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Analysis of predicted amino acid biosynthesis in Rv3344c in Mycobacterium tuberculosis H(37)Rv using bioinformatics tools

机译:用生物信息学工具分析抗结核术中RV3344C中的预测氨基酸生物合成

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According to World Health Organization (WHO) report, Mycobacterium tuberculosis H(37)Rv (M. tuberculosis) affects one-third population of the world. Emergence of effective treatment/research against this disease is need of the hour. Therefore, we present some important aspects of Rv3344c, which is a PE_PGRS protein. Evidence shows that PE_PGRS proteins show fibronectin binding activity. This protein has affinity for calcium and also shows motifs of GTP-binding protein. It also shows the presence of sites for ribose-5-phosphate binding and motifs of aspartate-beta-semialdehyde dehydrogenase, both of which are involved in amino acid biosynthesis. Thus, this protein might be targeted to block the amino acid biosynthesis in M. tuberculosis. This article takes into consideration some important aspects of Rv3344c protein as its function is still unknown. This study includes retrieval of protein sequence database, multiple sequence alignment, protein-protein interaction, epitope prediction, localization, function prediction, phosphorylation site prediction, model building and its validation, ligand-binding prediction along with mutational analysis. Hence, this study might be an important step in the development of new drugs and treatment of tuberculosis.
机译:根据世界卫生组织(世卫组织)报告,结核病H(37)RV(肺结核)影响世界三分之一的人口。对这种疾病有效治疗/研究的出现需要一小时。因此,我们介绍了RV3344C的一些重要方面,即PE_PGRS蛋白。证据表明,PE_PGR蛋白显示纤维素结合活性。该蛋白质对钙具有亲和力,并且还显示了GTP结合蛋白的基序。它还显示出存在核糖-5-磷酸盐结合和基序的核苷酸 - β-半醛脱氢酶的基位的存在,两者都参与氨基酸生物合成。因此,该蛋白质可能靶向阻断氨基酸生物合成的氨基酸。本文考虑了RV3344C蛋白的一些重要方面,因为其功能仍然是未知的。该研究包括检索蛋白质序列数据库,多序列比对,蛋白质 - 蛋白质相互作用,表位预测,定位,功能预测,磷酸化位点预测,模型建设及其验证,配体结合预测以及突变分析。因此,本研究可能是开发新药和结核病治疗的重要一步。

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