Peter Söderman
AstraZeneca
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Publication
Featured researches published by Peter Söderman.
Journal of Medicinal Chemistry | 2012
Stefan Berg; Margareta Bergh; Sven Hellberg; Katharina Högdin; Y. Lo-Alfredsson; Peter Söderman; S. von Berg; T. Weigelt; Mats Ormö; Yafeng Xue; J. Tucker; Jan Neelissen; E. Jerning; Yvonne Nilsson; Ratan Bhat
Glycogen synthase kinase-3β, also called tau phosphorylating kinase, is a proline-directed serine/threonine kinase which was originally identified due to its role in glycogen metabolism. Active forms of GSK3β localize to pretangle pathology including dystrophic neuritis and neurofibrillary tangles in Alzheimers disease (AD) brain. By using a high throughput screening (HTS) approach to search for new chemical series and cocrystallization of key analogues to guide the optimization and synthesis of our pyrazine series, we have developed highly potent and selective inhibitors showing cellular efficacy and blood-brain barrier penetrance. The inhibitors are suitable for in vivo efficacy testing and may serve as a new treatment strategy for Alzheimers disease.
Journal of Medicinal Chemistry | 2012
Britt-Marie Swahn; Karin Kolmodin; Sofia Karlström; Stefan Berg; Peter Söderman; Jörg Holenz; Johan Lindström; M. Sundstrom; Jacob Kihlström; Can Slivo; Lars I. Andersson; David Pyring; Didier Rotticci; Liselotte Öhberg; Annika Kers; Krisztián Bogár; Fredrik von Kieseritzky; Margareta Bergh; Lise-Lotte Olsson; Juliette Janson; Susanna Eketjäll; Biljana Georgievska; Fredrik Jeppsson; Johanna Fälting
The evaluation of a series of aminoisoindoles as β-site amyloid precursor protein cleaving enzyme 1 (BACE1) inhibitors and the discovery of a clinical candidate drug for Alzheimers disease, (S)-32 (AZD3839), are described. The improvement in permeability properties by the introduction of fluorine adjacent to the amidine moiety, resulting in in vivo brain reduction of Aβ40, is discussed. Due to the basic nature of these compounds, they displayed affinity for the human ether-a-go-go related gene (hERG) ion channel. Different ways to reduce hERG inhibition and increase hERG margins for this series are described, culminating in (S)-16 and (R)-41 showing large in vitro margins with BACE1 cell IC(50) values of 8.6 and 0.16 nM, respectively, and hERG IC(50) values of 16 and 2.8 μM, respectively. Several compounds were advanced into pharmacodynamic studies and demonstrated significant reduction of β-amyloid peptides in mouse brain following oral dosing.
Chemistry & Biodiversity | 2012
Ulrika Yngve; Peter Söderman; Mats Svensson; Susanne Rosqvist; Per I. Arvidsson
In this study, we explored the effect of bioisostere replacement in a series of glycogen synthase kinase 3 (GSK3) inhibitors based on the imidazopyridine core. The synthesis and biological evaluation of a number of novel sulfonamide, 1,2,4‐oxadiazole, and thiazole derivates as amide bioisosteres, as well as a computational rationalization of the obtained results are reported.
Archive | 2003
Stefan Berg; Sven Hellberg; Peter Söderman
Archive | 2006
Per I. Arvidsson; Erwan Arzel; Jeremy N. Burrows; Helena Gyback; Tobias Rein; Didier Rotticci; Peter Söderman
Archive | 2006
Per I. Arvidsson; Erwan Arzel; Jeremy N. Burrows; Martina Claesson; Colin Ray; Tobias Rein; Didier Rotticci; Peter Söderman
Archive | 2009
Jörg Holenz; Sofia Karlström; Jacob Kihlström; Karin Kolmodin; Johan Lindström; Laszlo Rakos; Didier Rotticci; Peter Söderman; M. Sundstrom; Britt-Marie Swahn; Berg Stefan Von
Archive | 2013
Gabor Csjernyik; Sofia Karlström; Annika Kers; Karin Kolmodin; Martin Nylöf; Liselotte Öhberg; Laszlo Rakos; Lars Sandberg; Fernando Sehgelmeble; Peter Söderman; Britt-Marie Swahn; Stefan Berg
Archive | 2009
Jörg Holenz; Sofia Karlström; Jacob Kihlström; Karin Kolmodin; Laszlo Rakos; Peter Söderman; Britt-Marie Swahn; Stefan Berg; Fredrik von Kieseritzky
Archive | 2007
Stefan Berg; Sofia Karlström; Karin Kolmodin; Johan Lindström; Jan-Erik Nyström; Fernando Sehgelmeble; Peter Söderman