Hygromycin A: Activity, Biosynthesis, Export, Resistance and Regulation

潮霉素 A：活性、生物合成、输出、耐药性和监管

• 批准号: 8537947
• 负责人: KEVIN A REYNOLDS
• 金额: $ 28.31万
• 依托单位: PORTLAND STATE UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2011
• 资助国家: 美国
• 起止时间: 2011-09-20 至 2015-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8537947
• 关键词: Actinobacteria class; Address; Aminoglycosides; Anabolism; Antibiotic Resistance; Antibiotics; Architecture; Azithromycin; Bacteria; Bacterial Infections; Binding; Biochemical; Biological; Biological Factors; Cells; Chemicals; Chromosomes; Clinical; Complex; Development; Enzymatic Biochemistry; Enzymes; Gene Cluster; Gene Expression; Genes; Genetic; Gram-Negative Bacteria; Infection; Lead; Linezolid; Macrolides; Modification; Molecular; Multi-Drug Resistance; Organism; Oxazolidinones; Pathway interactions; Process; Protein Biosynthesis; Proteins; Regulation; Relative (related person); Resistance; Resistance Process; Resistance development; Ribonucleoproteins; Ribosomal Interaction; Ribosomes; Role; Shunt Device; Soil; Source; Staging; Streptomyces; Structure; Tetracyclines; Work; antibiotic efflux; bacterial resistance; base; biosynthetic product; drug development; drug resistant bacteria; fascinate; hygromycin A; insight; interdisciplinary approach; interest; microbial; microorganism; mutant; novel; repository; resistance mechanism; telithromycin; uptake

DESCRIPTION (provided by applicant): Many clinically important classes of antibiotics, including macrolides (azithromycin, telithromycin), tetracyclines, aminoglycosides (gentamycin), and more recently oxazolidinones (linezolid) target the bacterial ribosome, which is essential for intracellular protein synthesis. Use of these and other antibiotics against pathogenic microorganisms inevitably leads to development of bacterial resistance, an increasing problem within the clinical setting. There is thus a continued need to develop new antibiotics, effective against multi-drug resistant bacteria, and for approaches which can retard the inevitable development of resistance to these. The ribosome represents one of the richest and most effective targets for development of new antibiotics. Such drug development efforts can build upon a molecular level understanding of the ribosomal interactions with chemically distinct architectures, structural requirements for other aspects of biologically activity (including cellular uptake) and likely mechanisms for development of resistance. Hygromycin A (HygA), an antibiotic isolated from Streptomyces hygroscopicus and is active against both Gram-positive and Gram-negative bacteria and a mechanism of action which involves a distinct but enigmatic binding to the ribosome. HygA also has a chemical architecture which differs significantly from other antibiotics which target the ribosome. For these reasons HygA is of interest for potential development into new class of clinically-useful antibiotics. The long term project objective is to build a comprehensive understanding of hygromycin A (HygA) activity, biosynthesis, export, resistance and regulation (ABERR). This project period has 5 specific aims which will be pursed using a multi-interdisciplinary and collaborative approach with genetic, biochemical and structural studies. Aim 1. Obtain a detailed understanding of the enzymology of key and novel steps in the HygA biosynthetic process. Aim 2. Elucidate how HygA, biosynthetic pathway intermediates and shunt products, bind to ribosomes. Aim 3. Determine mechanisms by which the final product HygA is excreted from the cell. Aim 4. Evaluate the relative roles of covalent modification of both the antibiotic and the S. hygroscopicus ribosome in conferring resistance to HygA and related biosynthetic products. Aim 5. Determine how HygA ABERR processes are regulated, and to what extent are they coordinated.

性状（由申请方提供）：许多临床重要类别的抗生素，包括大环内酯类（阿奇霉素、泰利霉素）、四环素类、氨基糖苷类（庆大霉素）和最近的恶唑烷酮类（利奈唑胺），靶向细菌核糖体，这是细胞内蛋白质合成所必需的。使用这些和其他抗生素对抗病原微生物不可避免地导致细菌耐药性的发展，这是临床环境中日益严重的问题。因此，持续需要开发有效对抗多重耐药细菌的新抗生素，以及可以延缓对这些细菌不可避免的耐药性发展的方法。核糖体是开发新抗生素的最丰富和最有效的靶点之一。这种药物开发工作可以建立在对核糖体与化学上不同的结构的相互作用、生物活性的其他方面（包括细胞摄取）的结构要求和产生抗性的可能机制的分子水平理解的基础上。 潮霉素A（HygA），一种从吸水链霉菌中分离出来的抗生素，对革兰氏阳性和革兰氏阴性细菌都有活性，其作用机制涉及与核糖体的独特但神秘的结合。HygA还具有与靶向核糖体的其他抗生素显著不同的化学结构。由于这些原因，HygA对于潜在开发成新类别的临床有用的抗生素是有意义的。 长期项目目标是建立对潮霉素A（HygA）活性、生物合成、输出、抗性和调节（ABERR）的全面了解。该项目期间有5个具体目标，将采用多学科和遗传，生物化学和结构研究的合作方法进行追求。目标1.详细了解HygA生物合成过程中关键和新步骤的酶学。目标二。阐明HygA、生物合成途径中间体和分流产物如何与核糖体结合。目标3。确定最终产物HygA从细胞中分泌的机制。目标4。评价抗生素和沙门氏菌共价修饰的相对作用。吸水菌核糖体赋予对HygA和相关生物合成产物的抗性。目标5。确定HygA ABERR过程是如何调节的，以及它们在多大程度上是协调的。