Genomics

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Gene Expression Profiles Characterize Inflammation Stages in the Acute Respiratory Distress Syndrome in Mice


ABSTRACT: Acute respiratory distress syndrome (ARDS) carries about a 50 percent mortality and is frequently associated with an infection (sepsis). Life-support treatment with assisted ventilation rescues many patients, although superimposed infection or multiple organ failure can result in death. The outcome of a patient developing sepsis highly depends on the degree of pre-existing inflammation prior to the infection. In this study, we describe each stage of the inflammation process using a transcriptomic approach. Female C57BL6/J mice received an intra-veinous oleic acid injection to induce an acute lung injury and lung expression patterns have been analyzed using a 9900 cDNA mouse microarray (MusV29K). Our gene-expression analysis revealed maked changes in the immune and inflammatory response metabolic pathways, notably lipid metabolism and transcription. The early pro-inflammatory stage (1H-1H30) is characterized by the release of immune response and activation of inflammatory mechanisms. Later (3H-4H), the immune cells migrate into inflamed tissues through interaction with vascular endothelial cells. Finally, at late stages of inflammation (18H-24H), metabolism is deeply disturbed. Highly expressed pro-inflammatory cytokines activate transcription of many genes as well as lipid metabolism. This global overview of critical events occuring during lung inflammation is essential to understand infectious pathologies such as sepsis where inflammation and infection are interwined. From now on, it becomes possible to isolate the impact of a pathogen at the transcriptomic level from the global gene expression modifications resulting from the infection associated with the inflammation. Also, our work allowed to identify genes involved in the response to inflammation. Among those, several may be candidate fro gene therapy.

ORGANISM(S): Mus musculus

PROVIDER: GSE18712 | GEO | 2010/08/23

SECONDARY ACCESSION(S): PRJNA121509

REPOSITORIES: GEO

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