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Differential expression of receptors for advanced glycation end-products in peritoneal mesothelial cells exposed to glucose degradation products

机译:暴露于葡萄糖降解产物的腹膜间皮细胞中晚期糖基化终产物受体的差异表达

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摘要

Autoclaving peritoneal dialysate fluid (PDF) degrades glucose into glucose degradation products (GDPs) that impair peritoneal mesothelial cell functions. While glycation processes leading to formation of advanced glycation end-products (AGE) were viewed commonly as being mediated by glucose present in the PDF, recent evidence indicates that certain GDPs are even more powerful inducers of AGE formation than glucose per se. In the present study, we examined the expression and modulation of AGE receptors on human peritoneal mesothelial cells (HPMC) cultured with GDPs, conventional PDF or PDF with low GDP content. HPMC cultured with GDPs differentially modulated AGE receptors (including RAGE, AGE–R1, AGE–R2 and AGE–R3) expression in a dose-dependent manner. At subtoxic concentrations, GDPs increased RAGE mRNA expression in HPMC. 2-furaldehyde (FurA), methylglyoxal (M-Glx) and 3,4-dideoxy-glucosone-3-Ene (3,4-DGE) increased the expression of AGE–R1 and RAGE, the receptors that are associated with toxic effects. These three GDPs up-regulated the AGE synthesis by cultured HPMC. In parallel, these GDPs also increased the expression of vascular endothelial growth factor (VEGF) in HPMC. PDF with lower GDP content exerted less cytotoxic effect than traditional heat-sterilized PDF. Both PDF preparations up-regulated the protein expression of RAGE and VEGF. However, the up-regulation of VEGF in HPMC following 24-h culture with conventional PDF was higher than values from HPMC cultured with PDF containing low GDP. We have demonstrated, for the first time, that in addition to RAGE, other AGE receptors including AGE–R1, AGE–R2 and AGE–R3 are expressed on HPMC. Different GDPs exert differential regulation on the expression of these receptors on HPMC. The interactions between GDPs and AGE receptors may bear biological relevance to the intraperitoneal homeostasis and membrane integrity.
机译:高压灭菌腹膜透析液(PDF)将葡萄糖降解为损害腹膜间皮细胞功能的葡萄糖降解产物(GDPs)。尽管通常认为导致形成高级糖基化终产物(AGE)的糖基化过程是由PDF中存在的葡萄糖介导的,但最近的证据表明,某些GDP比葡萄糖本身更能促进AGE形成。在本研究中,我们研究了在用GDP,常规PDF或低GDP含量的PDF培养的人腹膜间皮细胞(HPMC)上AGE受体的表达和调控。用GDP差异调节的AGE受体(包括RAGE,AGE-R1,AGE-R2和AGE-R3)表达的HPMC培养呈剂量依赖性。在亚毒性浓度下,GDP会增加HPMC中RAGE mRNA的表达。 2-呋喃醛(FurA),甲基乙二醛(M-Glx)和3,4-二脱氧葡萄糖苷-3-烯(3,4-DGE)增加了AGE-R1和RAGE的表达,RAGE和RAGE是与毒性作用相关的受体。这三个国内生产总值上调了培养的HPMC的AGE合成。同时,这些GDP也增加了HPMC中血管内皮生长因子(VEGF)的表达。 GDP含量较低的PDF与传统的热灭菌PDF相比,其细胞毒性作用较小。两种PDF制剂均上调RAGE和VEGF的蛋白表达。但是,使用常规PDF进行24小时培养后,HPMC中VEGF的上调高于使用GDP较低的PDF培养后的HPMC中的上调值。我们已经首次证明,除了RAGE,HPMC还表达了其他AGE受体,包括AGE-R1,AGE-R2和AGE-R3。不同的GDP对HPMC上这些受体的表达施加不同的调节。 GDP和AGE受体之间的相互作用可能与腹膜内稳态和膜完整性具有生物学相关性。

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