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Impact of a Low-Oxygen Environment on the Efficacy of Antimicrobials against Intracellular Chlamydia trachomatis

机译:低氧环境对抗菌剂抗沙眼衣原体细胞内作用的影响

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摘要

Emergence of chronic inflammation in the urogenital tract induced by Chlamydia trachomatis infection in females is a long-standing concern. To avoid the severe sequelae of C. trachomatis infection, such as pelvic inflammatory diseases (PID), ectopic pregnancies, and tubal infertility, antibiotic strategies aim to eradicate the pathogen even in asymptomatic and uncomplicated infections. Although first-line antimicrobials have proven successful for the treatment of C. trachomatis infection, treatment failures have been observed in a notable number of cases. Due to the obligate intracellular growth of C. trachomatis, reliable antimicrobial susceptibility assays have to consider environmental conditions and host cell-specific factors. Oxygen concentrations in the female urogenital tract are physiologically low and decrease further during an inflammatory process. We compared MIC testing and time-kill curves (TKC) for doxycycline, azithromycin, rifampin, and moxifloxacin under hypoxia (2% O2) and normoxia (20% O2). While low oxygen availability only moderately decreased the antichlamydial activity of azithromycin in conventional MIC testing (0.08 μg/ml versus 0.04 μg/ml; P < 0.05), TKC analyses revealed profound divergences for antibiotic efficacies between the two conditions. Thus, C. trachomatis was significantly less rapidly killed by doxycycline and azithromycin under hypoxia, whereas the efficacies of moxifloxacin and rifampin remained unaffected using concentrations at therapeutic serum levels. Chemical inhibition of multidrug resistance protein 1 (MDR-1), but not multidrug resistance-associated protein 1 (MRP-1), restored doxycycline activity against intracellular C. trachomatis under hypoxia. We suggest careful consideration of tissue-specific characteristics, including oxygen availability, when testing antimicrobial activities of antibiotics against intracellular bacteria.
机译:由沙眼衣原体感染引起的女性泌尿生殖道慢性炎症的出现一直是人们长期以来关注的问题。为了避免沙眼衣原体感染的严重后遗症,例如盆腔炎(PID),异位妊娠和输卵管不育,抗生素策略旨在消除病原体,即使是无症状且不复杂的感染。尽管一线抗菌药物已被证明可成功治疗沙眼衣原体感染,但在许多情况下仍观察到治疗失败。由于沙眼衣原体的专一性细胞内生长,可靠的抗菌药敏试验必须考虑环境条件和宿主细胞特异性因子。女性泌尿生殖道中的氧气浓度在生理上较低,在炎症过程中会进一步降低。我们比较了在缺氧(2%O2)和常氧(20%O2)下强力霉素,阿奇霉素,利福平和莫西沙星的MIC测试和时间杀灭曲线(TKC)。尽管低氧利用率仅在常规MIC测试中仅适度降低了阿奇霉素的抗衣原体活性(0.08μg/ ml对0.04μg/ ml; P <0.05),但TKC分析显示两种条件下抗生素功效存在巨大差异。因此,在低氧条件下,沙眼衣原体被强力霉素和阿奇霉素杀死的速度明显较慢,而在治疗性血清水平下,莫西沙星和利福平的疗效仍然不受影响。化学抑制多药抗性蛋白1(MDR-1),而不是多药抗性相关蛋白1(MRP-1),在缺氧条件下恢复了对细胞内沙眼衣原体的强力霉素活性。我们建议在测试抗生素对细胞内细菌的抗菌活性时,应仔细考虑组织的特定特征,包括氧气的可用性。

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