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核黄素生物合成途径酶抑制剂作为潜在的抗菌药物。

Inhibitors of riboflavin biosynthetic pathway enzymes as potential antibacterial drugs.

作者信息

Islam Zeyaul, Kumar Pankaj

机构信息

Qatar Biomedical Research Institute (QBRI), Qatar Foundation, Hamad Bin Khalifa University, Doha, Qatar.

Department of Biochemistry, Jamia Hamdard, New Delhi, India.

出版信息

Front Mol Biosci. 2023 Jul 11;10:1228763. doi: 10.3389/fmolb.2023.1228763. eCollection 2023.

Abstract

Multiple drug resistance is the main obstacle in the treatment of bacterial diseases. Resistance against antibiotics demands the exploration of new antimicrobial drug targets. A variety of and genetic approaches show that the enzymes of the riboflavin biosynthetic pathway are crucial for the survival of bacteria. This pathway is absent in humans thus enzymes of the riboflavin biosynthetic pathway are emerging drug targets for resistant pathogenic bacterial strains. Exploring the structural details, their mechanism of action, intermediate elucidation, and interaction analysis would help in designing suitable inhibitors of these enzymes. The riboflavin biosynthetic pathway consists of seven distinct enzymes, namely, 3,4-dihydroxy-2-butanone 4-phosphate synthase, GTP cyclohydrolase II, pyrimidine deaminase/reductase, phosphatase, lumazine synthase, and riboflavin synthase. The present review summarizes the research work that has been carried out on these enzymes in terms of their structures, active site architectures, and molecular mechanism of catalysis. This review also walks through small molecule inhibitors that have been developed against several of these enzymes.

摘要

多重耐药性是细菌性疾病治疗中的主要障碍。对抗生素的耐药性促使人们探索新的抗菌药物靶点。多种生化和遗传学方法表明,核黄素生物合成途径的酶对细菌的生存至关重要。人类不存在这条途径,因此核黄素生物合成途径的酶正成为耐药病原菌菌株新的药物靶点。探索其结构细节、作用机制、中间体解析以及相互作用分析,将有助于设计这些酶的合适抑制剂。核黄素生物合成途径由七种不同的酶组成,即3,4 - 二羟基 - 2 - 丁酮4 - 磷酸合酶、GTP环化水解酶II、嘧啶脱氨酶/还原酶、磷酸酶、鲁棒嗪合酶和核黄素合酶。本综述总结了针对这些酶在结构、活性位点结构和催化分子机制方面所开展的研究工作。本综述还介绍了针对其中几种酶开发的小分子抑制剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/28d4/10366380/57791e49d744/fmolb-10-1228763-g001.jpg

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