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Mesenchymal Conversion of Mesothelial Cells Is a Key Event in the Pathophysiology of the Peritoneum during Peritoneal Dialysis

机译:间皮细胞间充质转化是腹膜透析过程中腹膜病理生理学中的关键事件

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Peritoneal dialysis (PD) is a therapeutic option for the treatment of end-stage renal disease and is based on the use of the peritoneum as a semipermeable membrane for the exchange of toxic solutes and water. Long-term exposure of the peritoneal membrane to hyperosmotic PD fluids causes inflammation, loss of the mesothelial cells monolayer, fibrosis, vasculopathy, and angiogenesis, which may lead to peritoneal functional decline. Peritonitis may further exacerbate the injury of the peritoneal membrane. In parallel with these peritoneal alterations, mesothelial cells undergo an epithelial to mesenchymal transition (EMT), which has been associated with peritoneal deterioration. Factors contributing to the bioincompatibility of classical PD fluids include the high content of glucose/glucose degradation products (GDPs) and their acidic pH. New generation low-GDPs-neutral pH fluids have improved biocompatibility resulting in better preservation of the peritoneum. However, standard glucose-based fluids are still needed, as biocompatible solutions are expensive for many potential users. An alternative approach to preserve the peritoneal membrane, complementary to the efforts to improve fluid biocompatibility, is the use of pharmacological agents protecting the mesothelium. This paper provides a comprehensive review of recent advances that point to the EMT of mesothelial cells as a potential therapeutic target to preserve membrane function.
机译:腹膜透析(PD)是治疗终末期肾脏疾病的一种治疗选择,它基于腹膜作为半透膜的使用,用于交换有毒溶质和水。腹膜长期暴露于高渗PD液体会引起炎症,间皮细胞单层丧失,纤维化,血管病变和血管生成,这可能导致腹膜功能下降。腹膜炎可能会进一步加重腹膜的损伤。与这些腹膜改变并行,间皮细胞经历上皮到间充质转变(EMT),这与腹膜恶化有关。导致经典PD流体生物不相容的因素包括高含量的葡萄糖/葡萄糖降解产物(GDPs)及其酸性pH。新一代的低GDP中性pH值液体具有改善的生物相容性,从而可以更好地保护腹膜。但是,仍需要标准的基于葡萄糖的液体,因为生物相容性解决方案对于许多潜在用户而言价格昂贵。与改善液体生物相容性的努力相辅相成的一种保护腹膜的替代方法是使用保护间皮的药物。本文提供了对最新进展的全面综述,这些进展指出间皮细胞的EMT作为保留膜功能的潜在治疗靶点。

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