肺炎链球菌对利福平的低水平耐药性。
Low-level resistance to rifampin in Streptococcus pneumoniae.
作者信息
Meier Patricia Stutzmann, Utz Silvia, Aebi Suzanne, Mühlemann Kathrin
机构信息
Institute for Infectious Diseases, University of Bern, University Hospital Bern, Switzerland.
出版信息
Antimicrob Agents Chemother. 2003 Mar;47(3):863-8. doi: 10.1128/AAC.47.3.863-868.2003.
Rifampin is recommended for combination therapy of meningitis due to beta-lactam-resistant Streptococcus pneumoniae. High-level rifampin resistance (MIC, > or =4 mg/liter) has been mapped to point mutations in clusters I and III of rpoB of the pneumococcus. The molecular basis of low-level resistance (MICs, > or =0.5 and <4 mg/liter) was analyzed. Spontaneous mutants of clinical pneumococcal isolates were selected on Columbia sheep blood agar plates containing rifampin at 0.5, 4, 10, or 50 mg/liter. Low-level resistance could be assigned to mutations in cluster II (I(545)N, I(545)L). Sensitive (MIC, <0.048 mg/liter) wild-type strains acquired low-level resistance at a rate approximately 10 times higher than that at which they acquired high-level resistance (average mutation frequencies, 2.4 x 10(-7) for low-level resistance versus 2.9 x 10(-8) for high-level resistance [P < 0.0001]). In second-step experiments, the frequencies of mutations from low- to high-level resistance were over 10 times higher than the frequencies of mutations from susceptibility to high-level resistance (average mutation frequencies, 7.2 x 10(-7) versus 5.0 x 10(-8) [P < 0.001]). Mutants with low-level resistance were stable upon passage. Sequencing of a clinical isolate with low-level resistance (MIC, 0.5 mg/liter) revealed a Q(150)R mutation upstream of cluster I. The frequencies of mutations to high-level resistance for this strain were even higher than the rates observed for the in vitro mutants. Therefore, a resistance-mediating mutation located outside clusters I, II, and III has been described for the first time in the pneumococcus. In vitro low-level rifampin resistance in S. pneumoniae could be mapped to cluster II of rpoB. Mutants of pneumococcus with low-level resistance may be selected in vivo during therapy in tissue compartments with low antibiotic concentrations and play a role in the development of resistance.
利福平推荐用于耐β-内酰胺类肺炎链球菌所致脑膜炎的联合治疗。高水平利福平耐药(最低抑菌浓度[MIC]≥4毫克/升)已被定位到肺炎链球菌rpoB基因第一和第三簇的点突变。分析了低水平耐药(MIC≥0.5且<4毫克/升)的分子基础。在含0.5、4、10或50毫克/升利福平的哥伦比亚绵羊血琼脂平板上筛选临床肺炎链球菌分离株的自发突变体。低水平耐药可归因于第二簇的突变(I(545)N、I(545)L)。敏感(MIC<0.048毫克/升)野生型菌株获得低水平耐药的速率比获得高水平耐药的速率高约10倍(平均突变频率,低水平耐药为2.4×10⁻⁷,高水平耐药为2.9×10⁻⁸[P<0.0001])。在第二步实验中,从低水平耐药突变为高水平耐药的频率比从敏感突变为高水平耐药的频率高10倍以上(平均突变频率,7.2×10⁻⁷对5.0×10⁻⁸[P<0.001])。低水平耐药突变体传代后稳定。对一株低水平耐药(MIC为0.5毫克/升)的临床分离株进行测序,发现在第一簇上游有一个Q(150)R突变。该菌株突变为高水平耐药的频率甚至高于体外突变体观察到的速率。因此,首次在肺炎链球菌中描述了位于第一、第二和第三簇之外的耐药介导突变。肺炎链球菌体外低水平利福平耐药可定位到rpoB基因的第二簇。低水平耐药的肺炎链球菌突变体可能在抗生素浓度低的组织腔室治疗期间在体内被选择,并在耐药性发展中起作用。
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