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Urinary proteomic biomarkers to predict cardiovascular events

  • Catriona E. Brown
  • , Nina S. McCarthy
  • , Alun D. Hughes
  • , Peter Sever
  • , Angelique Stalmach
  • , William Mullen
  • , Anna F. Dominiczak
  • , Naveed Sattar
  • , Harald Mischak
  • , Simon Thom
  • , Jamil Mayet
  • , Alice V. Stanton
  • , Christian Delles

نتاج البحث: Articleمراجعة النظراء

35 اقتباسات (Scopus)

ملخص

Purpose: We have previously demonstrated associations between the urinary proteome profile and coronary artery disease (CAD) in cross-sectional studies. Here, we evaluate the potential of a urinary proteomic panel as a predictor of CAD in the hypertensive atherosclerotic cardiovascular disease (HACVD) substudy population of the Anglo-Scandinavian Cardiac Outcomes Trial study. Experimental design: Thirty-seven cases with primary CAD endpoint were matched for sex and age to controls who had not reached a CAD endpoint during the study. Spot urine samples were analyzed using CE coupled to Micro-TOF MS. A previously developed 238-marker CE-MS model for diagnosis of CAD (CAD238) was assessed for its predictive potential. Results: Sixty urine samples (32 cases; 28 controls; 88% male, mean age 64 ± 5 years) were analyzed. There was a trend toward healthier values in controls for the CAD model classifier (-0.432 ± 0.326 versus -0.587 ± 0.297, p = 0.170), and the CAD model showed statistical significance on Kaplan-Meier survival analysis p = 0.021. We found 190 individual markers out of 1501 urinary peptides that separated cases and controls (AUC >0.6). Of these, 25 peptides were also components of CAD238. Conclusion and clinical relevance: A urinary proteome panel originally developed in a cross-sectional study predicts CAD endpoints independent of age and sex in a well-controlled prospective study.

اللغة الأصليةEnglish
الصفحات (من إلى)610-617
عدد الصفحات8
دوريةProteomics - Clinical Applications
مستوى الصوت9
رقم الإصدار5-6
المعرِّفات الرقمية للأشياء
حالة النشرPublished - 1 يونيو 2015

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