首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Expression levels of Mycobacterium tuberculosis antigen-encoding genes versus production levels of antigen-specific T cells during stationary level lung infection in mice.
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Expression levels of Mycobacterium tuberculosis antigen-encoding genes versus production levels of antigen-specific T cells during stationary level lung infection in mice.

机译:小鼠固定水平肺部感染期间结核分枝杆菌抗原编码基因的表达水平与抗原特异性T细胞的产生水平。

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Mycobacterium tuberculosis lung infection in mice was controlled at an approximately stationary level after 20 days of log linear growth. Onset of stationary level infection was associated with the generation by the host of T helper type 1 (Th1) immunity, as evidenced by the accumulation of CD4 Th1 cells specific for the early secretory antigen (ESAT-6) of M. tuberculosis encoded by esat6, and for a mycolyl transferase (Ag85B) encoded by fbpB. CD4 T cells specific for these antigens were maintained at relatively high numbers throughout the course of infection. The number of CD4 T cells generated against ESAT-6 was larger than the number generated against Ag85B, and this was associated with a higher transcription level of esat6. The total number of transcripts of esat6 increased during the first 15 days of infection, after which it decreased and then approximately stabilized at 10(6.5) per lung. The total number of fbpB transcripts increased for 20 days of infection before decreasing and then approximately stabilizing at 10(4.8) per lung. The number of transcripts of esat6 per colony-forming unit of M. tuberculosis fell from 8.6 to 0.8 after day 15, and of fbpB from 0.3 to less than 0.02 after day 10, suggesting that at any given time during stationary level infection the latter gene was expressed by a very small percentage of bacilli. Expressed at an even lower level was an M. tuberculosis replication gene involved in septum formation (ftsZ), indicating that there was no significant turnover of the M. tuberculosis population during stationary level infection.
机译:对数线性增长20天后,将小鼠结核分枝杆菌的肺部感染控制在大约静止的水平。固定水平感染的发作与T辅助1型(Th1)免疫宿主的产生有关,这由esat6编码的结核分枝杆菌的早期分泌性抗原(ESAT-6)特异的CD4 Th1细胞积累所证明。 ,以及由fbpB编码的霉菌基转移酶(Ag85B)。在整个感染过程中,对这些抗原特异的CD4 T细胞保持相对较高的数量。针对ESAT-6生成的CD4 T细胞数量大于针对Ag85B生成的CD4 T细胞数量,这与esat6的更高转录水平相关。 esat6的转录本总数在感染的前15天中增加,此后下降,然后稳定在每个肺10(6.5)。在感染前20天,fbpB转录物总数增加,然后下降,然后稳定在每肺10(4.8)。第15天后,结核分枝杆菌每个菌落形成单位esat6的转录物数量从8.6降至0.8,而第10天后fbpB的转录物数量从0.3降至0.02以下,表明在静止水平感染的任何给定时间,后者基因用很小比例的细菌表达。表达甚至更低的是参与间隔形成(ftsZ)的结核分枝杆菌复制基因,表明在稳定水平的感染过程中结核分枝杆菌种群没有明显的更新。

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