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Dive into the research topics where Otmar Klingler is active.

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Featured researches published by Otmar Klingler.


Bioorganic & Medicinal Chemistry Letters | 2003

Design, synthesis, and structure-activity relationship of a new class of amidinophenylurea-based factor VIIa inhibitors.

Otmar Klingler; Hans Matter; Manfred Schudok; S. Paul Bajaj; Joerg Czech; Martin Lorenz; Hans Peter Nestler; Herman Schreuder; Peter Wildgoose

Selective inhibition of coagulation factor VIIa has recently gained attraction as interesting approach towards antithrombotic treatment. Using parallel synthesis supported by structure-based design and X-ray crystallography, we were able to identify a novel series of amidinophenylurea derivatives with remarkable affinity for factor VIIa. The most potent compound displays a K(i) value of 23 nM for factor VIIa.


Letters in Peptide Science | 1998

From a peptide lead to an orally active peptidomimetic fibrinogen receptor antagonist

Hans Ulrich Stilz; Wolfgang Guba; Bernd Jablonka; Melitta Just; Otmar Klingler; Wolfgang König; Volkmar Wehner; Gerhard Zoller

Antagonists of the platelet fibrinogen receptor (GP IIb/IIIa receptor) are expected to be a new promising class of antithrombotic agents. The binding of fibrinogen to the fibrinogen receptor depends on an Arg-Gly-Asp-Ser (RGDS) tetrapeptide recognition motif. Structural modifications of the RGDS lead have led to the discovery of a non-peptide RGD mimetic GP IIb/IIIa antagonist20 (S 1197). Compound20 inhibits dose-dependently and reversibly human platelet aggregation. Modeling studies based on structure-activity data revealed the following structural features of the drug as important for receptor binding: the amidino group, the carboxylate group, hydrophobic substitutions at the carboxyl-terminus and at the side chain carrying the positive charge, the carboxyl-terminal NH group of the β-amino acid as a hydrogen bond donor and one oxygen atom of the hydantoin as a hydrogen bond acceptor. The ethyl ester prodrug of20 (S 5740) is an orally active antithrombotic agent which has the potential to be used to treat and prevent thrombotic diseases in humans.


Chemistry & Biology | 2005

Structural Basis for the Highly Selective Inhibition of MMP-13

Christian Engel; Bernard Pirard; Sandra Schimanski; Reinhard Kirsch; Jörg Habermann; Otmar Klingler; Volkhard Schlotte; Klaus Ulrich Weithmann; K. Ulrich Wendt


Journal of Medicinal Chemistry | 2001

Discovery of an orally active non-peptide fibrinogen receptor antagonist based on the hydantoin scaffold.

Hans Ulrich Stilz; Wolfgang Guba; Bernd Jablonka; Melitta Just; Otmar Klingler; Wolfgang König; Volkmar Wehner; Gerhard Zoller


Archive | 1998

Indole derivatives as inhibitors or factor Xa

Elisabeth Defossa; Uwe Heinelt; Otmar Klingler; Gerhard Zoller; Fahad Al-Obeidi; Armin Walser; Peter Wildgoose; Hans Matter


Archive | 1994

Substituted 5-ring heterocycles, their preparation and their use

Gerhard Zoller; Otmar Klingler; Bernd Jablonka; Melitta Just; Gerhard Breipohl; Jochen Knolle; Wolfgang Dr. König; Hans-Ulrich Stilz


Archive | 1995

2-Amino-1,3-thiazines as nitric oxide synthase inhibitors

Hartmut Strobel; Helmut Bohn; Peter Klemm; Otmar Klingler; Ursula Schindler; Karl Schonafinger; Gerhard Zoller


Archive | 1993

Phenylimidazolidine derivatives and their use

Gerhard Zoller; Bernd Jablonka; Melitta Just; Otmar Klingler; Gerhard Breipohl; Jochen Knolle; Wolfgang Dr. König


Archive | 1994

Heterocycles, their preparation and their use

Otmar Klingler; Gerhard Zoller; Bernd Jablonka; Melitta Just; Gerhard Breipohl; Jochen Knolle; Wolfgang Dr. König


Journal of Medicinal Chemistry | 2002

Structural requirements for inhibition of the neuronal nitric oxide synthase (NOS-I): 3D-QSAR analysis of 4-oxo- and 4-amino-pteridine-based inhibitors.

Hans Matter; Peter Kotsonis; Otmar Klingler; Hartmut Strobel; Lothar G. Fröhlich; Armin Frey; Wolfgang Pfleiderer; Harald Schmidt

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