Nos3-/- iPSCs model concordant signatures of in utero cardiac pathogenesis [iPSCs]

GSE69316

Mus musculus

30 Downloadable Samples

Affymetrix Mouse Genome 430 2.0 Array (mouse4302)

Submitter Supplied Information

Description

Through genome-wide transcriptional comparisons, this study interrogates the capacity of iPSCs to accurately model pathogenic signatures of structural cardiac defects. Herein, we studied the molecular etiology of structural cardiac defects in Nos3-/- mice via transcriptional analysis of stage-matched embryonic and iPSC-derived tissues. In vitro comparisons of differentiated embryoid bodies were calibrated to in utero benchmarks of health and disease. Integrated systems biology analysis of WT and Nos3-/- transcriptional profiles revealed 50% concordant expression patterns between in utero embryonic and ex vivo iPSC-derived tissue. In particular, up-regulation of glucose metabolism (p-value = 3.95x10-12) and down-regulation of fatty acid metabolism (p-value = 6.71x10-12) highlight a bioenergetic signature of early Nos3 deficiency during cardiogenesis that can be recapitulated in iPSC-derived tissues. The in vitro concordance of early Nos3-/- disease signatures supports the utility of iPSCs as a cell-autonomous model of structural heart defects. Moreover, this study supports the use of iPSCs as a platform to pinpoint initial stages of cardiac pathogenesis.

PubMed ID

26344701

Publication Title

Nos3-/- iPSCs model concordant signatures of in utero cardiac pathogenesis.

Total Samples

Submitter’s Institution

Mayo Clinic

Authors

Campbell KA, Li X, Biendarra SM, Terzic A, Nelson TJ

Source Repository

Gene Expression Omnibus (GEO)

Alternate Accession IDs

E-GEOD-69316

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