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首页> 外文期刊>The journal of immunology >Erbb2 DNA Vaccine Combined with Regulatory T Cell Deletion Enhances Antibody Response and Reveals Latent Low-Avidity T Cells: Potential and Limits of Its Therapeutic Efficacy
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Erbb2 DNA Vaccine Combined with Regulatory T Cell Deletion Enhances Antibody Response and Reveals Latent Low-Avidity T Cells: Potential and Limits of Its Therapeutic Efficacy

机译:Erbb2 DNA疫苗结合调节性T细胞缺失增强抗体反应并揭示潜在的低亲和力T细胞:潜力和治疗功效的局限性

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Rat (r)Erbb2 transgenic BALB-neuT mice genetically predestined to develop multiple invasive carcinomas allow an assessment of the potential of a vaccine against the stages of cancer progression. Because of rErbb2 expression in the thymus and its overexpression in the mammary gland, CD8+ T cell clones reacting at high avidity with dominant rErbb2 epitopes are deleted in these mice. In BALB-neuT mice with diffuse and invasive in situ lesions and almost palpable carcinomas, a temporary regulatory T cells depletion combined with anti-rErbb2 vaccine markedly enhanced the anti-rErbb2 Ab response and allowed the expansion of latent pools of low-avidity CD8 + T cells bearing TCRs repertoire reacting with the rErbb2 dominant peptide. This combination of a higher Ab response and activation of a low-avidity cytotoxic response persistently blocked tumor progression at stages in which the vaccine alone was ineffective. However, when diffuse and invasive microscopic cancers become almost palpable, this combination was no longer able to secure a significant extension of mice survival.
机译:遗传上注定会发展为多种浸润性癌的大鼠(r)Erbb2转基因BALB-neuT小鼠可以评估针对癌症进展阶段的疫苗潜力。由于胸腺中的rErbb2表达及其在乳腺中的过度表达,在这些小鼠中缺失了以高亲和力与显性rErbb2表位反应的CD8 + T细胞克隆。在具有弥漫性和浸润性原位病变和几乎可触及的癌的BALB-neuT小鼠中,暂时性调节性T细胞耗竭与抗rErbb2疫苗联合可显着增强抗rErbb2 Ab反应,并允许扩大低亲和力CD8 +的潜伏库携带TCR的T细胞库与rErbb2优势肽反应。在单独的疫苗无效的阶段,较高的Ab应答和较低的细胞毒性应答的激活的结合持续阻止了肿瘤的进展。但是,当弥漫性和浸润性显微镜下的癌症几乎可以触及时,这种组合不再能够确保小鼠存活的显着延长。

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