Brazilian Journal of Nephrology (May 2018)

Biomarkers of cardio-renal syndrome in uremic myocardiopathy animal model

  • Laura Mattana Dionísio,
  • Mateus Justi Luvizoto,
  • Caroline Gribner,
  • Danielle Carneiro,
  • Viviane Carvalho,
  • Franciele Robes,
  • Marcos Sheidemantel,
  • Fabiane Rego,
  • Lúcia de Noronha,
  • Roberto Pecoits-Filho,
  • Aline Borsato Hauser

DOI
https://doi.org/10.1590/2175-8239-jbn-3878
Journal volume & issue
no. 0

Abstract

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ABSTRACT Introduction: Cardio-renal syndrome subtype 4 (CRS4) is a condition of primary chronic kidney disease that leads to reduction of cardiac function, ventricular hypertrophy, and risk of cardiovascular events. Objective: Our aim was to understand the mechanisms involved on the onset of CRS4. Methods: We used the nephrectomy 5/6 (CKD) animal model and compared to control (SHAM). Serum biomarkers were analyzed at baseline, 4, and 8 weeks. After euthanasia, histology and immunohistochemistry were performed in the myocardium. Results: Troponin I (TnI) was increased at 4 weeks (W) and 8W, but nt-proBNP showed no difference. The greater diameter of cardiomyocytes indicated left ventricular hypertrophy and the highest levels of TNF-α were found at 4W declining in 8W while fibrosis was more intense in 8W. Angiotensin expression showed an increase at 8W. Conclusions: TnI seems to reflect cardiac injury as a consequence of the CKD however nt-proBNP did not change because it reflects stretching. TNF-α characterized an inflammatory peak and fibrosis increased over time in a process connecting heart and kidneys. The angiotensin showed increased activity of the renin-angiotensin axis and corroborates the hypothesis that the inflammatory process and its involvement with CRS4. Therefore, this animal study reinforces the need for renin-angiotensin blockade strategies and the control of CKD to avoid the development of CRS4.

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