The TGF-beta profibrotic cascade targets ecto-5 '-nucleotidase gene in proximal tubule epithelial cells and is a traceable marker of progressive diabetic kidney disease

Cappelli, Claudio; Tellez, Analia; Jara, Claudia; Alarcon, Sebastian; Torres, Angelo; Mendoza, Pablo; Podesta, Loreto; Flores, Claudio; Quezada, Claudia; Oyarzun, Carlos; San Martin, Rody

Abstract

Progressive diabetic nephropathy (DN) and loss of renal function correlate with kidney fibrosis. Crosstalk between TGF-beta and adenosinergic signaling contributes to the phenotypic transition of cells and to renal fibrosis in DN models. We evaluated the role of TGF-beta on NT5E gene expression coding for the ecto-5'-nucleotidase CD73, the limiting enzyme in extracellular adenosine production. We showed that high D-glucose may predispose HK-2 cells towards active transcription of the proximal promoter region of the NT5E gene while additional TGF-beta results in full activation. The epigenetic landscape of the NT5E gene promoter was modified by concurrent TGF-beta with occupancy by the p300 co-activator and the phosphorylated forms of the Smad2/3 complex and RNA Pol II. Transcriptional induction at NT5E in response to TGF-beta was earlier compared to the classic responsiveness genes PAI-1 and Fnl. CD73 levels and AMPase activity were concomitantly increased by TGF-beta in HK-2 cells. Interestingly, we found increased CD73 content in urinary extracellular vesicles only in diabetic patients with renal repercussions. Further, CD73-mediated AMPase activity was increased in the urinary sediment of DN patients. We conclude that the NT5E gene is a target of the profibrotic TGF-beta cascade and is a traceable marker of progressive DN.

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Título según WOS: The TGF-beta profibrotic cascade targets ecto-5 '-nucleotidase gene in proximal tubule epithelial cells and is a traceable marker of progressive diabetic kidney disease
Título de la Revista: BIOCHIMICA ET BIOPHYSICA ACTA-MOLECULAR BASIS OF DISEASE
Volumen: 1866
Número: 7
Editorial: Elsevier
Fecha de publicación: 2020
DOI:

10.1016/J.BBADIS.2020.165796

Notas: ISI