A systems approach to mapping transcriptional networks controlling surfactant homeostasis

A systems approach to mapping transcriptional networks controlling surfactant homeostasis

Pulmonary surfactant is required for lung function at birth and throughout life. Lung lipid and surfactant homeostasis requires regulation among multi-tiered processes, coordinating the synthesis of surfactant proteins and lipids, their assembly, trafficking, and storage in type II cells of the lung...

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Bibliographic Details
Published in:BMC genomics Vol. 11; no. 1; p. 451
Main Authors: Xu, Yan, Zhang, Minlu, Wang, Yanhua, Kadambi, Pooja, Dave, Vrushank, Lu, Long J, Whitsett, Jeffrey A
Format: Journal Article
Language:English
Published: England BioMed Central Ltd 26-07-2010
BioMed Central
BMC
Subjects:
Animals
Chromosome mapping
DNA microarrays
Gene Regulatory Networks
Genetic aspects
Health aspects
Homeostasis
Lung - metabolism
Mice
Physiological aspects
Pulmonary surfactant
Pulmonary Surfactants - metabolism
Transcription Factors - metabolism
United States
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Summary:Pulmonary surfactant is required for lung function at birth and throughout life. Lung lipid and surfactant homeostasis requires regulation among multi-tiered processes, coordinating the synthesis of surfactant proteins and lipids, their assembly, trafficking, and storage in type II cells of the lung. The mechanisms regulating these interrelated processes are largely unknown. We integrated mRNA microarray data with array independent knowledge using Gene Ontology (GO) similarity analysis, promoter motif searching, protein interaction and literature mining to elucidate genetic networks regulating lipid related biological processes in lung. A Transcription factor (TF)-target gene (TG) similarity matrix was generated by integrating data from different analytic methods. A scoring function was built to rank the likely TF-TG pairs. Using this strategy, we identified and verified critical components of a transcriptional network directing lipogenesis, lipid trafficking and surfactant homeostasis in the mouse lung. Within the transcriptional network, SREBP, CEBPA, FOXA2, ETSF, GATA6 and IRF1 were identified as regulatory hubs displaying high connectivity. SREBP, FOXA2 and CEBPA together form a common core regulatory module that controls surfactant lipid homeostasis. The core module cooperates with other factors to regulate lipid metabolism and transport, cell growth and development, cell death and cell mediated immune response. Coordinated interactions of the TFs influence surfactant homeostasis and regulate lung function at birth.
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ISSN:1471-2164
1471-2164
DOI:10.1186/1471-2164-11-451