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Dive into the research topics where Norbert Dipl Chem Dr Hauel is active.

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Featured researches published by Norbert Dipl Chem Dr Hauel.


British Journal of Pharmacology | 1993

Pharmacological characterization of the novel nonpeptide angiotensin II receptor antagonist, BIBR 277

Wolfgang Wienen; Norbert Dipl Chem Dr Hauel; J.C.A. Van Meel; Berthold Narr; Uwe Ries; Michael Entzeroth

1 The pharmacological profile of BIBR 277, 4′‐[(1,4′‐dimethyl‐2′‐propyl[2,6′‐bi‐1H‐benzimidazol]‐1′‐yl)methyl]‐[1,1′‐biphenyl]‐2‐carboxylic acid, a novel, nonpeptide angiotensin II receptor antagonist has been investigated by use of receptor binding studies, enzymatic assays, functional in vitro assays in rabbit aorta as well as in vivo experiments in pithed, anaesthetized and conscious rats. 2 BIBR 277 potently interacted with rat AT1 receptors (Ki 3.7 nm). Competitive receptor interaction was shown by radioligand saturation experiments performed in the presence of BIBR 277. The failure to inhibit radioligand binding to AT2 sites demonstrates the selectivity of BIBR 277 for AT1 receptors. This is further substantiated by the findings that BIBR 277 neither interacted with other receptor systems investigated nor affected the activity of components of the human renin‐angiotensin system, such as plasma renin or serum converting enzyme. 3 In rabbit aorta, BIBR 277 had no agonistic properties and was shown to be an insurmountable antagonist of angiotensin II‐induced contractions (KB 0.33 nm). The antagonistic effect persisted even after several wash‐out procedures. However, this interaction was not irreversible since the insurmountable antagonism was concentration‐dependently reversed when BIBR 277 (0.1 μm) and the surmountable antagonist, losartan (0.1 and 1.0 μm) were incubated simultaneously. The specificity of BIBR 277 for the AT1 receptor was further substantiated in this preparation since micromolar concentrations of BIBR 277 neither affected potassium chloride and noradrenaline‐induced contractions nor acetylcholine‐mediated tissue relaxation. 4 In pithed rats, i.v. administration of BIBR 277 (0.1, 0.3 and 1.0 mg kg−1) shifted the dose‐pressor response curve to angiotensin II dose‐dependently to the right with ED50 values of 0.23 μg kg−1 (control) and 1.4 μg kg−1, 4.7 μg kg−1 and 20 μg kg−1, respectively. As observed in the in vitro experiments no agonistic effect was detected and the maximum of the blood pressure response to angiotensin II at the highest dose of BIBR 277 was decreased by 29%. 5 In anaesthetized rats, bolus i.v. administration of 0.1, 0.3 and 1.0 mg kg−1 BIBR 277 attenuated the blood pressure response to bolus i.v. injections of angiotensin II (0.1 μg kg−1). At the highest dose an almost complete blockade was observed even after 2 h. 6 Single oral administration of BIBR 277 (0.3 and 1.0 mg kg−1) to conscious, chronically instrumented renovascular hypertensive rats dose‐dependently decreased the mean arterial blood pressure by 15 and 30 mmHg, respectively. At the higher dose a significant antihypertensive effect was maintained for more than 24 h. Moreover, consecutive daily dosing of 1 mg kg−1 orally resulted in a sustained reduction in blood pressure over the 4 day observation period. 7 It is concluded that BIBR 277 is an effective and selective angiotensin II antagonist with antihypertensive activity after oral administration.


Archive | 1983

Benzazepine derivatives, their pharmaceutical compositions and method of use

Manfred Dipl Chem Dr Reiffen; Joachim Dr. Dipl.-Chem. Heider; Norbert Dipl Chem Dr Hauel; Volkhard Dipl Chem Dr Austel; Wolfgang Dipl Chem Dr Eberlein; Walter Kobinger; Christian Lillie; Klaus Dipl Chem Dr Noll; Helmut Dipl Chem Dr Pieper; Gerd Kruger; Johannes Dr. Dipl.-Chem. Keck


Archive | 1986

Neue imidazo-benzoxazinone, ihre herstellung und diese verbindungen enthaltende arzneimittel

Berthold Narr; Norbert Dipl Chem Dr Hauel; Klaus Dipl Chem Dr Noll; Joachim Heider; Manfred Psiorz; Andreas Bomhard; Jacobus Van Dr Meel; Willi Diederen


Archive | 1993

Substituted benzimidazolyl derivatives, therapeutic agents containing them and process for their preparation

Norbert Dipl Chem Dr Hauel; Uwe Dipl Chem Dr Ries; Berthold Narr; Meel Jacques Dr. Van; Wolfgang Wienen; Michael Entzeroth


Archive | 1991

New phenylalkyl derivs. - are angiotensin II antagonists used to treat hypertension, coronary insufficiency, angina, cns disorders etc.

Uwe Dipl Chem Dr Ries; Berthold Narr; Norbert Dipl Chem Dr Hauel; Wolfgang Dipl Chem Dr Wienen; Jacques Van Dr Meel; Michael Entzeroth


Archive | 1985

Neue Aminotetralinderivate, diese Verbindungen enthaltende Arzneimittel und Verfahren zu ihrer Herstellung

Manfred Dipl Chem Dr Reiffen; Joachim Heider; Volkhard Dipl Chem Dr Austel; Norbert Dipl Chem Dr Hauel; Walter Kobinger; Christian Lillie


Archive | 1984

Novel 2-pnenyl-imidazoles, their preparation and drugs containing them

Volkhard Austel; Joachim Heider; Norbert Dipl Chem Dr Hauel; Manfred Reiffen; Josef Nickl; Meel Jacobus C.A. Dr. Van; Willi Diederen


Archive | 1987

Novel imidazopyridines and purines, medicaments containing these compounds, and processes for their preparation

Norbert Dipl Chem Dr Hauel; Joachim Heider; Willi Diederen; Jacques Van Dr Meel


Archive | 1992

New 1-bi:phenyl:methyl- benzimidazole derivs. - used as angiotensin antagonists, e.g. for treating cardiovascular, pulmonary and CNS disorders e.g. Alzheimer's disease, ischaemia etc.

Norbert Dipl Chem Dr Hauel; Berthold Narr; Uwe Dipl Chem Dr Ries; Jacques Van Dr Meel; Wolfgang Wienen; Michael Entzeroth


Archive | 1992

Phenylalkylderivatives, compounds containing them and process for their fabrication

Uwe Dipl Chem Dr Ries; Manfred Reiffen; Wolfgang Grell; Norbert Dipl Chem Dr Hauel; Berthold Narr; Armin Heckel; Andreas Bomhard; Meel Jacques Dr. Van; Wolfgang Wienen; Michael Entzeroth

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Volkhard Dipl Chem Dr Austel

Massachusetts Institute of Technology

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Manfred Dipl Chem Dr Reiffen

Massachusetts Institute of Technology

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Klaus Dipl Chem Dr Noll

Massachusetts Institute of Technology

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Wolfgang Wienen

Max Delbrück Center for Molecular Medicine

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