首页> 外文期刊>European Journal of Immunology >The Shiga toxin B-subunit targets antigen in vivo to dendritic cells and elicits anti-tumor immunity.
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The Shiga toxin B-subunit targets antigen in vivo to dendritic cells and elicits anti-tumor immunity.

机译:志贺毒素b亚单位抗原在体内的目标树突细胞和抒发抗肿瘤免疫力。

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摘要

The non-toxic B-subunit of Shiga toxin (STxB) interacts with the glycolipid Gb3, which is preferentially expressed on dendritic cells (DC) and B cells. After administration of STxB chemically coupled to OVA (STxB-OVA) in mice, we showed that the immunodominant OVA(257-264) peptide restricted by K(b) molecules is specifically presented by CD11c+ CD8alpha- DC, some of them displaying a mature phenotype. Using mice carrying a transgene encoding a diphtheria toxin receptor (DTR) under the control of the murine CD11c promoter, which allows inducible ablation of DC, we showed that DC are required for efficient priming of CTL after STxB-OVA vaccination. Immunization of mice with STxB-OVA induced OVA-specific CD8+ T cells detected ex vivo; these cells were long lasting, since they could be detected even 91 days after the last immunization and were composed of both central and memory T cells. Vaccination of mice with STxB-OVA and STxB coupled to E7, a protein derived from HPV16, inhibited tumor growth in prophylactic and therapeutic experiments. This effect was mainly mediated by CD8+ T cells. STxB therefore appears to be a powerful carrier directly targeting DC in vivo, resulting in a strong and durable CTL response associated with tumor protection.
机译:志贺毒素的无毒b亚单位(STxB)与醣脂类交互Gb3,优先表达对树突状细胞(DC)和B细胞。化学耦合在小鼠卵巢(STxB-OVA),我们表明immunodominant卵子(257 - 264)肽限制K (b)分子特别是由CD11c + CD8alpha -直流,他们中的一些人显示一个成熟的表型。老鼠携带转基因编码白喉毒素受体(DTR)的控制下小鼠CD11c启动子,它允许诱导直流的消融,我们表明,DC是必需的为有效的CTL STxB-OVA后启动接种疫苗。诱导OVA-specific CD8 + T细胞检测的前女友体内;甚至可以检测到最后后91天吗免疫和组成的中央和记忆T细胞。STxB-OVA和STxB耦合E7蛋白来自HPV16,抑制肿瘤的生长预防和治疗实验。影响主要是由CD8 + T细胞。因此,似乎是一个强大的载体直接针对DC体内,导致坚固耐用CTL反应相关肿瘤保护。

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