• 主题
高级搜索  >
历史搜索 清空历史
首页> 外文OA文献 >Synergistic Killing of Polymyxin B in Combination With the Antineoplastic Drug Mitotane Against Polymyxin-Susceptible and -Resistant Acinetobacter baumannii: A Metabolomic Study
【2h】

Synergistic Killing of Polymyxin B in Combination With the Antineoplastic Drug Mitotane Against Polymyxin-Susceptible and -Resistant Acinetobacter baumannii: A Metabolomic Study

机译:多粘菌素B与抗肿瘤药物培养物联合多羟虫酸敏感和 - 抗生素的抗肿瘤患者的协同杀伤:一种代谢物研究

代理获取
本网站仅为用户提供外文OA文献查询和代理获取服务,本网站没有原文。下单后我们将采用程序或人工为您竭诚获取高质量的原文,但由于OA文献来源多样且变更频繁,仍可能出现获取不到、文献不完整或与标题不符等情况,如果获取不到我们将提供退款服务。请知悉。
页面导航
  • 摘要
  • 著录项
  • 相似文献
  • 相关主题

摘要

Polymyxins are currently used as the last-resort antibiotics against multidrug-resistant Acinetobacter baumannii. As resistance to polymyxins emerges in A. baumannii with monotherapy, combination therapy is often the only remaining treatment option. A novel approach is to employ the combination of polymyxin B with non-antibiotic drugs. In the present study, we employed metabolomics to investigate the synergistic mechanism of polymyxin B in combination with the antineoplastic drug mitotane against polymyxin-susceptible and -resistant A. baumannii. The metabolomes of four A. baumannii strains were analyzed following treatment with polymyxin B, mitotane and the combination. Polymyxin B monotherapy induced significant perturbation in glycerophospholipid (GPL) metabolism and histidine degradation pathways in polymyxin-susceptible strains, and minimal perturbation in polymyxin-resistant strains. Mitotane monotherapy induced minimal perturbation in the polymyxin-susceptible strains, but caused significant perturbation in GPL metabolism, pentose phosphate pathway and histidine degradation in the LPS-deficient polymyxin-resistant strain (FADDI-AB065). The polymyxin B – mitotane combination induced significant perturbation in all strains except the lipid A modified polymyxin-resistant FADDI-AB225 strain. For the polymyxin-susceptible strains, the combination therapy significantly perturbed GPL metabolism, pentose phosphate pathway, citric acid cycle, pyrimidine ribonucleotide biogenesis, guanine ribonucleotide biogenesis, and histidine degradation. Against FADDI-AB065, the combination significantly perturbed GPL metabolism, pentose phosphate pathway, citric acid cycle, and pyrimidine ribonucleotide biogenesis. Overall, these novel findings demonstrate that the disruption of the citric acid cycle and inhibition of nucleotide biogenesis are the key metabolic features associated with synergistic bacterial killing by the combination against polymyxin-susceptible and -resistant A. baumannii.
机译:多元辛目前被用作对抗多药抗性的抗生素Baumannii的最后一个度假抗生素。由于A.Baumannii与单一疗法出现的多粘蛋白抗性,联合治疗通常是唯一剩余的治疗选择。一种新的方法是使用具有非抗生素药物的多粘蛋白B的组合。在本研究中,我们使用代谢组学,以研究多粘蛋白B与抗肿瘤药物培养物联合多粘物敏和-Resistant A.Baumannii的协同机制。在用多粘菌素B,Mitotane和组合处理后,分析了四个A.Baumannii菌株的代谢物。多酶B单药治疗在多粘菌素易感菌株中诱导甘油磷脂(GPL)代谢和组氨酸降解途径的显着扰动,并且在多粘菌素抗性菌株中最小的扰动。 Mitotane单药治疗在多粘菌素易感菌株中诱导最小的扰动,但在LPS缺陷的多辛菌株菌株(FADDI-AB065)中导致GPL代谢,磷酸磷途径和组氨酸降解引起的显着扰动。除了脂质的改性的多羟胞素抗性Faddi-AB225菌株外,多粘菌素B - Mitotane组合诱导了所有菌株的显着扰动。对于多辛溶解的菌株,联合治疗显着扰动GPL代谢,戊糖磷酸途径,柠檬酸循环,嘧啶核糖核苷酸生物发生,鸟嘌呤核糖核苷酸生物发生和组氨酸的降解。针对Faddi-AB065,组合显着扰动GPL代谢,戊糖磷酸途径,柠檬酸循环和嘧啶核糖核苷酸生物发生。总体而言,这些新颖的研究结果表明,柠檬酸循环和核苷酸生物发生的抑制是与通过对多粘物菌素易感和-Resistant A.Baumannii的协同细菌杀伤相关的关键代谢特征。

著录项

相似文献

  • 外文文献
  • 中文文献
  • 专利
代理获取

客服邮箱:kefu@zhangqiaokeyan.com

京公网安备:11010802029741号 ICP备案号:京ICP备15016152号-6 六维联合信息科技 (北京) 有限公司©版权所有

  • 客服微信

  • 服务号