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Screening of Mycobacterium avium subsp. paratuberculosis mutants for attenuation in a bovine monocyte-derived macrophage model

机译:鸟分枝杆菌亚种的筛选。牛单核细胞衍生的巨噬细胞模型中用于减毒的肺结核旁突变体

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摘要

Vaccination remains a major tool for prevention and progression of Johne's disease, a chronic enteritis of ruminants worldwide. Currently there is only one licensed vaccine within the United States and two vaccines licensed internationally against Johne's disease. All licensed vaccines reduce fecal shedding of Mycobacterium avium subsp. paratuberculosis (MAP) and delay disease progression. However, there are no available vaccines that prevent disease onset. A joint effort by the Johne's Disease Integrated Program (JDIP), a USDA-funded consortium, and USDA—APHIS/VS sought to identify transposon insertion mutant strains as vaccine candidates in part of a three phase study. The focus of the Phase I study was to evaluate MAP mutant attenuation in a well-defined in vitro bovine monocyte-derived macrophage (MDM) model. Attenuation was determined by colony forming unit (CFUs) counts and slope estimates. Based on CFU counts alone, the MDM model did not identify any mutant that significantly differed from the wild-type control, MAP K-10. Slope estimates using mixed models approach identified six mutants as being attenuated. These were enrolled in protection studies involving murine and baby goat vaccination-challenge models. MDM based approach identified trends in attenuation but this did not correlate with protection in a natural host model. These results suggest the need for alternative strategies for Johne's disease vaccine candidate screening and evaluation.
机译:疫苗接种仍然是预防和发展约翰内氏病的主要工具,该病是全世界反刍动物的慢性肠炎。目前,在美国只有一种许可的疫苗,而在国际上有两种针对约翰氏病的许可疫苗。所有获得许可的疫苗都可减少禽分枝杆菌亚种的粪便脱落。副结核病(MAP)和疾病延误。但是,没有可用的预防疾病发作的疫苗。由美国农业部资助的约翰内氏病综合计划(JDIP)和USDA-APHIS / VS共同努力,在三阶段研究的一部分中寻求确定转座子插入突变株作为候选疫苗。 I期研究的重点是在定义明确的体外牛单核细胞衍生巨噬细胞(MDM)模型中评估MAP突变体的衰减。衰减通过菌落形成单位(CFU)计数和斜率估计值确定。仅基于CFU计数,MDM模型未发现任何与野生型对照MAP K-10明显不同的突变体。使用混合模型方法的斜率估计确定了六个突变体被减弱。这些被纳入了涉及鼠类和小山羊疫苗接种挑战模型的保护研究。基于MDM的方法确定了衰减趋势,但这与自然宿主模型中的保护无关。这些结果表明,有必要采用其他策略来筛选和评估约翰尼氏病疫苗候选者。

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