Dipeptidyl peptidase 4 promotes peritoneal fibrosis and its inhibitions prevent failure of peritoneal dialysis.
Yi-Chen LiPei-Hsun SungYao-Hsu YangJohn Y ChiangHon-Kan YipChih-Chao YangPublished in: Communications biology (2021)
Peritoneal dialysis (PD) possesses multiple advantages for end stage renal disease. However, long-term PD triggers peritoneal fibrosis (PF). From the nationwide analysis of diabetic PD patients (n = 19,828), we identified the incidence of PD failure was significantly lower in diabetic patients treated with dipeptidyl peptidase 4 (DPP4) inhibitors. Experimental study further showed high concentration of glucose remarkably enhanced DPP4 to promote epithelial-mesenchymal transition (EMT) in the mesothelial cells. In chlorhexidine gluconate (CG)-induced PF model of rats, DPP4 expression was enriched at thickening peritoneum. Moreover, as to CG-induced PF model, DPP4 deficiency (F344/DuCrlCrlj strain), sitagliptin and exendin-4 treatments significantly inhibited DPP4 to reverse the EMT process, angiogenesis, oxidative stress, and inflammation, resulting in the protection from PF, preservation of peritoneum and the corresponding functional integrity. Furthermore, DPP4 activity was significantly correlated with peritoneal dysfunction. Taken together, DPP4 caused peritoneal dysfunction/PF, whereas inhibition of DPP4 protected the PD patients against PD failure.
Keyphrases
- end stage renal disease
- peritoneal dialysis
- chronic kidney disease
- oxidative stress
- epithelial mesenchymal transition
- diabetic rats
- induced apoptosis
- type diabetes
- poor prognosis
- high glucose
- transforming growth factor
- newly diagnosed
- risk factors
- ejection fraction
- cross sectional
- dna damage
- wound healing
- adipose tissue
- metabolic syndrome
- ischemia reperfusion injury
- prognostic factors
- drug induced
- blood glucose
- patient reported outcomes
- stress induced
- binding protein