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In Vitro Effect of Rifampin on Mycobacteria

机译:利福平对分枝杆菌的体外作用

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Rifampin inhibited 20 strains of Mycobacterium tuberculosis in concentrations of 0.005 to 0.02 μg/ml in 7H-9 broth with Tween 80 and killed all or nearly all of the inoculum in four to eight times greater concentrations. In the same medium without Tween 80, as well as on 7H-10 agar, about 16 to 64 times these amounts were required to produce the same effect. Rifampin was also active against M. kansasii and some of the nonchromogenic mycobacteria. The incidence of mycobacterial cells resistant to rifampin within the cultures studied was in the range of one to four per 108 to 109 colony-forming units with concentrations of 4 to 125 μg of rifampin per ml. Only one of the Battey cultures and that of M. fortuitum yielded cells resistant to rifampin at 125 μg/ml but not at 500 μg/ml. The same strains yielded more than double that number of organisms resistant to streptomycin and up to 100 times more organisms resistant to isoniazid. All three drugs stopped the growth or reduced the mycobacterial population in growing cultures after contact for 24 to 48 hr. Complete inhibition of growth was produced by rifampin at 1.0 μg/ml in an average of 6 days and by streptomycin at 5.0 μg/ml in 3 days. After an average contact of 10.7 days with rifampin, five of seven strains resumed growth and all strains began regrowth after exposure to streptomycin for 9.4 days. The marked susceptibility of M. tuberculosis and of atypical mycobacteria to rifampin in vitro and the relatively low incidence of resistant mutants suggests that this agent may have clinical usefulness in the treatment of tuberculosis and some other mycobacterioses.
机译:利福平在7H-9肉汤中用Tween 80抑制浓度为0.005至0.02μg/ ml的20株结核分枝杆菌,并以四到八倍的浓度杀死所有或几乎所有接种物。在没有Tween 80的相同培养基中,以及在7H-10琼脂上,需要约16至64倍的这些量才能产生相同的效果。利福平还对堪萨斯分枝杆菌和某些非生色分枝杆菌具有活性。在研究的培养物中,对利福平具有抗性的分枝杆菌细胞的发生率为每108至109个菌落形成单位1至4个,浓度为每毫升4至125μg利福平。仅有一种Battey培养物和Fort M. fortuitum产生的细胞对利福平具有抗性,浓度为125μg/ ml,但对500μg/ ml无效。相同的菌株产生的抗链霉素生物数量是其两倍以上,而抗异烟肼的生物数量则高达100倍以上。接触24至48小时后,所有三种药物均停止生长或减少生长中培养物中的分枝杆菌种群。在平均6天内,以1.0μg/ ml的利福平和在3天内以5.0μg/ ml的链霉素产生对生长的完全抑制。与利福平平均接触10.7天后,七个菌株中的五个恢复了生长,所有菌株在暴露于链霉素9.4天后开始再生长。结核分枝杆菌和非典型分枝杆菌在体外对利福平具有明显的敏感性,并且耐药突变体的发生率相对较低,表明该药物在治疗结核病和其他分枝杆菌中可能具有临床价值。

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