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首页> 外文期刊>Biological chemistry >Elucidating the anti-biofilm and anti-quorum sensing potential of selenocystine against respiratory tract infections causing bacteria: in vitro and in silico studies
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Elucidating the anti-biofilm and anti-quorum sensing potential of selenocystine against respiratory tract infections causing bacteria: in vitro and in silico studies

机译:阐明硒阴压术的抗生物膜和抗法力感测潜力对呼吸道感染引起细菌的呼吸道感染:体外和硅研究

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Bacteria are increasingly relying on biofilms to develop resistance to antibiotics thereby resulting in their failure in treating many infections. In spite of continuous research on many synthetic and natural compounds, ideal anti-biofilm molecule is still not found thereby warranting search for new class of molecules. The current study focuses on exploring anti-biofilm potential of selenocystine against respiratory tract infection (RTI)-causing bacteria. Anti-bacterial and anti-biofilm assays demonstrated that selenocystine inhibits the growth of bacteria in their planktonic state, and formation of biofilms while eradicating preformed-biofilm effectively. Selenocystine at a MIC50 as low as 42 and 28 mu g/mL effectively inhibited the growth of Klebsiella pneumonia and Pseudomonas aeruginosa. The antibacterial effect is further reconfirmed by agar cup diffusion assay and growth-kill assay. Selenocystine showed 30-60% inhibition of biofilm formation in K. pneumonia, and 44-70% in P. aeruginosa respectively. It also distorted the preformed-biofilms by degrading the eDNA component of the Extracellular Polymeric Substance matrix. Molecular docking studies of selenocystine with quorum sensing specific proteins clearly showed that through the carboxylic acid moiety it interacts and inhibits the protein function, thereby confirming its anti-biofilm potential. With further validation selenocystine can be explored as a potential candidate for the treatment of RTIs.
机译:细菌越来越依赖于生物膜来显影对抗生素的抗性,从而导致它们在治疗许多感染方面的失败。尽管对许多合成和天然化合物进行了不断的研究,但仍未发现理想的抗生物膜分子,从而保证寻找新的分子。目前的研究侧重于探索硒阴压症的抗生物膜潜力免受呼吸道感染(RTI)的分警。抗细菌和抗生物膜测定表明,硒耳囊肿抑制了它们的浮鳞状态的细菌生长,并在有效地消除了预成型的生物膜的同时形成生物膜。 MIC50的Selenocystine低至42和28μmg/ ml有效地抑制了Klebsiella肺炎和假单胞菌铜绿假单胞菌的生长。通过琼脂杯扩散测定和生长杀死测定进一步重新确认抗菌效果。 Selenocystine分别表现出30-60%的K.Pnuumonia抑制生物膜形成,分别为44-70%的铜绿假单胞菌。通过降解细胞外聚合物物质基质的EDNA组分,它还扭曲了预成型的生物膜。 Selenocystine与Quorum感测的特异性蛋白质的分子对接研究清楚地表明,通过羧酸部分相互作用并抑制蛋白质功能,从而证实其抗生物膜电位。通过进一步的验证,可以探索Selenocystine作为治疗RTIS的潜在候选者。

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