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C7L 和 K1L 基因缺失导致天坛痘苗病毒重组病毒毒力显著降低。

Deletion of C7L and K1L genes leads to significantly decreased virulence of recombinant vaccinia virus TianTan.

机构信息

Division of Research on Virology and Immunology, State Key Laboratory for Infectious Disease Prevention and Control, National Center for AIDS/STD Control and Prevention-NCAIDS, China CDC, Beijing, China.

出版信息

PLoS One. 2013 Jul 1;8(7):e68115. doi: 10.1371/journal.pone.0068115. Print 2013.

Abstract

The vaccinia virus TianTan (VTT) has been modified as an HIV vaccine vector in China and has shown excellent performance in immunogenicity and safety. However, its adverse effects in immunosuppressed individuals warrant the search for a safer vector in the following clinic trails. In this study, we deleted the C7L and K1L genes of VTT and constructed six recombinant vaccinia strains VTT△C7L, VTT△K1L, VTT△C7LK1L, VTKgpe△C7L, VTKgpe△K1L and VTT△C7LK1L-gag. The pathogenicity and immunogenicity of these recombinants were evaluated in mouse and rabbit models. Comparing to parental VTT, VTT△C7L and VTT△K1L showed significantly decreased replication capability in CEF, Vero, BHK-21 and HeLa cell lines. In particular, replication of VTT△C7LK1L decreased more than 10-fold in all four cell lines. The virulence of all these mutants were decreased in BALB/c mouse and rabbit models; VTT△C7LK1L once again showed the greatest attenuation, having resulted in no evident damage in mice and erythema of only 0.4 cm diameter in rabbits, compared to 1.48 cm for VTT. VTKgpe△C7L, VTKgpe△K1L and VTT△C7LK1L-gag elicited as strong cellular and humoral responses against HIV genes as did VTKgpe, while humoral immune response against the vaccinia itself was reduced by 4-8-fold. These data show that deletion of C7L and K1L genes leads to significantly decreased virulence without compromising animal host immunogenicity, and may thus be key to creating a more safe and effective HIV vaccine vector.

摘要

天坛痘苗病毒(VTT)已被中国作为 HIV 疫苗载体进行了修饰,在免疫原性和安全性方面表现出色。然而,其在免疫抑制个体中的不良反应需要在后续临床试验中寻找更安全的载体。在这项研究中,我们删除了 VTT 的 C7L 和 K1L 基因,并构建了六个重组痘苗菌株 VTT△C7L、VTT△K1L、VTT△C7LK1L、VTKgpe△C7L、VTKgpe△K1L 和 VTT△C7LK1L-gag。我们在小鼠和兔模型中评估了这些重组体的致病性和免疫原性。与亲本 VTT 相比,VTT△C7L 和 VTT△K1L 在 CEF、Vero、BHK-21 和 HeLa 细胞系中的复制能力显著降低。特别是,VTT△C7LK1L 在所有四个细胞系中的复制能力降低了 10 倍以上。这些突变体在 BALB/c 小鼠和兔模型中的毒力均降低;VTT△C7LK1L 再次显示出最大的衰减,在小鼠中没有明显的损伤,而在兔子中仅出现 0.4cm 直径的红斑,而 VTT 则为 1.48cm。VTKgpe△C7L、VTKgpe△K1L 和 VTT△C7LK1L-gag 诱导的针对 HIV 基因的细胞和体液免疫反应与 VTKgpe 一样强,而针对痘苗自身的体液免疫反应则降低了 4-8 倍。这些数据表明,删除 C7L 和 K1L 基因可显著降低毒力而不影响动物宿主的免疫原性,因此可能是创建更安全有效的 HIV 疫苗载体的关键。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5c26/3698190/744905fc9504/pone.0068115.g001.jpg

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