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首页> 美国卫生研究院文献>Journal of Translational Medicine >A lipidated bi-epitope vaccine comprising of MHC-I and MHC-II binder peptides elicits protective CD4 T cell and CD8 T cell immunity against Mycobacterium tuberculosis
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A lipidated bi-epitope vaccine comprising of MHC-I and MHC-II binder peptides elicits protective CD4 T cell and CD8 T cell immunity against Mycobacterium tuberculosis

机译:包含MHC-I和MHC-II结合肽的脂化双表位疫苗可引起针对结核分枝杆菌的保护性CD4 T细胞和CD8 T细胞免疫

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BackgroundThe clinical trials conducted at Chingleput India suggest that BCG fails to protect against tuberculosis (TB) in TB-endemic population. Recent studies advocate that non-tuberculous mycobacteria and latent Mycobacterium tuberculosis (Mtb) infection interferes in the antigen processing and presentation of BCG in inducing protective immunity against Mtb. Thereby, indicating that any vaccine that require extensive antigen processing may not be efficacious in TB-endemic zones. Recently, we have demonstrated that the vaccine candidate L91, which is composed of lipidated promiscuous MHC-II binder epitope, derived from latency associated Acr1 antigen of Mtb is immunogenic in the murine and Guinea pig models of TB and conferred better protection than BCG against Mtb.
机译:背景在印度Chingleput进行的临床试验表明,BCG无法预防结核病流行人群的结核病(TB)。最近的研究主张非结核分枝杆菌和潜伏结核分枝杆菌(Mtb)感染会干扰BCG的抗原加工和呈递,从而诱导针对Mtb的保护性免疫。因此,表明需要大量抗原加工的任何疫苗在结核病流行区可能无效。最近,我们已经证明,由Mtb潜伏期相关Acr1抗原衍生的脂化混杂MHC-II结合物表位组成的候选疫苗L91在鼠和豚鼠的TB模型中具有免疫原性,并且比BCG具有更好的针对Mtb的保护作用。

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