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首页> 外文期刊>Applied Biochemistry and Biotechnology >Subtractive Genomics Approach to Identify Putative Drug Targets and Identification of Drug-like Molecules for Beta Subunit of DNA Polymerase III in Streptococcus Species
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Subtractive Genomics Approach to Identify Putative Drug Targets and Identification of Drug-like Molecules for Beta Subunit of DNA Polymerase III in Streptococcus Species

机译:减法基因组学方法来确定推定的药物靶标和链球菌属物种中DNA聚合酶III的β亚基的类药物分子的鉴定。

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摘要

The prolonged use of the antibiotics over the years has transformed many organisms resistant to multiple drugs. This has made the field of drug discovery of vital importance in curing various infections and diseases. The drugs act by binding to a specific target protein of prime importance for the cell’s survival. Streptococcus agalactiae, Streptococcus pneumoniae, and Streptococcus pyogenes are the few gram positive organisms that have developed resistance to drugs. It causes pneumonia, meningitis, pharyngitis, otitis media, sinusitis, bacteremia, pericarditis, and arthritis infections. The present study was carried out to identify potential drug targets and inhibitors for beta subunit of DNA polymerase III in these three Streptococcus species that might facilitate the discovery of novel drugs in near future. Various steps were adopted to find out novel drug targets. And finally 3D structure of DNA polymerase III subunit beta was modeled. The ligand library was generated from various databases to find the most suitable ligands. All the ligands were docked using Molegro Virtual Docker and the lead molecules were investigated for ADME and toxicity.
机译:这些年来,抗生素的长期使用已经改变了许多对多种药物具有耐药性的生物。这使得药物发现领域对于治疗各种感染和疾病至关重要。这些药物通过与对细胞存活至关重要的特定靶蛋白结合而起作用。无乳链球菌,肺炎链球菌和化脓性链球菌是少数对药物产生耐药性的革兰氏阳性生物。它会引起肺炎,脑膜炎,咽炎,中耳炎,鼻窦炎,菌血症,心包炎和关节炎感染。进行本研究以鉴定这三种链球菌中潜在的药物靶标和DNA聚合酶IIIβ亚基的抑制剂,这可能会在不久的将来促进新药的发现。采取了各种步骤来找出新的药物靶标。最后,对DNA聚合酶III亚基β的3D结构进行了建模。配体库从各种数据库生成,以找到最合适的配体。使用Molegro Virtual Docker对接所有配体,并研究了铅分子的ADME和毒性。

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