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Vaccines Displaying Mycobacterial Proteins on Biopolyester Beads Stimulate Cellular Immunity and Induce Protection against Tuberculosis

机译:在生物聚酯微珠上显示分枝杆菌蛋白的疫苗可刺激细胞免疫并诱导抗结核保护

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摘要

New improved vaccines are needed for control of both bovine and human tuberculosis. Tuberculosis protein vaccines have advantages with regard to safety and ease of manufacture, but efficacy against tuberculosis has been difficult to achieve. Protective cellular immune responses can be preferentially induced when antigens are displayed on small particles. In this study, Escherichia coli and Lactococcus lactis were engineered to produce spherical polyhydroxybutyrate (PHB) inclusions which displayed a fusion protein of Mycobacterium tuberculosis, antigen 85A (Ag85A)–early secreted antigenic target 6-kDa protein (ESAT-6). L. lactis was chosen as a possible production host due its extensive use in the food industry and reduced risk of lipopolysaccharide contamination. Mice were vaccinated with PHB bead vaccines with or without displaying Ag85A–ESAT-6, recombinant Ag85A–ESAT-6, or M. bovis BCG. Separate groups of mice were used to measure immune responses and assess protection against an aerosol M. bovis challenge. Increased amounts of antigen-specific gamma interferon, interleukin-17A (IL-17A), IL-6, and tumor necrosis factor alpha were produced from splenocytes postvaccination, but no or minimal IL-4, IL-5, or IL-10 was produced, indicating Th1- and Th17-biased T cell responses. Decreased lung bacterial counts and less extensive foci of inflammation were observed in lungs of mice receiving BCG or PHB bead vaccines displaying Ag85A–ESAT-6 produced in either E. coli or L. lactis compared to those observed in the lungs of phosphate-buffered saline-treated control mice. No differences between those receiving wild-type PHB beads and those receiving recombinant Ag85A–ESAT-6 were observed. This versatile particulate vaccine delivery system incorporates a relatively simple production process using safe bacteria, and the results show that it is an effective delivery system for a tuberculosis protein vaccine.
机译:需要新的改良疫苗来控制牛和人结核病。结核蛋白疫苗在安全性和易于制造方面具有优势,但是很难获得抗结核的功效。当抗原显示在小颗粒上时,可以优先诱导保护性细胞免疫反应。在这项研究中,对大肠杆菌和乳酸乳球菌进行了工程改造,以产生球形多羟基丁酸酯(PHB)内含物,该内含物显示出结核分枝杆菌的融合蛋白,抗原85A(Ag85A)–早期分泌的抗原靶标6-kDa蛋白(ESAT-6)。选择乳酸乳球菌作为可能的生产宿主,因为其在食品工业中的广泛使用和降低了脂多糖污染的风险。用具有或不具有Ag85A–ESAT-6,重组Ag85A–ESAT-6或牛分枝杆菌BCG的PHB珠状疫苗接种小鼠。将单独的小鼠组用于测量免疫应答和评估针对气溶胶牛分枝杆菌攻击的保护。接种疫苗后的脾细胞产生的抗原特异性伽马干扰素,白介素17A(IL-17A),IL-6和肿瘤坏死因子α的数量增加,但没有或仅有极少量的IL-4,IL-5或IL-10产生。产生,表明Th1和Th17偏向T细胞反应。与磷酸盐缓冲盐水肺部观察到的相比,接受BCG或PHB珠状疫苗接种的小鼠的肺部细菌计数降低,发炎范围较小,显示出在大肠杆菌或乳酸乳球菌中产生的Ag85A–ESAT-6疫苗。治疗的对照小鼠。接受野生型PHB珠的人与接受重组Ag85A–ESAT-6的人之间没有观察到差异。这种通用的颗粒疫苗输送系统结合了使用安全细菌的相对简单的生产过程,结果表明,它是用于结核蛋白疫苗的有效输送系统。

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