Narendra Panday
Hoffmann-La Roche
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Publication
Featured researches published by Narendra Panday.
Bioorganic & Medicinal Chemistry Letters | 2010
Lillli Anselm; David W. Banner; Jörg Benz; Katrin Groebke Zbinden; Jacques Himber; Hans Hilpert; Walter Huber; Bernd Kuhn; Jean-Luc Mary; Michael B. Otteneder; Narendra Panday; Fabienne Ricklin; Martin Stahl; Stefan Thomi; Wolfgang Haap
A series of (3R,4R)-pyrrolidine-3,4-dicarboxylic acid amides was investigated with respect to their factor Xa inhibitory activity, selectivity, pharmacokinetic properties, and ex vivo antithrombotic activity. The clinical candidate from this series, R1663, exhibits excellent selectivity against a panel of serine proteases and good pharmacokinetic properties in rats and monkeys. A Phase I clinical study with R1663 has been finalized.
Bioorganic & Medicinal Chemistry Letters | 2009
Hassen Ratni; Denise Blum-Kaelin; Henrietta Dehmlow; Peter Hartman; Philippe Jablonski; Raffaello Masciadri; Cyrille Maugeais; Angelique Patiny-Adam; Narendra Panday; Matthew Blake Wright
A series of tetrahydro-cyclopenta[b]indoles modulating the activity of the liver-X-receptor (LXR) were derived from a high throughput screening hit. The potency and selectivity for LXRbeta versus LXRalpha was improved. One compound, administered to wild-type mice modestly increased plasma HDL-cholesterol with no change in plasma triglycerides (TG) and reduced effects on liver TG content compared to T0901317. This novel series of LXR agonists shows promise to improve therapeutic efficacy with reduced potential to increase TG.
European Journal of Medicinal Chemistry | 2009
Katrin Groebke Zbinden; Lilli Anselm; David W. Banner; Jörg Benz; Francesca Blasco; Guillaume Décoret; Jacques Himber; Bernd Kuhn; Narendra Panday; Fabienne Ricklin; Philippe Risch; Daniel Schlatter; Martin Stahl; Stefan Thomi; Robert Unger; Wolfgang Haap
Starting from a hit identified by focused screening, 3-aminopyrrolidine factor Xa inhibitors were designed. The binding mode as determined by X-ray structural analysis as well as the pharmacokinetic behaviour of selected compounds is discussed.
Chimia | 2005
Henrietta Dehmlow; Jean Ackermann; Johannes Aebi; Denise Blum-Kaelin; Alexander Chucholowski; Philippe Coassolo; Peter Hartman; Manfred Kansy; Hans Peter Märki; Olivier Morand; Elisabeth von der Mark; Narendra Panday; Armin Ruf; Ralf Thoma; Tanja Schulz-Gasch
Novel inhibitors of oxidosqualene cyclase (OSC) for the treatment of dyslipidemia are reported. Starting point for the chemistry program was a set of compounds derived from a fungicide project which, in addition to high affinity for OSC from Candida albicans, also showed high affinity for the human enzyme (hOSC). Here the evaluation process of different scaffolds is outlined for two representative series, the phenyl substituted benzo[d]isothiazoles and the aminocyclohexanes. The most promising compounds derived from the latter series were further profiled in vivo and showed promising properties with respect to modulation of lipid parameters.
Archive | 2005
Henrietta Dehmlow; Bernd Kuhn; Narendra Panday; Hasane Ratni; Tanja Schulz-Gasch; Matthew Blake Wright
Archive | 2005
Henrietta Dehmlow; Bernd Kuhn; Raffaello Masciadri; Narendra Panday; Hasane Ratni; Matthew Blake Wright
Tetrahedron Letters | 2005
Sally J. Oxenford; Jonathan M. Wright; Peter O’Brien; Narendra Panday; Mark R. Shipton
Archive | 2005
Henrietta Dehmlow; Bernd Kuhn; Narendra Panday; Hasane Ratni; Matthew Blake Wright
Archive | 2007
Gregory Martin Benson; Konrad Bleicher; Alexander Chucholowski; Henrietta Dehmlow; Uwe Grether; Bernd Kuhn; Rainer E. Martin; Eric J. Niesor; Narendra Panday; Hans Richter; Franz Schuler; Xavier Warot; Matthew Blake Wright; Minmin Yang
Archive | 2006
Markus Boehringer; Zbinden Katrin Groebke; Wolfgang Haap; Narendra Panday; Fabienne Ricklin; Martin Stahl; Petra Schmitz
