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首页> 外文期刊>Microbial Pathogenesis >Paradigm redux Mycobacterium avium subspecies paratuberculosis-macrophage interactions show clear variations between bovine and human physiological body temperatures.
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Paradigm redux Mycobacterium avium subspecies paratuberculosis-macrophage interactions show clear variations between bovine and human physiological body temperatures.

机译:范例范型鸟分枝杆菌亚种副结核与巨噬细胞的相互作用显示出牛与人的生理体温之间的明显差异。

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The physiological conditions encountered by pathogenic mycobacteria inside their hosts significantly influence their adaptation, virulence, and gene expression. Current in vitro models investigating host-pathogen interactions of Mycobacterium avium subsp. paratuberculosis use 37 degrees C, the normal body temperatures of mice and humans. However since the physiological temperature of MAP's natural host is 39 degrees C, we hypothesized that host and pathogen behavior to vary considerably in comparison to 37 degrees C. Our MAP-macrophage interaction studies show striking differences in regards to velocity of cell invasion of MAP as well as bacterial and host gene regulation at 39 degrees C compared with 37 degrees C. Upregulation of host genes (nod2, tlr2, mapkp38 and il-10) follow a similar trend at 37 degrees C and 39 degrees C; however, there is over a five-fold increase as early as 0.5 and 2 h in 39 degrees C treatments. While host signaling is completed by 48 h p.i. at 39 degrees C in MDMs cultures due to early cell death, signaling and infection is sustained at 37 degrees C. Surprisingly, transcription of MAP genes did not show a set pattern and were upregulated at different time points for both temperatures. Interestingly, MAP genes encoding a lipase (lipN) and an oxidoreductase (MAP3464) are staggered at 39 degrees C, while they increase steadily at 37 degrees C. In conclusion, infection and culture at a physiologically relevant temperature influences host-pathogen interaction, which may have far reaching ramifications including for currently used animal models, in vitro culture methods, bacterial pathogenesis and host responses, and vaccine candidate design and screening.
机译:寄主内的致病性分枝杆菌遇到的生理条件会显着影响其适应性,毒力和基因表达。当前体外模型研究鸟分枝杆菌亚种的宿主-病原体相互作用。副结核病使用37摄氏度,小鼠和人类的正常体温。但是,由于MAP天然宿主的生理温度为39摄氏度,因此我们假设宿主和病原体的行为与37摄氏度相比有很大差异。我们的MAP-巨噬细胞相互作用研究显示,在MAP的细胞侵袭速度方面存在显着差异以及细菌和宿主基因在39摄氏度(37摄氏度)下的调控。宿主基因(nod2,tlr2,mapkp38和il-10)的上调在37摄氏度和39摄氏度下遵循相似的趋势;但是,在39摄氏度的处理中,最早在0.5和2小时时增加了五倍。主机信号在48小时p.i之前完成。由于早期细胞死亡,在39°C的MDMs培养物中,信号传导和感染在37°C持续。令人惊讶的是,MAP基因的转录没有显示出固定的模式,并且在两个温度的不同时间点均被上调。有趣的是,编码脂肪酶(lipN)和氧化还原酶(MAP3464)的MAP基因在39°C时错开,而在37°C时则稳定增加。总而言之,在生理相关温度下的感染和培养会影响宿主与病原体的相互作用。可能会产生深远的影响,包括当前使用的动物模型,体外培养方法,细菌发病机理和宿主反应以及候选疫苗的设计和筛选。

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