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首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Virus-encoded ectopic CD74 enhances poxvirus vaccine efficacy.
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Virus-encoded ectopic CD74 enhances poxvirus vaccine efficacy.

机译:病毒编码的异位CD74可增强痘病毒疫苗的功效。

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摘要

Vaccinia virus (VV) has been used globally as a vaccine to eradicate smallpox. Widespread use of this viral vaccine has been tempered in recent years because of its immuno-evasive properties, with restrictions prohibiting VV inoculation of individuals with immune deficiencies or atopic skin diseases. VV infection is known to perturb several pathways for immune recognition including MHC class II (MHCII) and CD1d-restricted antigen presentation. MHCII and CD1d molecules associate with a conserved intracellular chaperone, CD74, also known as invariant chain. Upon VV infection, cellular CD74 levels are significantly reduced in antigen-presenting cells, consistent with the observed destabilization of MHCII molecules. In the current study, the ability of sustained CD74 expression to overcome VV-induced suppression of antigen presentation was investigated. Viral inhibition of MHCII antigen presentation could be partially ameliorated by ectopic expression of CD74 or by infection of cells with a recombinant VV encoding murine CD74 (mCD74-VV). In contrast, virus-induced disruptions in CD1d-mediated antigen presentation persisted even with sustained CD74 expression. Mice immunized with the recombinant mCD74-VV displayed greater protection during VV challenge and more robust anti-VV antibody responses. Together, these observations suggest that recombinant VV vaccines encoding CD74 may be useful tools to improve CD4? T-cell responses to viral and tumour antigens.
机译:牛痘病毒(VV)已在全球范围内用作根除天花的疫苗。由于其免疫逃逸特性,近年来已对该病毒疫苗的广泛使用进行了调整,但限制条件是禁止对有免疫缺陷或特应性皮肤病的人进行VV接种。已知VV感染会干扰免疫识别的几种途径,包括II类MHC(MHCII)和CD1d限制性抗原呈递。 MHCII和CD1d分子与保守的细胞内分子伴侣CD74(也称为不变链)结合。在VV感染后,抗原呈递细胞中的细胞CD74水平显着降低,这与观察到的MHCII分子失稳相一致。在当前的研究中,研究了持续的CD74表达克服VV诱导的抗原呈递抑制的能力。通过异位表达CD74或用编码鼠CD74的重组VV(mCD74-VV)感染细胞,可以部分缓解MHCII抗原呈递的病毒抑制作用。相反,即使持续的CD74表达,病毒诱导的CD1d介导抗原呈递破坏仍持续存在。用重组mCD74-VV免疫的小鼠在VV攻击过程中显示出更大的保护作用,并表现出更强大的抗VV抗体反应。总之,这些观察结果提示,编码CD74的重组VV疫苗可能是改善CD4的有用工具? T细胞对病毒和肿瘤抗原的反应。

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