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Virulence and drug susceptibility of Mycobacterium celatum

机译:分枝杆菌的毒力和药物易感性

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The virulence and drug susceptibility of a clinical isolate of Mycobacterium celatum which showed smooth transparent (ST) and smooth opaque (SO) colonies were studied. While ST cells multiplied intracellularly and maintained their coccobacillary form in a human macrophage model of infection, SO cells formed long filaments and completely destroyed the phagocytes. In BALB/c mice, the ST variant, but not the SO variant, grew efficiently in the spleen, liver and lung. The ST variant was usually more resistant in vitro than the SO variant to drugs, with MIC values for clarithromycin (CLA), azithromycin (AZI), ciprofloxacin, sparfloxacin, amikacin, clofazimine, ethambutol and isoniazid being higher than those of the SO variant. In beige mice infected with the more highly virulent variant ST, CLA and AZI were the most active drugs in terms of viable count reduction in organs and mutant selection. Together, these observations indicate that the ST variant of M. celatum is a virulent form that can be efficiently inhibited in vivo by CLA and AZI.
机译:研究了分枝杆菌的临床分离物的毒力和药物易感性,其显示出光滑透明(ST)和光滑的不透明(SO)菌落。虽然ST细胞在感染的人巨噬细胞模型中乘以细胞内并保持其茧形式,因此细胞形成长丝并完全摧毁吞噬细胞。在Balb / c小鼠中,ST变体,但不是那么变体,在脾脏,肝脏和肺部有效地增长。在体外,ST变体通常比如此变体对药物更耐药,具有克拉霉素(CLA),阿奇霉素(AZI),环丙沙星,斯芬氟吡喃,Amikacin,Clofazimine,乙胺丁醇和异烟肼高于如此变体的麦克风。在感染米的米色小鼠中,感染了更高的毒性变异ST,Cla和Azi在可行的计数减少的器官和突变选择方面是最活跃的药物。这些观察结果表明,M. Castum的ST变体是一种毒力形式,可以通过CLA和AZI有效地抑制体内。

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