iTRAQ proteomic analysis of extracellular matrix remodeling in aortic valve disease

被引:37
作者
Martin-Rojas, Tatiana [1 ]
Mourino-Alvarez, Laura [1 ]
Alonso-Orgaz, Sergio [1 ]
Rosello-Lleti, Esther [2 ]
Calvo, Enrique [3 ]
Fernando Lopez-Almodovar, Luis [4 ]
Rivera, Miguel [2 ]
Padial, Luis R. [5 ]
Antonio Lopez, Juan [3 ]
de la Cuesta, Fernando [1 ]
Barderas, Maria G. [1 ]
机构
[1] SESCAM, Hosp Nacl Paraplej, Dept Vasc Physiopathol, Toledo, Spain
[2] Hosp La Fe, Hlth Res Inst, Cardiocirculatory Unit, Valencia, Spain
[3] CNIC, Prote Core Facil, Madrid, Spain
[4] SESCAM, Hosp Virgen Salud, Cardiac Surg, Toledo, Spain
[5] SESCAM, Hosp Virgen Salud, Dept Cardiol, Toledo, Spain
关键词
LEUCINE-RICH REPEAT; OSTEOBLAST-SPECIFIC FACTOR; TOLL-LIKE RECEPTOR-4; ATHEROSCLEROTIC PLAQUES; INTERSTITIAL-CELLS; PERIOSTIN; BIGLYCAN; PROTEIN; STENOSIS; EXPRESSION;
D O I
10.1038/srep17290
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Degenerative aortic stenosis (AS) is the most common worldwide cause of valve replacement. The aortic valve is a thin, complex, layered connective tissue with compartmentalized extracellular matrix (ECM) produced by specialized cell types, which directs blood flow in one direction through the heart. There is evidence suggesting remodeling of such ECM during aortic stenosis development. Thus, a better characterization of the role of ECM proteins in this disease would increase our understanding of the underlying molecular mechanisms. Aortic valve samples were collected from 18 patients which underwent aortic valve replacement (50% males, mean age of 74 years) and 18 normal control valves were obtained from necropsies (40% males, mean age of 69 years). The proteome of the samples was analyzed by 2D-LC MS/MS iTRAQ methodology. The results showed an altered expression of 13 ECM proteins of which 3 (biglycan, periostin, prolargin) were validated by Western blotting and/or SRM analyses. These findings are substantiated by our previous results demonstrating differential ECM protein expression. The present study has demonstrated a differential ECM protein pattern in individuals with AS, therefore supporting previous evidence of a dynamic ECM remodeling in human aortic valves during AS development.
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页数:12
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