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Dive into the research topics where Annika Björe is active.

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Featured researches published by Annika Björe.


Drug Discovery Today | 2009

Making medicinal chemistry more effective—application of Lean Sigma to improve processes, speed and quality

Shalini Andersson; Alan Armstrong; Annika Björe; Sue Bowker; Steve Chapman; Robert D. M. Davies; Craig S. Donald; Bryan J. Egner; Thomas Elebring; Sara Holmqvist; Tord Inghardt; Petra Johannesson; Magnus Johansson; Craig Johnstone; Paul D. Kemmitt; Jan Kihlberg; Pernilla Korsgren; Malin Lemurell; Jane E. Moore; Jonas Pettersson; Helen Pointon; Paul Schofield; Nidhal Selmi; Paul R.O. Whittamore

The pharmaceutical industry, particularly the small molecule domain, faces unprecedented challenges of escalating costs, high attrition as well as increasing competitive pressure from other companies and from new treatment modes such as biological products. In other industries, process improvement approaches, such as Lean Sigma, have delivered benefits in speed, quality and cost of delivery. Examining the medicinal chemistry contributions to the iterative improvement process of design-make-test-analyse from a Lean Sigma perspective revealed that major improvements could be made. Thus, the cycle times of synthesis, as well as compound analysis and purification, were reduced dramatically. Improvements focused on team, rather than individual, performance. These new ways of working have consequences for staff engagement, goals, rewards and motivation, which are also discussed.


Bioorganic & Medicinal Chemistry Letters | 2013

Synthesis and evaluation of diphenylphosphinic amides and diphenylphosphine oxides as inhibitors of Kv1.5.

Roine I. Olsson; Ingemar Jacobson; Jonas Boström; Tomas Fex; Annika Björe; Christina Olsson; Johan Sundell; Ulrik Gran; Anna Öhrn; Andreas Nordin; Jonna Gyll; Maria Thorstensson; Ahlke Hayen; Karolina Aplander; Olle Hidestål; Fanyi Jiang; Gunilla Linhardt; Elin Forsström; Teresa Collins; Monika Sundqvist; Emma Lindhardt; Annika Åstrand; Boel Löfberg

Diphenylphosphinic amides and diphenylphosphine oxides have been synthesized and tested as inhibitors of the Kv1.5 potassium ion channel as a possible treatment for atrial fibrillation. In vitro structure-activity relationships are discussed and several compounds with Kv1.5 IC(50) values of <0.5 μM were discovered. Selectivity over the ventricular IKs current was monitored and selective compounds were found. Results from a rabbit PD-model are included.


Bioorganic & Medicinal Chemistry Letters | 2014

Lactam sulfonamides as potent inhibitors of the Kv1.5 potassium ion channel

Roine I. Olsson; Ingemar Jacobson; Tommy Iliefski; Jonas Boström; Öjvind Davidsson; Ola Fjellström; Annika Björe; Christina Olsson; Johan Sundell; Ulrik Gran; Jonna Gyll; Jesper Malmberg; Olle Hidestål; Hans Emtenäs; Tor Svensson; Zhong-Qing Yuan; Gert Strandlund; Annika Åstrand; Emma Lindhardt; Gunilla Linhardt; Elin Forsström; Ågot Högberg; Frida Persson; Birgit Andersson; Anna Rönnborg; Boel Löfberg

A series of lactam sulfonamides has been discovered and optimized as inhibitors of the Kv1.5 potassium ion channel for treatment of atrial fibrillation. In vitro structure-activity relationships from lead structure C to optimized structure 3y are described. Compound 3y was evaluated in a rabbit PD-model and was found to selectively prolong the atrial effective refractory period at submicromolar concentrations.


Bioorganic & Medicinal Chemistry Letters | 2016

Isoindolinone compounds active as Kv1.5 blockers identified using a multicomponent reaction approach

Johan Kajanus; Ingemar Jacobson; Annika Åstrand; Roine I. Olsson; Ulrik Gran; Annika Björe; Ola Fjellström; Öjvind Davidsson; Hans Emtenäs; Anders Dahlén; Boel Löfberg; Zhong-Qing Yuan; Johan Sundell; Johan Cassel; Jonna Gyll; Tommy Iliefski; Ågot Högberg; Emma Lindhardt; Jesper Malmberg

A series of isoindolinone compounds have been developed showing good in vitro potency on the Kv1.5 ion channel. By modification of two side chains on the isoindolinone scaffold, metabolically stable compounds with good in vivo PK profile could be obtained leaving the core structure unsubstituted. In this way, low microsomal intrinsic clearance (CLint) could be achieved despite a relatively high logD. The compounds were synthesized using the Ugi reaction, in some cases followed by Suzuki and Diels-Alder reactions, giving a diverse set of compounds in a small number of reaction steps.


Archive | 1998

Novel bispidine antiarrhythmic compounds

Gert Strandlund; Christer Alstermark; Annika Björe; Magnus Björsne; Marianne Frantsi; Torbjörn Halvarsson; Kurt-Jürgen Hoffmann; Eva-Lotte Lindstedt; Magnus Polla


Archive | 2006

New oxabispidine compounds useful in the treatment of cardiac arrhythmias

Annika Björe; Magnus Björsne; David Cladingboel; Kurt-Jürgen Hoffmann; John Pavey; Gert Strandlund; Peder Svensson; Colin Thomson; Michael Wilsterman


Archive | 2007

Isoindoline Derivatives For The Treatment Of Arrhythmias

Annika Björe; Jonas Boström; Öjvind Davidsson; Hans Emtenäs; Ulrik Gran; Tommy Iliefski; Johan Kajanus; Roine I. Olsson; Lars Sandberg; Gert Strandlund; Johan Sundell; Zhong-Qing Yuan


Archive | 2002

3,7-diazabicyclo [3.3.1] formulations as antiarhythmic compounds

Neil Barnwell; Annika Björe; Lal Cheema; David Cladingboel; Adam Herring; Karin Lövqvist


Archive | 2003

New bispidine compounds and their use in the treatment of cardiac arrhythmias

Kjell H. Andersson; Annika Björe; Magnus Björsne; Gert Strandlund; Peder Svensson; Louise Tottie


Archive | 2006

New oxabispidine compounds for the treatment of cardiac arrhythmias

Annika Björe; David Cladingboel; Gareth AstraZeneca R D Charnwood Ensor; Adam Herring; Johan Kajanus; Robert Lundqvist; Christina Olsson; Carl-Gustav Sigfridsson; Gert Strandlund

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