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工程酶组装线生产新抗生素。

Engineering enzymatic assembly lines to produce new antibiotics.

机构信息

Department of Molecular Microbiology, John Innes Centre, Norwich Research Park, Norwich NR4 7UH, UK.

Department of Chemistry, Manchester Institute for Biotechnology, The University of Manchester, 131 Princess Street, Manchester M1 7DN, UK.

出版信息

Curr Opin Microbiol. 2019 Oct;51:88-96. doi: 10.1016/j.mib.2019.10.007. Epub 2019 Nov 16.

Abstract

Numerous important therapeutic agents, including widely-used antibiotics, anti-cancer drugs, immunosuppressants, agrochemicals and other valuable compounds, are produced by microorganisms. Many of these are biosynthesised by modular enzymatic assembly line polyketide synthases, non-ribosomal peptide synthetases, and hybrids thereof. To alter the backbone structure of these valuable but difficult to modify compounds, the respective enzymatic machineries can be engineered to create even more valuable molecules with improved properties and/or to bypass resistance mechanisms. In the past, many attempts to achieve assembly line pathway engineering failed or led to enzymes with compromised activity. Recently our understanding of assembly line structural biology, including an appreciation of the conformational changes that occur during the catalytic cycle, have improved hugely. This has proven to be a driving force for new approaches and several recent examples have demonstrated the production of new-to-nature molecules, including anti-infectives. We discuss the developments of the last few years and highlight selected, illuminating examples of assembly line engineering.

摘要

许多重要的治疗药物,包括广泛使用的抗生素、抗癌药物、免疫抑制剂、农用化学品和其他有价值的化合物,都是由微生物产生的。其中许多是通过模块化酶装配线聚酮合酶、非核糖体肽合酶及其杂种生物合成的。为了改变这些有价值但难以修饰的化合物的骨架结构,可以对相应的酶机制进行工程改造,从而创造出具有改进性能和/或绕过耐药机制的更有价值的分子。过去,许多尝试进行装配线途径工程的努力都失败了,或者导致酶的活性受损。最近,我们对装配线结构生物学的理解有了很大的提高,包括对催化循环中发生的构象变化的认识。这已被证明是新方法的驱动力,最近的几个例子证明了新的天然分子的生产,包括抗感染药物。我们讨论了过去几年的发展,并强调了装配线工程的一些精选、有启发性的例子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5c2b/6908967/8fafb89d314b/gr1.jpg

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