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Enhanced mortality despite control of lung infection in mice aerogenically infected with a Mycobacterium tuberculosis mce1 operon mutant

机译:尽管控制了肺结核分枝杆菌mce1操纵子突变体的小鼠被肺部感染但死亡率增加

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摘要

Mycobacterium tuberculosis causes a variety of host clinical outcomes. We previously showed that M. tuberculosis disrupted in an operon called mce1 proliferates unchecked in BALB/c mouse lungs. The observed outcome could be attributed either to the mutant bacterial burden or to the host immunopathologic response. To differentiate these possibilities, we studied the outcomes of infection in a mouse strain less susceptible to M. tuberculosis than BALB/c--C57BL/6. We found that the mutant infection reached a plateau in the lungs at a rate similar to that of the wild type. All mice infected with the mutant, but only half of the groups of mice infected with the wild type or complemented strain, died by 40 weeks (p<0.05). At 12–21 weeks of infection, histological examination of the lungs of mice infected with the mutant showed a diffuse pattern of lymphocyte infiltration, while that of mice infected with the other strains exhibited a nodular cellular infiltration pattern. Surprisingly, the number of bacilli recovered from the lungs was similar in all three groups. These observations suggest that rather than the bacterial burden, products of the mce1 operon may directly or indirectly modulate the host immune response that is protective to both the tubercle bacilli and the host.
机译:结核分枝杆菌引起多种宿主临床结果。我们以前显示结核杆菌在一个称为mce1的操纵子中被破坏,在BALB / c小鼠肺中未经检查而增殖。观察到的结果可能归因于突变的细菌负担或宿主的免疫病理反应。为了区分这些可能性,我们研究了比BALB / c-C57BL / 6更不易感染结核分枝杆菌的小鼠品系的感染结果。我们发现突变体感染以与野生型相似的速率到达肺的平稳期。所有感染了该突变体的小鼠,但只有一半感染野生型或互补菌株的小鼠死亡了40周(p <0.05)。在感染的第12-21周时,感染该突变体的小鼠的肺组织学检查显示出淋巴细胞浸润的弥散模式,而感染其他菌株的小鼠则显示出结节性细胞浸润模式。令人惊讶的是,在所有三个组中,从肺中回收的细菌数量均相似。这些观察结果表明,mce1操纵子的产物可直接或间接调节宿主免疫应答,从而保护结核杆菌和宿主,而不是细菌负担。

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