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基于病毒样颗粒疫苗的肠道病毒 71 高效表达。

Efficient expression of enterovirus 71 based on virus-like particles vaccine.

机构信息

Division of Vaccine Research, Center for Infectious Diseases, Korea National Institutes of Health, Korea Centers for Disease Control and Prevention, Osong-eup, Cheongju, Chungcheongbuk-do, Republic of Korea.

Division of Strategic Planning for Emerging Infectious Disease, Centers for Disease Control and Prevention, Osong, CheongJu, Chungcheongbuk-do, South Korea.

出版信息

PLoS One. 2019 Mar 7;14(3):e0210477. doi: 10.1371/journal.pone.0210477. eCollection 2019.

Abstract

Enterovirus (EV) 71 is the main pathogen associated with hand-foot-mouth disease (HFMD) and can lead to the disease with severe mortality in children. Since 2009, in the Republic of Korea, an outbreak of EV71 C4a infection with neurologic involvement emerged, where in HFMD involvement was identified and central nervous system complications were reported. In this study, EV71 C4a virus-like particles (VLPs) produced by recombinant technology were generated in a baculovirus expression system. To improve the production yield, EV71 VLP was constructed using the dual promoter system baculovirus P1 and 3CD (baculo-P1-3CD), which harbored both the structural protein-encoding P1 region under the control of the polyhedron promoter and the 3CD protease gene under the regulation of the CMV-IE, lef3, gp41, or chitinase promoters to augment the level of gene transcription. Efficient VLP expression was demonstrated through optimization of incubation time and insect cell type. In addition, to evaluate the potential of VLP as a vaccine candidate, we tested the neutralizing antibodies and total anti-EV71 IgG from the purified EV71 C4a VLP serum. The recombinant EV71 VLP exhibited the morphology of self-assembled VLP, as determined by electron microscopy. Use of baculo-P1-3CD-gp41 led to a high yield (11.3mg/L < 40kDa) of VLPs in High-FiveTM cells at 3 days post-infection. Furthermore, the potential of VLP as a vaccine was evaluated through the neutralizing ability elicited by the purified EV71 VLP after immunization of BALB/c mice, which was shown to induce potent and long-lasting humoral immune responses as evidenced by the cross-neutralization titer. Our results could be used to expedite the developmental process for vaccines under clinical trials and to ensure manufacturing consistency for licensing requirements.

摘要

肠道病毒 71 型(EV71)是手足口病(HFMD)的主要病原体,可导致儿童发病死亡率较高。自 2009 年以来,在韩国出现了一种与神经系统受累有关的 EV71 C4a 感染爆发,在手足口病中已确定存在这种感染,并报告了中枢神经系统并发症。在这项研究中,使用重组技术在杆状病毒表达系统中产生了 EV71 C4a 病毒样颗粒(VLPs)。为了提高产量,使用杆状病毒 P1 和 3CD(baculo-P1-3CD)的双启动子系统构建了 EV71 VLP,其中结构蛋白编码 P1 区受多角体启动子控制,3CD 蛋白酶基因受 CMV-IE、lef3、gp41 或几丁质酶启动子调控,以增加基因转录水平。通过优化孵育时间和昆虫细胞类型,证明了高效的 VLP 表达。此外,为了评估 VLP 作为候选疫苗的潜力,我们测试了从纯化的 EV71 C4a VLP 血清中获得的中和抗体和总抗-EV71 IgG。电子显微镜观察结果表明,重组 EV71 VLP 呈现出自我组装 VLP 的形态。使用 baculo-P1-3CD-gp41 在感染后 3 天可在 High-FiveTM 细胞中获得 11.3mg/L<40kDa 的高产量 VLPs。此外,通过 BALB/c 小鼠免疫后纯化的 EV71 VLP 诱导的中和能力评估了 VLP 作为疫苗的潜力,结果表明,交叉中和效价证明了其诱导强大且持久的体液免疫应答的能力。我们的结果可用于加速临床试验中的疫苗开发过程,并确保符合许可要求的生产一致性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dc79/6405078/f72e8ac182e5/pone.0210477.g001.jpg

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