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Dive into the research topics where Eija Tiainen is active.

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Featured researches published by Eija Tiainen.


Chemical Biology & Drug Design | 2013

Discovery and Structural Characterization of a Phospholamban-Binding Cyclic Peptide and Design of Novel Inhibitors of Phospholamban

Carola Tilgmann; Piero Pollesello; Martti Ovaska; Juha Kaivola; Jarmo Pystynen; Eija Tiainen; Marjo Yliperttula; Arto Annila; Jouko Levijoki

The interplay between cardiac sarcoplasmic Ca2+ATPase and phospholamban is a key regulating factor of contraction and relaxation in the cardiac muscle. In heart failure, aberrations in the inhibition of sarcoplasmic Ca2+ATPase by phospholamban are associated with anomalies in cardiac functions. In experimental heart failure models, modulation of the interaction between these two proteins has been shown to be a potential therapeutic approach. The aim of our research was to find molecules able to interfere with the inhibitory activity of phospholamban on sarcoplasmic Ca2+ATPase. For this purpose, a portion of phospholamban was synthesized and used as target for a phage‐display peptide library screening. The cyclic peptide C‐Y‐W‐E‐L‐E‐W‐L‐P‐C‐A was found to bind to phospholamban (1–36) with high specificity. Its functional activity was tested in Ca2+uptake assays utilizing preparations from cardiac sarcoplasmic reticulum. By synthesizing and testing a series of alanine point‐mutated cyclic peptides, we identified which amino acid was important for the inhibition of the phospholamban function. The structures of active and inactive alanine‐mutated cyclic peptides, and of phospholamban (1–36), were determined by NMR. This structure–activity analysis allowed building a model of phospholamban –cyclic peptide complex. Thereafter, a simple pharmacophore was defined and used for the design of small molecules. Finally, examples of such molecules were synthesized and characterized as phospholamban inhibitors.


Archive | 2006

New pharmaceutical compounds

Marko Ahlmark; Reijo Bäckström; Anne Maria Luiro; Jarmo Pystynen; Eija Tiainen


Archive | 1999

Phospholamban inhibitors and a method for increasing coronary flow

Jarmo Pystynen; Heimo Haikala; Petri Kaheinen; Juha Kaivola; Piero Pollesello; Ismo Ulmanen; Jukka Tenhunen; Carola Tilgmann; Eija Tiainen; Kari Lönnberg; Pentti Nore; Seppo Parhi; Arto Karjalainen; Jouko Levijoki


Archive | 2002

New compounds, which are potent inhibitors of na+/ca2+ exchange mechanism and are useful in the treatment of arrhythmias

Tuula Koskelainen; Leena Otsomaa; Arto Johannes Karjalainen; Pekka Kotovuori; Jukka Tenhunen; Sirpa Rasku; Pentti Nore; Eija Tiainen; Olli Törmäkangas


Archive | 1998

Bisethers of 1-oxa, aza and thianaphthalen-2-ones as phospholamban inhibitors

Jarmo Pystynen; Eija Tiainen; Kari Lönnberg; Pentti Nore; Seppo Parhi; Arto Johannes Karjalainen; Heimo Haikala; Jouko Levijoki


Archive | 2013

CATECHOL O-METHYLTRANSFERASE ACTIVITY INHIBITING COMPOUNDS

Marko Ahlmark; David Din Belle; Mika Kauppala; Anne Maria Luiro; Taina Pajunen; Jarmo Pystynen; Eija Tiainen; Matti Vaismaa; Josef Messinger


Archive | 2017

compostos inibidores da atividade de catecol o-metiltransferase

Anne Maria Luiro; David Din Belle; Eija Tiainen; Jarmo Pystynen; Josef Messinger; Marko Ahlmark; Matti Vaismaa; Mika Kauppala; Taina Pajunen


Archive | 2016

COMPUESTOS NO ESTEROIDEOS INHIBIDORES DE CYP17 / ANTIANDRÓGENOS

Eija Tiainen; Emilia Visnen; Anssi Haikarainen; Pekka Pietikinen; Mikko Passiniemi; Arja Karjalainen; Petteri Rummakko; Gerd Wohlfahrt


Archive | 2015

COMPUESTOS INHIBIDORES DE LA ACTIVIDAD DE LA CATECOL O-METILTRANSFERASA

Matti Vaismaa; Josef Messinger; Jarmo Pystynen; David Din Belle; Mika Kauppala; Anne Maria Luiro; Taina Pajunen; Eija Tiainen; Marko Ahlmark


Archive | 2014

NOVEL CYP17 INHIBITORS/ANTIANDROGENS

Gerd Wohlfahrt; Petteri Rummakko; Arja Karjalainen; Mikko Passiniemi; Pekka Pietikäinen; Anssi Haikarainen; Emilia Väisänen; Eija Tiainen

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