Lothar G Fröhlich

Sanofi-Aventis, Chemical Sciences, Drug Design, Building G 878, D-65926 Frankfurt am Main, Germany.

Publications of Lothar G Fröhlich

  • Structural analysis of isoform-specific inhibitors targeting the tetrahydrobiopterin binding site of human nitric oxide synthases.

    Authors: Hans Matter, H S Arun Kumar, Roman Fedorov, Armin Frey, Peter Kotsonis, Elisabeth Hartmann, Lothar G Fröhlich, Andreas Reif, Wolfgang Pfleiderer, Peter Scheurer, Dipak K Ghosh, Ilme Schlichting, Harald H H W Schmidt

    Journal of medicinal chemistry. 08/2005; 48(15):4783-92.

    Nitric oxide synthesized from l-arginine by nitric oxide synthase isoforms (NOS-I-III) is physiologically important but also can be deleterious when overproduced. Selective NOS inhibitors are of
  • Structural requirements for inhibition of the neuronal nitric oxide synthase (NOS-I): 3D-QSAR analysis of 4-oxo- and 4-amino-pteridine-based inhibitors.

    Authors: Hans Matter, Peter Kotsonis, Otmar Klingler, Hartmut Strobel, Lothar G Fröhlich, Armin Frey, Wolfgang Pfleiderer, Harald H H W Schmidt

    Journal of medicinal chemistry. 08/2002; 45(14):2923-41.

    The family of homodimeric nitric oxide synthases (NOS I-III) catalyzes the generation of the cellular messenger nitric oxide (NO) by oxidation of the substrate L-arginine. The rational design of
  • Anti-pterins as tools to characterize the function of tetrahydrobiopterin in NO synthase

    Authors: Heike M. Bömmel, Andreas Reif, Lothar G Fröhlich, Armin Frey, Heinrich Hofmann, Dale M. Marecak, Viola Groehn, Peter Kotsonis, Mylinh La, Sandra Köster, Matthias Meinecke, Manfred Bernhardt, Monika Weeger, Sandro Ghisla, Glenn D. Prestwich, Wolfgang Pfleiderer, Harald H H W Schmidt

    First publ. in: Journal of Biological Chemistry 273 (1998), 50, pp. 33142-33149.

    Nitric oxide synthases (NOS) are homodimeric enzymes that NADPH-dependently convert L-arginine to nitric oxide and L-citrulline. Interestingly, all NOS also require

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Keywords of Lothar G Fröhlich

Basal NOS activity
 
binding site
 
H(4)Bip binding site
 
II anti-pterins
 
nitric oxide synthases
 
NOS activity
 
NOS inhibitors
 
oxide synthases
 
pterin-based NOS inhibitors
 
rational design
 
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