Combined logical and data-driven models for linking signalling pathways to cellular response

Signalling pathways are the cornerstone on understanding cell function and predicting cell behavior. Recently, logical models of canonical pathways have been optimised with high-throughput phosphoproteomic data to construct cell-type specific pathways. However, less is known on how signalling pathwa...

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Bibliographic Details
Published in:BMC systems biology 2011-07, Vol.5 (101), p.107-107, Article 107
Main Authors: Melas, Ioannis N, Mitsos, Alexander, Messinis, Dimitris E, Weiss, Thomas S, Alexopoulos, Leonidas G
Format: Article
Language:English
Subjects:
Analysis
Calibration
Cancer
Care and treatment
Cell Line, Tumor
Cytokines
Databases, Factual
Gene expression
Genetic aspects
Humans
Linear Models
Logic
Models, Biological
Physiological aspects
Reproducibility of Results
Signal Transduction
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Summary:Signalling pathways are the cornerstone on understanding cell function and predicting cell behavior. Recently, logical models of canonical pathways have been optimised with high-throughput phosphoproteomic data to construct cell-type specific pathways. However, less is known on how signalling pathways can be linked to a cellular response such as cell growth, death, cytokine secretion, or transcriptional activity. In this work, we measure the signalling activity (phosphorylation levels) and phenotypic behavior (cytokine secretion) of normal and cancer hepatocytes treated with a combination of cytokines and inhibitors. Using the two datasets, we construct "extended" pathways that integrate intracellular activity with cellular responses using a hybrid logical/data-driven computational approach. Boolean logic is used whenever a priori knowledge is accessible (i.e., construction of canonical pathways), whereas a data-driven approach is used for linking cellular behavior to signalling activity via non-canonical edges. The extended pathway is subsequently optimised to fit signalling and behavioural data using an Integer Linear Programming formulation. As a result, we are able to construct maps of primary and transformed hepatocytes downstream of 7 receptors that are capable of explaining the secretion of 22 cytokines. We developed a method for constructing extended pathways that start at the receptor level and via a complex intracellular signalling pathway identify those mechanisms that drive cellular behaviour. Our results constitute a proof-of-principle for construction of "extended pathways" that are capable of linking pathway activity to diverse responses such as growth, death, differentiation, gene expression, or cytokine secretion.
ISSN:1752-0509
1752-0509
DOI:10.1186/1752-0509-5-107