Mediators of Inflammation (Jan 2015)

TGF-Beta Blockade Increases Renal Inflammation Caused by the C-Terminal Module of the CCN2

  • Raquel Rodrigues-Díez,
  • Sandra Rayego-Mateos,
  • Macarena Orejudo,
  • Luiz Stark Aroeira,
  • Rafael Selgas,
  • Alberto Ortiz,
  • Jesús Egido,
  • Marta Ruiz-Ortega

DOI
https://doi.org/10.1155/2015/506041
Journal volume & issue
Vol. 2015

Abstract

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The CCN family member 2 (CCN2, also known as connective tissue growth factor) may behave as a risk biomarker and a potential therapeutic target for renal disease. CCN2 participates in the regulation of inflammation and fibrosis. TGF-β is considered the main fibrogenic cytokine; however, in some pathological settings TGF-β also has anti-inflammatory properties. CCN2 has been proposed as a downstream profibrotic mediator of TGF-β, but data on TGF-β role in CCN2 actions are scarce. Our aim was to evaluate the effect of TGF-β blockade in CCN2-mediated experimental renal damage. Systemic administration of the C-terminal module of CCN2 to mice caused sustained renal inflammation. In these mice, TGF-β blockade, using an anti-TGF-β neutralizing antibody, significantly increased renal expression of the NGAL (a kidney injury biomarker), kidney infiltration by monocytes/macrophages, and upregulation of MCP-1 expression. The anti-inflammatory effect of TGF-β seems to be mediated by a dysregulation of the systemic Treg immune response, shown by decreased levels of circulating CD4+/Foxp3+Treg cells. Our experimental data support the idea that TGF-β exerts anti-inflammatory actions in the kidney and suggest that it is not an optimal therapeutic target.