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A Multi-Antigenic Adenoviral-Vectored Vaccine Improves BCG-Induced Protection of Goats against Pulmonary Tuberculosis Infection and Prevents Disease Progression

机译:一种多抗原腺病毒载体疫苗可提高BCG诱导的山羊对肺结核感染的保护并预防疾病进展。

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摘要

The “One world, one health” initiative emphasizes the need for new strategies to control human and animal tuberculosis (TB) based on their shared interface. A good example would be the development of novel universal vaccines against Mycobacterium tuberculosis complex (MTBC) infection. This study uses the goat model, a natural TB host, to assess the protective effectiveness of a new vaccine candidate in combination with Bacillus Calmette-Guerin (BCG) vaccine.Thirty-three goat kids were divided in three groups: Group 1) vaccinated with BCG (week 0), Group 2) vaccinated with BCG and boosted 8 weeks later with a recombinant adenovirus expressing the MTBC antigens Ag85A, TB10.4, TB9.8 and Acr2 (AdTBF), and Group 3) unvaccinated controls. Later on, an endobronchial challenge with a low dose of M. caprae was performed (week 15). After necropsy (week 28), the pulmonary gross pathology was quantified using high resolution Computed Tomography. Small granulomatous pulmonary lesions (< 0.5 cm diameter) were also evaluated through a comprehensive qualitative histopathological analysis. M. caprae CFU were counted from pulmonary lymph nodes.The AdTBF improved the effects of BCG reducing gross lesion volume and bacterial load, as well as increasing weight gain. The number of Ag85A-specific gamma interferon-producing memory T-cells was identified as a predictor of vaccine efficacy. Specific cellular and humoral responses were measured throughout the 13-week post-challenge period, and correlated with the severity of lesions.Unvaccinated goats exhibited the typical pathological features of active TB in humans and domestic ruminants, while vaccinated goats showed only very small lesions. The data presented in this study indicate that multi-antigenic adenoviral vectored vaccines boosts protection conferred by vaccination with BCG.
机译:“一个世界,一个健康”倡议强调需要基于其共享界面来控制人类和动物结核病的新策略。一个很好的例子是开发针对结核分枝杆菌复合物(MTBC)感染的新型通用疫苗。本研究使用天然结核病宿主山羊模型评估卡介苗芽孢杆菌(BCG)疫苗与新型候选疫苗的保护效果.33例山羊儿童分为三组:第一组接种BCG(第0周,第2组)接种了BCG,并在8周后用表达MTBC抗原Ag85A,TB10.4,TB9.8和Acr2(AdTBF)的重组腺病毒加强免疫,第3组未接种对照。后来,进行了低剂量卡普拉斯分枝杆菌的支气管内攻击(第15周)。尸检后(第28周),使用高分辨率计算机断层扫描对肺部总体病理进行定量。还通过全面的定性组织病理学分析评估了小的肉芽肿性肺部病变(直径<0.5 cm)。从肺淋巴结中计数出capraeCFU。AdTBF改善了BCG减少总病变体积和细菌载量以及增加体重的效果。 Ag85A特异性产生γ干扰素的记忆T细胞的数量被确定为疫苗效力的预测指标。在攻击后的整个13周内测量特定的细胞和体液反应,并与病变的严重程度相关。未接种山羊表现出人类和家庭反刍动物活动性TB的典型病理特征,而接种山羊仅表现出很小的病变。这项研究中提供的数据表明,多抗原腺病毒载体疫苗增强了卡介苗接种所赋予的保护作用。

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