4.7 Review

Preventing peritoneal membrane fibrosis in peritoneal dialysis patients

Journal

KIDNEY INTERNATIONAL
Volume 90, Issue 3, Pages 515-524

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.kint.2016.03.040

Keywords

biocompatibility; interventions; peritoneal fibrosis; peritoneal fluids; peritoneal inflammation

Funding

  1. National Natural Science Foundation [81130012, 81470942]
  2. National Basic Research Program of China [2012CB517706]
  3. Foundation of Sun Yat-sen University, China [15ykpy13]
  4. ISCIII-FEDER funds from the REDinREN program
  5. Fibroteam from Comunidad de Madrid
  6. IRSIN-FRIAT
  7. FIS [12/00241]

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Long-term peritoneal dialysis causes morphologic and functional changes in the peritoneal membrane. Although mesothelial-mesenchymal transition of peritoneal mesothelial cells is a key process leading to peritoneal fibrosis, and bioincompatible peritoneal dialysis solutions (glucose, glucose degradation products, and advanced glycation end products or a combination) are responsible for altering mesothelial cell function and proliferation, mechanisms underlying these processes remain largely unclear. Peritoneal fibrosis has 2 cooperative parts, the fibrosis process itself and the inflammation. The link between these 2 processes is frequently bidirectional, with each one inducing the other. This review outlines our current understanding about the definition and pathophysiology of peritoneal fibrosis, recent studies on key fibrogenic molecular machinery in peritoneal fibrosis, such as the role of transforming growth factor-beta/Smads, transforming growth factor-beta beta/Smad independent pathways, and noncoding RNAs. The diagnosis of peritoneal fibrosis, including effluent biomarkers and the histopathology of a peritoneal biopsy, which is the gold standard for demonstrating peritoneal fibrosis, is introduced in detail. Several interventions for peritoneal fibrosis based on biomarkers, cytology, histology, functional studies, and antagonists are presented in this review. Recent experimental trials in animal models, including pharmacology and gene therapy, which could offer novel insights into the treatment of peritoneal fibrosis in the near future, are also discussed in depth.

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