Genome-scale modeling and in silico analysis of mouse cell metabolic network

被引:54
|
作者
Selvarasu, Suresh [1 ,2 ]
Karimi, Iftekhar A. [1 ]
Ghim, Ghi-Hoon [3 ]
Lee, Dong-Yup [1 ,2 ]
机构
[1] Natl Univ Singapore, Dept Chem & Biomol Engn, Singapore 117576, Singapore
[2] ASTAR, Ctr Bioproc Technol, Singapore 138668, Singapore
[3] Cyram Co Ltd, Network Res Inst, SNU Res Pk Innovat Ctr, Seoul 151818, South Korea
关键词
SYSTEMS BIOTECHNOLOGY; DRUG DISCOVERY; RECONSTRUCTION; BIOLOGY; GROWTH; GLYCOSYLATION; VALIDATION; PREDICTION; GLUTAMINE; MECHANISM;
D O I
10.1039/b912865d
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Genome-scale metabolic modeling has been successfully applied to a multitude of microbial systems, thus improving our understanding of their cellular metabolisms. Nevertheless, only a handful of works have been done for describing mammalian cells, particularly mouse, which is one of the important model organisms, providing various opportunities for both biomedical research and biotechnological applications. Presented herein is a genome-scale mouse metabolic model that was systematically reconstructed by improving and expanding the previous generic model based on integrated biochemical and genomic data of Mus musculus. The key features of the updated model include additional information on gene-protein-reaction association, and improved network connectivity through lipid, amino acid, carbohydrate and nucleotide biosynthetic pathways. After examining the model predictability both quantitatively and qualitatively using constraints-based flux analysis, the structural and functional characteristics of the mouse metabolism were investigated by evaluating network statistics/centrality, gene/metabolite essentiality and their correlation. The results revealed that overall mouse metabolic network is topologically dominated by highly connected and bridging metabolites, and functionally by lipid metabolism that most of essential genes and metabolites are from. The current in silico mouse model can be exploited for understanding and characterizing the cellular physiology, identifying potential cell engineering targets for the enhanced production of recombinant proteins and developing diseased state models for drug targeting.
引用
收藏
页码:152 / 161
页数:10
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