoma Antigens Inducing Protective CD8 + T Cell Responses
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Archaeosome Adjuvant Overcomes Tolerance to Tumor-Associated Melanoma Antigens Inducing Protective CD8 + T Cell Responses

机译:古细菌佐剂克服了对肿瘤相关的黑色素瘤抗原诱导的保护性CD8 + T细胞应答的耐受性。

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Vesicles comprised of the ether glycerolipids of the archaeon Methanobrevibacter smithii (archaeosomes) are potent adjuvants for evoking CD8~(+)T cell responses. We therefore explored the ability of archaeosomes to overcome immunologic tolerance to self-antigens. Priming and boosting of mice with archaeosome-antigen evoked comparable CD8~(+)T cell response and tumor protection to an alternate boosting strategy utilizing live bacterial vectors for antigen delivery. Vaccination with melanoma antigenic peptides TRP_(181-189)and Gp100_(25-33)delivered in archaeosomes resulted in IFN- γ producing antigen-specific CD8~(+)T cells with strong cytolytic capability and protection against subcutaneous B16 melanoma. Targeting responses against multiple antigens afforded prolonged median survival against melanoma challenge. Entrapment of multiple peptides within the same vesicle or admixed formulations were both effective at evoking CD8~(+)T cells against each antigen. Melanoma-antigen archaeosome formulations also afforded therapeutic protection against established B16 tumors when combined with depletion of T-regulatory cells. Overall, we demonstrate that archaeosome adjuvants constitute an effective choice for formulating cancer vaccines.
机译:由古细菌Methanobrevibacter smithii(古生物体)的醚甘油脂组成的囊泡是引起CD8〜(+)T细胞应答的有效佐剂。因此,我们探索了古细菌克服自身抗原免疫耐受的能力。用古细菌抗原引发和加强小鼠诱发可比较的CD8〜(+)T细胞反应和肿瘤保护,这是利用活细菌载体进行抗原递送的另一种加强策略。用古细菌中递送的黑色素瘤抗原肽TRP_(181-189)和Gp100_(25-33)进行疫苗接种可产生IFN-γ产生具有强溶细胞能力并能抵抗皮下B16黑色素瘤的抗原特异性CD8〜(+)T细胞。针对多种抗原的靶向反应可延长针对黑色素瘤攻击的中位生存期。在同一囊泡或混合制剂中截留多种肽均有效诱发CD8〜(+)T细胞针对每种抗原。当与T调节细胞耗竭结合时,黑色素瘤抗原古菌体制剂还提供了针对已建立的B16肿瘤的治疗保护。总的来说,我们证明了古细菌佐剂是配制癌症疫苗的有效选择。

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