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Complete reconstitution of the diverse pathways of gentamicin B biosynthesis

Authors
Ban, Yeon HeeSong, Myoung ChongHwang, Jae-YeonShin, Hea-LyungKim, Hak JoongHong, Seung KonLee, Na JoonPark, Je WonCha, Sun-ShinLiu, Hung-wenYoon, Yeo Joon
Issue Date
3월-2019
Publisher
NATURE PUBLISHING GROUP
Citation
NATURE CHEMICAL BIOLOGY, v.15, no.3, pp.295 - +
Indexed
SCIE
SCOPUS
Journal Title
NATURE CHEMICAL BIOLOGY
Volume
15
Number
3
Start Page
295
End Page
+
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/67164
DOI
10.1038/s41589-018-0203-4
ISSN
1552-4450
Abstract
Gentamicin B (GB), a valuable starting material for the preparation of the semisynthetic aminoglycoside antibiotic isepamicin, is produced in trace amounts by the wild-type Micromonospora echinospora. Though the biosynthetic pathway to GB has remained obscure for decades, we have now identified three hidden pathways to GB production via seven hitherto unknown intermediates in M. echinospora. The narrow substrate specificity of a key glycosyltransferase and the C6'-amination enzymes, in combination with the weak and unsynchronized gene expression of the 2'-deamination enzymes, limits GB production in M. echinospora. The crystal structure of the aminotransferase involved in C6'-amination explains its substrate specificity. Some of the new intermediates displayed similar premature termination codon readthrough activity but with reduced toxicity compared to the natural aminoglycoside G418. This work not only led to the discovery of unknown biosynthetic routes to GB, but also demonstrated the potential to mine new aminoglycosides from nature for drug discovery.
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