Proteins IGFBP7 (5581 ng/mL), DSG1 (21 pg/mL), ADIPOQ (26686 ng/mL), and JUP (10.2 ng/mL) were significantly elevated (P<0.05) in severe aortic valve disease versus mild/moderate cases.
What are the differentially expressed proteins associated with severe aortic valve disease?
80 subjects including patients with aortic valve disease (mild/moderate and severe) and controls
Protein profiling using liquid chromatography-tandem mass spectrometry and ELISA
Comparisons between mild/moderate vs control, severe vs control, and severe vs mild/moderate
Differentially expressed proteins and their diagnostic value evaluated by receiver operating characteristic curvesurrogate
Increased levels of IGFBP7, DSG1, JUP, and ADIPOQ are identified as potential biomarkers for severe aortic valve disease.
Absolute Event Rate: 0% vs 0%
Background: Valvular heart disease, particularly aortic valve disease including stenosis and regurgitation, is a common heart disease. This study aimed to explore the protein profiling and the biomarkers in severe aortic valve disease and to provide new insights into the therapeutic strategy. Methods: Blood samples from 80 subjects were collected and analyzed by data independent acquisition technique in 3 comparisons (mild/moderate‐control, severe‐control, and severe–mild/moderate) and validated by ELISA. The diagnostic value of differentially expressed proteins associated with severe valvular heart disease was also evaluated by the receiver operating characteristic curve. Results: A total of 9976 peptides and 451 proteins were identified through liquid chromatography‐tandem mass spectrometry analysis. From these, 64 in mild/moderate‐control, 50 in severe‐control, and 50 in severe–mild/moderate comparisons were identified as differentially expressed proteins. IGFBP7 (insulin‐like growth factor‐binding protein 7; 5581.0±697.0 ng/mL), DSG1 (desmoglein‐1; 21.0±2.0 pg/mL), ADIPOQ (adiponectin; 26 686.0±3730 ng/mL), and JUP (junction plakoglobin; 10.2±0.6 ng/mL) levels in the severe group were significantly higher than that in the mild/moderate ( P <0.05) group. Additionally, ADIPOQ and JUP levels in the severe group were also higher than that in control ( P <0.001). Receiver operating characteristic curve analysis showed that IGFBP7, DSG1, JUP, and ADIPOQ had strong potential value to be associated with severe aortic valve disease. Conclusions: By constructing proteomics profile to identify the protein characteristics this study found that increased IGFBP7, DSG1, JUP, and ADIPOQ are the characteristics of proteins in patients with severe valvular heart disease. These findings provide new insight into the diagnosis and pathogenesis of valvular heart disease, particularly aortic valve disease.
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Chao Ni
Zhejiang University
Hai‐Tao Hou
Chinese Academy of Medical Sciences & Peking Union Medical College
Hemin Zhao
First Affiliated Hospital Zhejiang University
Journal of the American Heart Association
Zhejiang University
Chinese Academy of Medical Sciences & Peking Union Medical College
Tianjin Medical University
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Ni et al. (Tue,) reported a other. Proteins IGFBP7 (5581 ng/mL), DSG1 (21 pg/mL), ADIPOQ (26686 ng/mL), and JUP (10.2 ng/mL) were significantly elevated (P<0.05) in severe aortic valve disease versus mild/moderate cases.
synapsesocial.com/papers/69d894ce6c1944d70ce05b39 — DOI: https://doi.org/10.1161/jaha.125.047122