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Featured researches published by Rüdiger Streicher.


Biochemical Journal | 2008

Inhibition of the interaction between protein phosphatase 1 glycogen-targeting subunit and glycogen phosphorylase increases glycogen synthesis in primary rat hepatocytes

Darya Zibrova; Rolf Grempler; Rüdiger Streicher; Stefan Kauschke

In Type 2 diabetes, increased glycogenolysis contributes to the hyperglycaemic state, therefore the inhibition of GP (glycogen phosphorylase), a key glycogenolytic enzyme, is one of the possibilities to lower plasma glucose levels. Following this strategy, a number of GPis (GP inhibitors) have been described. However, certain critical issues are associated with their mode of action, e.g. an impairment of muscle function. The interaction between GP and the liver glycogen targeting subunit (termed G(L)) of PP1 (protein phosphatase 1) has emerged as a new potential anti-diabetic target, as the disruption of this interaction should increase glycogen synthesis, potentially providing an alternative approach to counteract the enhanced glycogenolysis without inhibiting GP activity. We identified an inhibitor of the G(L)-GP interaction (termed G(L)-GPi) and characterized its mechanism of action in comparison with direct GPis. In primary rat hepatocytes, at elevated glucose levels, the G(L)-GPi increased glycogen synthesis similarly to direct GPis. Direct GPis significantly reduced the cellular GP activity, caused a dephosphorylation of the enzyme and decreased the amounts of GP in the glycogen-enriched fraction; the G(L)-GPi did not influence any of these parameters. Both mechanisms increased glycogen accumulation at elevated glucose levels. However, at low glucose levels, only direct GPis led to increased glycogen amounts, whereas the G(L)-GPi allowed the mobilization of glycogen because it did not block the activity of GP. Due to this characteristic, G(L)-GPi in comparison with GPis could offer an advantageous risk/benefit profile circumventing the potential downsides of a complete prevention of glycogen breakdown while retaining glucose-lowering efficacy, suggesting that inhibition of the G(L)-GP interaction may provide an attractive novel approach for rebalancing the disturbed glycogen metabolism in diabetic patients.


Biochemical Journal | 1997

INTERLEUKIN-1-INDUCED NUCLEAR FACTOR KAPPA B ACTIVATION IS INHIBITED BY OVEREXPRESSION OF PHOSPHOLIPID HYDROPEROXIDE GLUTATHIONE PEROXIDASE IN A HUMAN ENDOTHELIAL CELL LINE

Regina Brigelius-Flohé; Bärbel Friedrichs; Stefanie Maurer; Manfred Schultz; Rüdiger Streicher


Journal of Natural Products | 2004

BI-32169, a bicyclic 19-peptide with strong glucagon receptor antagonist activity from Streptomyces sp.

Olivier Potterat; Klaus Wagner; Gerd Gemmecker; Jürgen Mack; Carsten Puder; Regine Vettermann; Rüdiger Streicher


Journal of Medicinal Chemistry | 2014

Potent cholesteryl ester transfer protein inhibitors of reduced lipophilicity: 1,1'-spiro-substituted hexahydrofuroquinoline derivatives.

Thomas Trieselmann; Holger Wagner; Klaus Fuchs; Dieter Hamprecht; Daniela Berta; Paolo Cremonesi; Rüdiger Streicher; Gerd Luippold; Astrid Volz; Michael Markert; Herbert Nar


Endocrinology | 2016

Aldosterone Synthase Inhibition Improves Glucose Tolerance in Zucker Diabetic Fatty (ZDF) Rats

Anja Hofmann; Coy Brunssen; Mirko Peitzsch; Melanie Martin; Jennifer Mittag; Anett Jannasch; Felix Engelmann; Nicholas F. Brown; Steven M. Weldon; Jochen Huber; Rüdiger Streicher; Andreas Deussen; Graeme Eisenhofer; Stefan R. Bornstein; Henning Morawietz


Archive | 2005

Cyanothiophenes, the production thereof and their use as medicaments

Ralf Anderskewitz; Gerd Morschhäuser; Rüdiger Streicher; Thomas Trieselmann; Rainer Walter


Archive | 2004

Verwendung von substituierten 2-Phenylbenzimidazolen als Arzneimittel

Rüdiger Streicher; Jürgen Mack; Rainer Walter; Ingo Konetzki; Thomas Trieselmann; Volkhard Austel


Archive | 2004

Bicyclic oligopeptides and their use as glucagon receptor antagonists

Olivier Potterat; Rüdiger Streicher; Klaus Wagner; Till Maurer; Jürgen Mack; Stefan Peters


Archive | 2009

Arylsulfonylaminomethyphosphonsäure-Derivate, deren Herstellung und deren Verwendung als Arzneimittel

Elke Langkopf; Holger Wagner; Rüdiger Streicher; Corinna Schoelch; Annette Schuler-Metz; Alexander Pautsch


Archive | 2008

Neue substituierte Arylsulfonylglycine, deren Herstellung und deren Verwendung als Arzneimittel

Holger Wagner; Elke Langkopf; Matthias Eckhardt; Rüdiger Streicher; Corinna Schoelch; Annette Schuler-Metz; Alexander Pautsch

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