Hyperosmolality-Mediated Peritoneal Microvascular Vasodilation Is Linked to Aquaporin Function
المؤلف | Zakaria, El Rasheid |
المؤلف | Al-Thani, Asma |
المؤلف | Fawzi, Ashraf |
المؤلف | Fituri, Omar |
تاريخ الإتاحة | 2016-01-12T12:00:11Z |
تاريخ النشر | 2014 |
اسم المنشور | Advances in Peritoneal Dialysis |
الاقتباس | Zakaria el R, Althani A, Fawzi AA, Fituri OM, Hyperosmolality-mediated peritoneal microvascular vasodilation is linked to aquaporin function. Advances in Peritoneal Dialysis, 2014, 30:63-74 |
الرقم المعياري الدولي للكتاب | 1197-8554 |
الملخص | Glucose-based peritoneal dialysis (PD) solutions dilate the parietal and visceral peritoneal microvasculature by endothelium-dependent mechanisms that primarily involve hyperosmolality. This PD-mediated dilation occurs by active intracellular glucose uptake and adenosine A1 receptor activation, and by hyperosmolality-stimulated glibenclamide-sensitive potassium channels. Both pathways invoke NO as a second messenger for vasodilation. We hypothesized that during crystalloid-induced osmosis, the osmotic water flux through the transendothelial water-exclusive aquaporin 1 (AQP1) channels is the primary mechanism whereby the endothelium is being stimulated to instigate hyperosmolality-driven vasodilation. Four microvascular levels (diameters in the range 6 – 100 μm) were visualized by intravital videomicroscopy of the terminal ileum in anesthetized rats. Microvascular diameters and flow were measured after topical exposure to a 5% hypertonic mannitol or 2.5% glucose-based PD solution, at baseline and after brief tissue pre-treatment (with 0.1% glutaraldehyde for 10 seconds) or after combined tissue pre-treatment and pharmacologic blockade of AQP1 with HgCl2 (100 μmol/L). Vascular endothelial integrity was verified by the response to acetylcholine (10–4 mol/L) and sodium nitroprusside (10–4 mol/L). The hyperosmolar solutions both caused rapid and sustained vasodilation at all microvascular levels, which was not altered by tissue pre-treatment. Inhibition of AQP1 completely abolished the mannitolinduced vasodilation and markedly attenuated the PD fluid–mediated vasodilation. Neither glutaraldehyde pre-treatment nor HgCl2 affected tissue integrity or endothelial cell function. We conclude that the peritoneal microvascular vasodilation caused by hyperosmolar PD fluid is instigated by the osmotic water flux through AQP1. Clinical PD solutions have components other than hyperosmolality that can induce endothelium-dependent peritoneal microvascular vasodilation independent of the AQP1-mediated osmosis. |
راعي المشروع | research grant NPRP 09-268-3-066, funded by the Qatar National Research Fund |
اللغة | en |
الناشر | Peritoneal dialysis publications Inc |
الموضوع | Hyperosmolality vascular reactivity adenosine receptors intestinal microcirculation vasodilation Peritoneal dialysis solution Glucose/pharmacokinetics Ileum/metabolism |
النوع | Article |
الصفحات | 63-74 |
رقم المجلد | 30 |
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