Issue 5, 2012

Construction of large signaling pathways using an adaptive perturbation approach with phosphoproteomic data

Abstract

Construction of large and cell-specific signaling pathways is essential to understand information processing under normal and pathological conditions. On this front, gene-based approaches offer the advantage of large pathway exploration whereas phosphoproteomic approaches offer a more reliable view of pathway activities but are applicable to small pathway sizes. In this paper, we demonstrate an experimentally adaptive approach to construct large signaling pathways from phosphoproteomic data within a 3-day time frame. Our approach—taking advantage of the fast turnaround time of the xMAP technology—is carried out in four steps: (i) screen optimal pathway inducers, (ii) select the responsive ones, (iii) combine them in a combinatorial fashion to construct a phosphoproteomic dataset, and (iv) optimize a reduced generic pathway via an Integer Linear Programming formulation. As a case study, we uncover novel players and their corresponding pathways in primary human hepatocytes by interrogating the signal transduction downstream of 81 receptors of interest and constructing a detailed model for the responsive part of the network comprising 177 species (of which 14 are measured) and 365 interactions.

Graphical abstract: Construction of large signaling pathways using an adaptive perturbation approach with phosphoproteomic data

Supplementary files

Additions and corrections

Article information

Article type
Paper
Submitted
21 Nov 2011
Accepted
28 Feb 2012
First published
23 Mar 2012

Mol. BioSyst., 2012,8, 1571-1584

Construction of large signaling pathways using an adaptive perturbation approach with phosphoproteomic data

I. N. Melas, A. Mitsos, D. E. Messinis, T. S. Weiss, J. Rodriguez and L. G. Alexopoulos, Mol. BioSyst., 2012, 8, 1571 DOI: 10.1039/C2MB05482E

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