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Featured researches published by Stephan Bartel.


Journal of Biological Chemistry | 2003

Specific and Potent Inhibition of NAD+-dependent DNA Ligase by Pyridochromanones

Heike Brötz-Oesterhelt; Igor Knezevic; Stephan Bartel; Thomas Lampe; Ute Warnecke-Eberz; Karl Ziegelbauer; Dieter Häbich; Harald Labischinski

Pyridochromanones were identified by high throughput screening as potent inhibitors of NAD+-dependent DNA ligase from Escherichia coli. Further characterization revealed that eubacterial DNA ligases from Gramnegative and Gram-positive sources were inhibited at nanomolar concentrations. In contrast, purified human DNA ligase I was not affected (IC50 > 75 μm), demonstrating remarkable specificity for the prokaryotic target. The binding mode is competitive with the eubacteria-specific cofactor NAD+, and no intercalation into DNA was detected. Accordingly, the compounds were bactericidal for the prominent human pathogen Staphylococcus aureus in the low μg/ml range, whereas eukaryotic cells were not affected up to 60 μg/ml. The hypothesis that inhibition of DNA ligase is the antibacterial principle was proven in studies with a temperature-sensitive ligase-deficient E. coli strain. This mutant was highly susceptible for pyridochromanones at elevated temperatures but was rescued by heterologous expression of human DNA ligase I. A physiological consequence of ligase inhibition in bacteria was massive DNA degradation, as visualized by fluorescence microscopy of labeled DNA. In summary, the pyridochromanones demonstrate that diverse eubacterial DNA ligases can be addressed by a single inhibitor without affecting eukaryotic ligases or other DNA-binding enzymes, which proves the value of DNA ligase as a novel target in antibacterial therapy.


Archive | 1996

Heterobenzocyclopentane oxazolidinones having antibacterial activity

Andreas Stolle; Dieter Habich; Stephan Bartel; Bernd Riedl; Martin Ruppelt; Hanno Wild; Rainer Endermann; Klaus-Dieter Bremm; Hein-Peter Kroll; Harald Labischinski; Klaus Schaller; Hans-Otto Werling


Archive | 1997

Heteroatom-containing cyclopentanopyridyl-oxazolidinones

Andreas Stolle; Dieter Habich; Bernd Riedl; Martin Ruppelt; Stephan Bartel; Walter Guarnieri; Hanno Wild; Rainer Endermann; Hein-Peter Kroll


Archive | 1997

Pyrido-fused thienyl- and furanyl-oxazolidinones

Bernd Riedl; Dieter Habich; Andreas Stolle; Martin Ruppelt; Stephan Bartel; Walter Guarnieri; Rainer Endermann; Hein-Peter Kroll


Archive | 1996

Heteroatom-containing benzocyclopentane-oxazolidinones

Andreas Stolle; Dieter Habich; Stephan Bartel; Bernd Riedl; Martin Ruppelt; Hanno Wild; Rainer Endermann; Klaus-Dieter Bremm; Hein-Peter Kroll; Harald Labischinski; Klaus Schaller; Hans-Otto Werling


Archive | 1998

Tricyclically substituted oxazolidinones

Stephan Bartel; Walter Guarnieri; Bernd Riedl; Dieter Häbich; Andreas Stolle; Martin Ruppelt; Siegfried Raddatz; Ulrich Rosentreter; Hanno Wild; Rainer Endermann; Hein-Peter Kroll


Archive | 1997

Use of 7-(2-oxa-5,8-diazabicyclo[4.3.0]non-8-yl)-quinolone carboxylic acid and naphthyridon carboxylic acid derivatives for the treatment of Helicobacter pylori infections and associated gastroduodenal diseases

Michael Matzke; Uwe Petersen; Thomas Jaetsch; Stephan Bartel; Thomas Schenke; Thomas Himmler; Bernd Baasner; Hans-Otto Werling; Klaus Schaller; Harald Labischinski


Archive | 1997

2-oxo- and 2-thio-1,2-dihydroquinolinyl-oxazolidinones

Dieter Habich; Andreas Stolle; Bernd Riedl; Martin Ruppelt; Stephan Bartel; Walter Guarnieri; Rainer Endermann; Hein-Peter Kroll


Archive | 1999

Novel bicyclene-substituted oxazolidinones

Stephan Bartel; Walter Guarnieri; Dieter Habich; Siegfried Raddatz; Bernd Riedl; Ulrich Rosentreter; Martin Ruppelt; Andreas Stolle; Hanno Wild; Rainer Endermann; Hein-Peter Kroll


Archive | 1999

Novel substituted phenyloxazolidone derivatives

Stephan Bartel; Siegfried Raddatz; Michael Härter; Ulrich Rosentreter; Hanno Wild; Rainer Endermann; Hein-Peter Kroll

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