Abstract
The majority of psychopharmaca acts by binding to G-protein coupled receptors and
thereby asserts it's action through the regulation of intracellular signaling networks.
The convergence and interactions of pathways within these networks make the detailed
signaling hard to study experimentally, and the response to a stimuli can be non-intuitive.
To approach these problems with systems biology and merging biochemical data in a
computer model to do virtual experiments with high time-resolution can shed new light
on the functioning of these networks. The phosphoprotein DARPP-32 is regulated by
several modulatory neurotransmitters, including dopamine, serotonin and adenosin,
and it's function has been proposed to be altered in schizophrenia. Moreover, the
well studied regulation of DARPP-32, and the vast amount of biochemical data makes
it a model molecule when it comes to intracellular signaling. To better understand
the interactions of the pathways that regulate DARPP-32 activation we constructed
a computer model based on experimental data. In this work we discovered unexpected
responses of DARPP-32 at fast timescales. An equally important outcome of the work
was to identify areas where additional work is needed in order to understand intracellular
signaling at the systems level, showing the need for close collaborations between
theoretical and experimental biologists.
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Correspondence
Dr. M. Lindskog
Department of Neuroscience
Karolinska Institutet
Retziusväg 8 A2:2
17177 Stockholm
Sweden
Phone: +46/8/524 87 08 1
Email: mia.lindskog@ki.se