首页> 外文期刊>Molecular therapy: the journal of the American Society of Gene Therapy >Alphavirus-based vaccines encoding nonstructural proteins of hepatitis c virus induce robust and protective T-cell responses
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Alphavirus-based vaccines encoding nonstructural proteins of hepatitis c virus induce robust and protective T-cell responses

机译:编码丙型肝炎病毒非结构蛋白的基​​于甲病毒的疫苗可诱导强大的保护性T细胞反应

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An absolute prerequisite for a therapeutic vaccine against hepatitis C virus (HCV) infection is the potency to induce HCV-specific vigorous and broad-spectrum T-cell responses. Here, we generated three HCV vaccines based on a recombinant Semliki Forest virus (rSFV) vector expressing all- or a part of the conserved nonstructural proteins (nsPs) of HCV. We demonstrated that an rSFV vector was able to encode a transgene as large as 6.1 kb without affecting its vaccine immunogenicity. Prime-boost immunizations of mice with rSFV expressing all nsPs induced strong and long-lasting NS3-specific CD8 + T-cell responses. The strength and functional heterogeneity of the T-cell response was similar to that induced with rSFV expressing only NS3/4A. Furthermore this leads to a significant growth delay and negative selection of HCV-expressing EL4 tumors in an in vivo mouse model. In general, as broad-spectrum T-cell responses are only seen in patients with resolved HCV infection, this rSFV-based vector, which expresses all nsPs, inducing robust T-cell activity has a potential for the treatment of HCV infections.
机译:抗丙型肝炎病毒(HCV)感染的治疗性疫苗的绝对前提是诱导HCV特异性强力和广谱T细胞反应的潜能。在这里,我们基于表达所有或部分HCV保守非结构蛋白(nsPs)的重组Semliki Forest病毒(rSFV)载体产生了三种HCV疫苗。我们证明了rSFV载体能够编码高达6.1 kb的转基因而不会影响其疫苗的免疫原性。表达所有nsP的rSFV小鼠的初次免疫接种诱导了强烈而持久的NS3特异性CD8 + T细胞应答。 T细胞反应的强度和功能异质性与仅表达NS3 / 4A的rSFV诱导的相似。此外,这导致体内小鼠模型中显着的生长延迟和表达HCV的EL4肿瘤的阴性选择。通常,由于广谱T细胞应答仅在已解决的HCV感染患者中可见,因此这种表达所有nsP的基于rSFV的载体均能诱导强大的T细胞活性,从而具有治疗HCV感染的潜力。

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