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首页> 美国卫生研究院文献>Elsevier Public Health Emergency Collection >A Novel Therapeutic and Prophylactic Vaccine (HVJ-Envelope / Hsp65 DNA + IL-12 DNA) against Tuberculosis Using the Cynomolgus Monkey Model
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A Novel Therapeutic and Prophylactic Vaccine (HVJ-Envelope / Hsp65 DNA + IL-12 DNA) against Tuberculosis Using the Cynomolgus Monkey Model

机译:使用食蟹猴模型的新型结核病治疗和预防性疫苗(HVJ-信封/ Hsp65 DNA + IL-12 DNA)

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We have developed a novel tuberculosis (TB) vaccine; a combination of the DNA vaccines expressing mycobacterial heat shock protein 65 (HSP65) and interleukin 12 (IL-12) delivered by the hemagglutinating virus of Japan (HVJ)-envelope and –liposome (HSP65 + IL-12/HVJ). An IL-12 expression vector (IL-12DNA) encoding single-chain IL-12 proteins comprised of p40 and p35 subunits were constructed. This vaccine provided remarkable protective efficacy in mouse and guinea pig models compared to the BCG vaccine on the basis of C.F.U of number of TB, survival, an induction of the CD8 positive CTL activity and improvement of the histopathological tuberculosis lesions. This vaccine also provided therapeutic efficacy against multi-drug resistant TB (MDR-TB) and extremely drug resistant TB (XDR-TB) (prolongation of survival time and the decrease in the number of TB in the lung) in murine models. Furthermore, we extended our studies to a cynomolgus monkey model, which is currently the best animal model of human tuberculosis. This novel vaccine provided a higher level of the protective efficacy than BCG based upon the assessment of mortality, the ESR, body weight, chest X-ray findings and immune responses. All monkeys in the control group (saline) died within 8 months, while 50% of monkeys in the HSP65+hIL-12/HVJ group survived more than 14 months post-infection (the termination period of the experiment). Furthermore, the BCG priming and HSP65 + IL-12/HVJ vaccine (booster) by the priming-booster method showed a synergistic effect in the TB-infected cynomolgus monkey (100% survival). In contrast, 33% of monkeys from BCG Tokyo alone group were alive (33% survival). Furthermore, this vaccine exerted therapeutic efficacy (100% survival) and augmentation of immune responses in the TB-infected monkeys. These data indicate that our novel DNA vaccine might be useful against including XDR-TB and MDR-TB for human therapeutic clinical trials.
机译:我们已经开发了一种新型的结核病(TB)疫苗;由日本血凝病毒(HVJ)包膜和–脂质体(HSP65 + IL-12 / HVJ)递送的表达分枝杆菌热休克蛋白65(HSP65)和白介素12(IL-12)的DNA疫苗的组合。构建了一个IL-12表达载体(IL-12DNA),该载体编码由p40和p35亚基组成的单链IL-12蛋白。与BCG疫苗相比,根据TB的C.F.U,存活率,CD8阳性CTL活性的诱导以及组织病理学肺结核病的改善,该疫苗在小鼠和豚鼠模型中提供了显着的保护功效。该疫苗还在鼠类模型中提供了针对多药耐药结核病(MDR-TB)和极耐药菌结核病(XDR-TB)的治疗功效(延长生存时间,减少肺结核病数量)。此外,我们将研究扩展到食蟹猴模型,这是目前人类结核病的最佳动物模型。根据死亡率,ESR,体重,胸部X线检查结果和免疫反应的评估,这种新型疫苗提供的保护功效比BCG更高。对照组(盐水)中的所有猴子在8个月内死亡,而HSP65 + hIL-12 / HVJ组中的50%的猴子在感染后(实验终止期)超过14个月存活。此外,BCG初免和HSP65 + IL-12 / HVJ疫苗(初免-加强型方法)在结核病感染的食蟹猴中表现出协同效应(100%存活率)。相比之下,仅来自BCG Tokyo组的猴子就有33%存活(存活率33%)。此外,这种疫苗在感染结核病的猴子中发挥了治疗功效(100%存活)并增强了免疫反应。这些数据表明,我们的新型DNA疫苗可能有益于将XDR-TB和MDR-TB用于人体治疗性临床试验。

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