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首页> 外文期刊>Journal of Clinical Microbiology >Characterization of Multidrug-Resistant Typhoid Outbreaks in Kenya
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Characterization of Multidrug-Resistant Typhoid Outbreaks in Kenya

机译:肯尼亚耐多药性伤寒暴发的特征

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We characterized by antibiotic susceptibility, plasmid analysis, incompatibility grouping, and pulsed-field gel electrophoresis (PFGE) of XbaI- and SpeI-digested DNA 102 Salmonella enterica serovar Typhi (serovar Typhi) isolated from recent outbreaks of typhoid in three different parts of Kenya. Only 13.7% were fully susceptible, whereas another 82.4% were resistant to each of the five commonly available drugs: ampicillin, chloramphenicol, and tetracycline (MICs of >256 μg/ml); streptomycin (MIC, >1,024 μg/ml); and cotrimoxazole (MIC of >32 μg/ml). Resistance to these antibiotics was encoded on a 110-kb self-transferable plasmid of IncHI1 incompatibility group. The MICs of nalidixic acid (MIC, 8 to 16 μg/ml) and ciprofloxacin (MIC of 0.25 to 0.38 μg/ml) for 41.7% of the 102 serovar Typhi isolates were 5- and 10-fold higher, respectively, than for sensitive strains. Amplification by PCR and sequencing of the genes coding for gyrase (gyrA and gyrB) and topoisomerase IV (parE and parC) within the quinolone resistance-determining region revealed that the increase in the MICs of the quinolones had not resulted from any significant mutation. Analysis of genomic DNA from both antimicrobial agent-sensitive and multidrug-resistant serovar Typhi by PFGE identified two distinct subtypes that were in circulation in the three different parts of Kenya. As the prevalence of multidrug-resistant serovar Typhi increases, newer, more expensive, and less readily available antimicrobial agents will be required for the treatment of typhoid in Kenya.
机译:我们通过对XbaI和SpeI消化的DNA 102 沙门氏菌血清型鼠伤寒沙门氏菌(serovar Typhi)的抗生素敏感性,质粒分析,不相容性分组和脉冲场凝胶电泳(PFGE)进行了表征肯尼亚三个不同地区的伤寒。完全易感的仅13.7%,而对5种常用药物:氨苄青霉素,氯霉素和四环素(MIC大于256μg/ ml)分别有82.4%的耐药性;链霉素(MIC,> 1,024μg/ ml);和cotrimoxazole(MIC> 32μg/ ml)。对这些抗生素的抗性在IncHI1不相容性组的110 kb自转移质粒上编码。 102种血清型Typhi分离物中41.7%的萘啶酸(MIC,8至16μg/ ml)和环丙沙星(MIC为0.25至0.38μg/ ml)的MIC分别比敏感菌株高5倍和10倍。株。通过PCR扩增并编码编码回旋酶( gyrA gyrB )和拓扑异构酶IV( parE parC )在喹诺酮抗性确定区域内显示,喹诺酮的MIC的增加不是由于任何明显的突变引起的。通过PFGE分析来自抗菌药敏感型和耐多药血清型的基因组DNA,确定了在肯尼亚三个不同地区流通的两种不同的亚型。随着耐多药血清型伤寒的流行,肯尼亚需要更多,更昂贵,更不易获得的抗菌剂来治疗伤寒。

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