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Non-heme iron oxygenases generate natural structural diversity in carbapenem antibiotics. | LitMetric

Non-heme iron oxygenases generate natural structural diversity in carbapenem antibiotics.

J Am Chem Soc

Department of Chemistry, Johns Hopkins University, 3400 North Charles Street, Baltimore, Maryland 21218, USA.

Published: January 2010

AI Article Synopsis

  • Carbapenems are a crucial class of antibiotics, with over 50 types that differ mainly by C-2 and C-6 side chains, affecting their effectiveness.
  • Researchers found that the ThnG and ThnQ enzymes from the thienamycin gene cluster in Streptomyces cattleya play key roles in oxidizing these side chains, enhancing the antibiotic properties of carbapenems.
  • Understanding how ThnG and ThnQ work can guide future studies on how carbapenem antibiotics are made, potentially leading to more effective treatments.

Article Abstract

Carbapenems are a clinically important antibiotic family. More than 50 naturally occurring carbapenam/ems are known and are distinguished primarily by their C-2/C-6 side chains where many are only differentiated by the oxidation states of these substituents. With a limited palette of variations the carbapenem family comprises a natural combinatorial library, and C-2/C-6 oxidation is associated with increased efficacy. We demonstrate that ThnG and ThnQ encoded by the thienamycin gene cluster in Streptomyces cattleya oxidize the C-2 and C-6 moieties of carbapenems, respectively. ThnQ stereospecifically hydroxylates PS-5 (5) giving N-acetyl thienamycin (2). ThnG catalyzes sequential desaturation and sulfoxidation of PS-5 (5), giving PS-7 (7) and its sulfoxide (9). The enzymes are relatively substrate selective but are proposed to give rise to the oxidative diversity of carbapenems produced by S. cattleya, and orthologues likely function similarly in allied streptomyces. Elucidating the roles of ThnG and ThnQ will focus further investigations of carbapenem antibiotic biosynthesis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2821876PMC
http://dx.doi.org/10.1021/ja907320nDOI Listing

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