A critical evaluation of methods for the reconstruction of tissue-specific models

C Gille; JD Orth; L Jerby; L Jerby; M Uhlen; MA Oberhardt; MN McCall; NC Duarte; NC Duarte; NE Lewis; P Flicek; R Agren; R Agren; R Kaddurah-Daouk; S Sahoo; S Sahoo; T Barrett; T Hao; T Shlomi; T Shlomi; Y Wang

research

A critical evaluation of methods for the reconstruction of tissue-specific models

Authors: C Gille
JD Orth
L Jerby
L Jerby
M Uhlen
MA Oberhardt
MN McCall
NC Duarte
NC Duarte
NE Lewis
P Flicek
R Agren
R Agren
R Kaddurah-Daouk
S Sahoo
S Sahoo
T Barrett
T Hao
T Shlomi
T Shlomi
Y Wang
Publication date: 1 January 2015
Publisher: 'Springer Science and Business Media LLC'
Doi

Abstract

Under the framework of constraint based modeling, genome-scale metabolic models (GSMMs) have been used for several tasks, such as metabolic engineering and phenotype prediction. More recently, their application in health related research has spanned drug discovery, biomarker identification and host-pathogen interactions, targeting diseases such as cancer, Alzheimer, obesity or diabetes. In the last years, the development of novel techniques for genome sequencing and other high-throughput methods, together with advances in Bioinformatics, allowed the reconstruction of GSMMs for human cells. Considering the diversity of cell types and tissues present in the human body, it is imperative to develop tissue-specific metabolic models. Methods to automatically generate these models, based on generic human metabolic models and a plethora of omics data, have been proposed. However, their results have not yet been adequately and critically evaluated and compared. This work presents a survey of the most important tissue or cell type specific metabolic model reconstruction methods, which use literature, transcriptomics, proteomics and metabolomics data, together with a global template model. As a case study, we analyzed the consistency between several omics data sources and reconstructed distinct metabolic models of hepatocytes using different methods and data sources as inputs. The results show that omics data sources have a poor overlapping and, in some cases, are even contradictory. Additionally, the hepatocyte metabolic models generated are in many cases not able to perform metabolic functions known to be present in the liver tissue. We conclude that reliable methods for a priori omics data integration are required to support the reconstruction of complex models of human cells.Acknowledgments. S.C. thanks the FCT for the Ph.D. Grant SFRH/BD/ 80925/2011. The authors thank the FCT Strategic Project of UID/BIO/04469/2013 unit, the project RECI/BBB-EBI/0179/2012 (FCOMP-01-0124-FEDER-027462) and the project “BioInd - Biotechnology and Bioengineering for improved Industrial and Agro-Food processes”, REF. NORTE-07-0124-FEDER-000028 Co-funded by the Programa Operacional Regional do Norte (ON.2 - O Novo Norte), QREN, FEDER