Aims The pathogenesis of disease progression targets for patients with heart failure after acute myocardial infarction was investigated by using plasma proteomics. Methods proteomes (MI-HF) and without (MI-WHF) were compared. Each group consisted 10 who matched age sex. peptides analyzed 2-dimensional liquid chromatography coupled to tandem mass spectrometry in a high definition mode. Parallel reaction monitoring (PRM) verified the selected target proteins. Results We identified quantified 2,589 2,222 proteins, respectively, found 117 differentially expressed proteins (DEPs) (≥1.5-fold), when MI-HF MI-WHF groups Of these 51 66 significantly up-regulated down-regulated, respectively. significant DEPs subjected protein–protein interaction network analysis which revealed central role NF-κB signaling pathway patients. PRM that MB, DIAPH1, VNN1, GOT2, SLC4A1, CRP, CKM, SOD3, F7, DLD, PGAM2, GOT1, UBA7 HYOU1 14 highly Conclusions These findings showed related poor outcomes experiencing MI-HF. may be useful candidate markers diagnosis as well help elucidate pathophysiology this major cause mortality older

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