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从与海洋海绵相关的睾丸酮丛毛单胞菌和弗氏柠檬酸杆菌中提取的次生代谢产物作为针对多重耐药病原体的潜在抗菌剂以及埃博拉病毒VP40基质蛋白的假定先导物:一项体外和计算机模拟研究。

Secondary metabolites extracted from marine sponge associated Comamonas testosteroni and Citrobacter freundii as potential antimicrobials against MDR pathogens and hypothetical leads for VP40 matrix protein of Ebola virus: an in vitro and in silico investigation.

作者信息

Skariyachan Sinosh, Acharya Archana B, Subramaniyan Saumya, Babu Sumangala, Kulkarni Shruthi, Narayanappa Rajeswari

机构信息

a Department of Biotechnology Engineering , Dayananda Sagar Institutions , Bengaluru 560 078 , Karnataka , India.

b Visvesvaraya Technological University , Belagavi , India.

出版信息

J Biomol Struct Dyn. 2016 Sep;34(9):1865-83. doi: 10.1080/07391102.2015.1094412. Epub 2015 Nov 18.

Abstract

The current study explores therapeutic potential of metabolites extracted from marine sponge (Cliona sp.)-associated bacteria against MDR pathogens and predicts the binding prospective of probable lead molecules against VP40 target of Ebola virus. The metabolite-producing bacteria were characterized by agar overlay assay and as per the protocols in Bergey's manual of determinative bacteriology. The antibacterial activities of extracted metabolites were tested against clinical pathogens by well-diffusion assay. The selected metabolite producers were characterized by 16S rDNA sequencing. Chemical screening and Fourier Transform Infrared (FTIR) analysis for selected compounds were performed. The probable lead molecules present in the metabolites were hypothesized based on proximate analysis, FTIR data, and literature survey. The drug-like properties and binding potential of lead molecules against VP40 target of Ebola virus were hypothesized by computational virtual screening and molecular docking. The current study demonstrated that clear zones around bacterial colonies in agar overlay assay. Antibiotic sensitivity profiling demonstrated that the clinical isolates were multi-drug resistant, however; most of them showed sensitivity to secondary metabolites (MIC-15 μl/well). The proximate and FTIR analysis suggested that probable metabolites belonged to alkaloids with O-H, C-H, C=O, and N-H groups. 16S rDNA characterization of selected metabolite producers demonstrated that 96% and 99% sequence identity to Comamonas testosteroni and Citrobacter freundii, respectively. The docking studies suggested that molecules such as Gymnastatin, Sorbicillactone, Marizomib, and Daryamide can designed as probable lead candidates against VP40 target of Ebola virus.

摘要

本研究探索了从海洋海绵(Cliona sp.)相关细菌中提取的代谢产物对多重耐药病原体的治疗潜力,并预测了可能的先导分子与埃博拉病毒VP40靶点的结合前景。通过琼脂覆盖试验并按照《伯杰氏鉴定细菌学手册》中的方案对产生代谢产物的细菌进行了鉴定。通过打孔扩散试验测试了提取的代谢产物对临床病原体的抗菌活性。通过16S rDNA测序对选定的代谢产物产生菌进行了鉴定。对选定的化合物进行了化学筛选和傅里叶变换红外(FTIR)分析。基于近似分析、FTIR数据和文献调查,推测了代谢产物中可能存在的先导分子。通过计算虚拟筛选和分子对接,推测了先导分子对埃博拉病毒VP40靶点的类药物性质和结合潜力。本研究表明,在琼脂覆盖试验中细菌菌落周围出现了清晰的抑菌圈。抗生素敏感性分析表明,临床分离株具有多重耐药性,然而,其中大多数对次生代谢产物敏感(最低抑菌浓度为15 μl/孔)。近似分析和FTIR分析表明,可能的代谢产物属于含有O-H、C-H、C=O和N-H基团的生物碱。对选定的代谢产物产生菌进行的16S rDNA鉴定表明,它们与睾丸酮丛毛单胞菌和弗氏柠檬酸杆菌的序列同一性分别为96%和99%。对接研究表明,如裸头草辛、山梨素内酯、马里佐米布和达里亚酰胺等分子可设计为针对埃博拉病毒VP40靶点的可能先导候选物。

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