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The anti-cancerous drug doxorubicin decreases the c-di-GMP content in Pseudomonas aeruginosa but promotes biofilm formation

机译:抗癌药阿霉素可降低铜绿假单胞菌中c-di-GMP含量,但可促进生物膜形成

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Current antibiotic treatments are insufficient in eradicating bacterial biofilms, which represent the primary cause of chronic bacterial infections. Thus, there is an urgent need for new strategies to eradicate biofilm infections. The second messenger c-di-GMP is a positive regulator of biofilm formation in many clinically relevant bacteria. It is hypothesized that drugs lowering the intracellular level of c-di-GMP will force biofilm bacteria into a more treatable planktonic lifestyle. To identify compounds capable of lowering c-di-GMP levels in Pseudomonas aeruginosa, we screened 5000 compounds for their potential c-di-GMP-lowering effect using a recently developed c-di-GMP biosensor strain. Our screen identified the anti-cancerous drug doxorubicin as a potent c-di-GMP inhibitor. In addition, the drug decreased the transcription of many biofilm-related genes. However, despite its effect on the c-di-GMP content in P. aeruginosa, doxorubicin was unable to inhibit biofilm formation or disperse established biofilms. On the contrary, the drug was found to promote P. aeruginosa biofilm formation, possibly through release of extracellular DNA from a subpopulation of killed bacteria. Our findings emphasize that lowering of the c-di-GMP content in bacteria might not be sufficient to mediate biofilm inhibition or dispersal.
机译:当前的抗生素治疗不足以消除细菌生物膜,这代表了慢性细菌感染的主要原因。因此,迫切需要消除生物膜感染的新策略。第二信使c-di-GMP是许多临床相关细菌中生物膜形成的正向调节剂。据推测,降低细胞内c-di-GMP水平的药物将迫使生物膜细菌进入更易治疗的浮游生活方式。为了鉴定能够降低铜绿假单胞菌中c-di-GMP水平的化合物,我们使用最近开发的c-di-GMP生物传感器菌株筛选了5000种可能降低c-di-GMP的化合物。我们的筛查确定抗癌药物阿霉素为有效的c-di-GMP抑制剂。此外,该药物还减少了许多生物膜相关基因的转录。然而,尽管阿霉素对铜绿假单胞菌中的c-di-GMP含量有影响,但阿霉素不能抑制生物膜的形成或分散已建立的生物膜。相反,发现该药物可能通过杀死的细菌亚群释放细胞外DNA来促进铜绿假单胞菌生物膜形成。我们的发现强调指出,降低细菌中c-di-GMP的含量可能不足以介导生物膜的抑制或扩散。

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