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Bioinformatic analysis to discover putative drug targets against diarrheal causative agents

机译:生物信息学分析以发现针对腹泻病原体的推定药物靶标

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Availability of genome sequences of pathogens has offered a tremendous amount of information that can be useful in drug target identification. Complete genome sequences of several pathogenic bacteria including?Shigella?spp.,?Escherichia coli,Vibrio cholerae,?Salmonella typhimurium?and?Yersinia enterocolitica?mostly involved in causing diarrheal diseases have been determined. Detection of bacterial genes that are common in all of them, non-homologous to human genes and essential for the survival of the pathogen represents a promising means of identifying novel drug targets. Results recommended that among these common proteins, surface associated proteins might be most useful. Our approach has identified seven essential proteins that may be considered as potential drug targets; motifs were identified for these proteins to determine their functions and antigenicity and profiling was also done to identify probable epitopes among the candidate antigens. This approach enables rapid potential drug target identification, thereby greatly facilitating the search for new drug targets against the causative agents of diarrheal diseases. These results highlight the significance of?in silico?systematic drug target identification in the post-genomic era.
机译:病原体基因组序列的可用性提供了可用于药物靶标识别的大量信息。已经确定了几种致病细菌的完整基因组序列,包括志贺氏菌,大肠杆菌,霍乱弧菌,鼠伤寒沙门氏菌和小肠结肠炎耶尔森菌,这些细菌主要引起腹泻病。细菌基因的检测在所有细菌基因中都是通用的,与人类基因非同源且对于病原体的生存至关重要,这是鉴定新型药物靶标的一种有前途的手段。结果建议,在这些常见蛋白质中,表面相关蛋白质可能是最有用的。我们的方法已经确定了七种必需蛋白,它们可能被视为潜在的药物靶标。为这些蛋白质确定了基序,以确定它们的功能和抗原性,并进行了分析以鉴定候选抗原中可能的表位。这种方法可以快速识别潜在的药物靶标,从而大大促进了针对腹泻病病原体的新药物靶标的寻找。这些结果凸显了在后基因组时代进行计算机系统药物靶标鉴定的重要性。

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