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Delineating the biosynthesis of gentamicin x2, the common precursor of the gentamicin C antibiotic complex.


ABSTRACT: Gentamicin C complex is a mixture of aminoglycoside antibiotics used worldwide to treat severe Gram-negative bacterial infections. Despite its clinical importance, the enzymology of its biosynthetic pathway has remained obscure. We report here insights into the four enzyme-catalyzed steps that lead from the first-formed pseudotrisaccharide gentamicin A2 to gentamicin X2, the last common intermediate for all components of the C complex. We have used both targeted mutations of individual genes and reconstitution of portions of the pathway in vitro to show that the secondary alcohol function at C-3? of A2 is first converted to an amine, catalyzed by the tandem operation of oxidoreductase GenD2 and transaminase GenS2. The amine is then specifically methylated by the S-adenosyl-l-methionine (SAM)-dependent N-methyltransferase GenN to form gentamicin A. Finally, C-methylation at C-4? to form gentamicin X2 is catalyzed by the radical SAM-dependent and cobalamin-dependent enzyme GenD1.

SUBMITTER: Huang C 

PROVIDER: S-EPMC4340712 | biostudies-literature | 2015 Feb

REPOSITORIES: biostudies-literature

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Delineating the biosynthesis of gentamicin x2, the common precursor of the gentamicin C antibiotic complex.

Huang Chuan C   Huang Fanglu F   Moison Eileen E   Guo Junhong J   Jian Xinyun X   Duan Xiaobo X   Deng Zixin Z   Leadlay Peter F PF   Sun Yuhui Y  

Chemistry & biology 20150129 2


Gentamicin C complex is a mixture of aminoglycoside antibiotics used worldwide to treat severe Gram-negative bacterial infections. Despite its clinical importance, the enzymology of its biosynthetic pathway has remained obscure. We report here insights into the four enzyme-catalyzed steps that lead from the first-formed pseudotrisaccharide gentamicin A2 to gentamicin X2, the last common intermediate for all components of the C complex. We have used both targeted mutations of individual genes and  ...[more]

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