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利用新型树突状细胞策略诱导对腺病毒载体的免疫耐受。

Induction of immunological tolerance to adenoviral vectors by using a novel dendritic cell-based strategy.

机构信息

Address correspondence to Jim Hu,

出版信息

J Virol. 2012 Apr;86(7):3422-35. doi: 10.1128/JVI.06172-11. Epub 2012 Jan 18.

Abstract

The success of helper-dependent adenoviral (HD-Ad) vector-mediated lung gene therapy is hampered by the host immune response, which limits pulmonary transgene expression following multiple rounds of vector readminstration. Here, we show that HD-Ad-mediated pulmonary gene expression is sustained even upon three rounds of readministration to immunodeficient mice, highlighting the need to suppress the adaptive immune response for sustained gene expression following vector readministration. Therefore, we devised a dendritic cell (DC)-based strategy for induction of immunological tolerance toward HD-Ad vectors. DCs derived in the presence of interleukin-10 (IL-10) are refractory to HD-Ad-induced maturation and instead facilitate generation of IL-10-producing Tr1 regulatory T cells which suppress HD-Ad-induced T cell proliferation. Delivery of HD-Ad-pulsed, IL-10-modified DCs to mice induces long-lasting immunological tolerance to HD-Ad vectors, whereby pulmonary DC maturation, the T cell response, and antibody response to HD-Ad vectors are suppressed even after three rounds of pulmonary HD-Ad readministration. Moreover, sustained transgene expression is also observed in the lungs of mice immunized with HD-Ad-pulsed, IL-10-modified DCs even after three rounds of pulmonary HD-Ad delivery. Taken together, these studies identify the use of DCs generated in the presence of IL-10 as a novel strategy to induce long-lasting immune tolerance to HD-Ad vectors.

摘要

辅助依赖型腺病毒(HD-Ad)载体介导的肺部基因治疗的成功受到宿主免疫反应的阻碍,这限制了多次载体重复给药后肺部转基因的表达。在这里,我们表明,即使在免疫缺陷小鼠中进行三轮重复给药,HD-Ad 介导的肺部基因表达也能持续存在,这突出表明需要抑制适应性免疫反应,以在载体重复给药后维持基因表达。因此,我们设计了一种基于树突状细胞(DC)的策略,以诱导对 HD-Ad 载体的免疫耐受。在白细胞介素-10(IL-10)存在的情况下产生的 DC 对 HD-Ad 诱导的成熟具有抗性,而是促进产生 IL-10 产生的 Tr1 调节性 T 细胞,从而抑制 HD-Ad 诱导的 T 细胞增殖。将 HD-Ad 脉冲、IL-10 修饰的 DC 递送至小鼠中可诱导对 HD-Ad 载体的长期免疫耐受,从而即使在三轮肺部 HD-Ad 重复给药后,肺部 DC 成熟、T 细胞反应和对 HD-Ad 载体的抗体反应也受到抑制。此外,在经 HD-Ad 脉冲、IL-10 修饰的 DC 免疫的小鼠的肺部中也观察到持续的转基因表达,即使在三轮肺部 HD-Ad 给药后也是如此。总之,这些研究确定了使用在 IL-10 存在下生成的 DC 作为诱导对 HD-Ad 载体的长期免疫耐受的新策略。

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