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支化多聚甘油的尺寸依赖性功效和生物相容性在腹膜透析中的应用。

The size-dependent efficacy and biocompatibility of hyperbranched polyglycerol in peritoneal dialysis.

机构信息

Department of Urologic Sciences, University of British Columbia, Vancouver, BC, Canada.

Division of Nephrology, Department of Medicine, University of British Columbia, Vancouver, BC, Canada.

出版信息

Biomaterials. 2014 Feb;35(5):1378-89. doi: 10.1016/j.biomaterials.2013.10.076. Epub 2013 Nov 15.

Abstract

Glucose is a common osmotic agent for peritoneal dialysis (PD), but has many adverse side effects for patients with end-stage renal disease. Recently, hyperbranched polyglycerol (HPG) has been tested as an alternative osmotic agent for PD. This study was designed to further examine the efficacy and biocompatibility of HPG over a range of different molecular weights. HPGs of varying molecular weights (0.5 kDa, 1 kDa, 3 kDa) were evaluated in a preclinical rodent model of PD. HPG PD solutions were standardized for osmolality and compared directly to conventional glucose-based Physioneal™ PD solution (PYS). The efficacy of HPG solutions was measured by their ultrafiltration (UF) capacity, solute removal, and free water transport; biocompatibility was determined in vivo by the histological analysis of the peritoneal membrane and the cell count of detached peritoneal mesothelial cells (PMCs) and neutrophils, and in vitro cytotoxicity to cultured human PMCs. All the different sized HPGs induced higher UF and sodium removal over a sustained period of time (up to 8 h) compared to PYS. Urea removal was significantly higher for 1-3 kDa than PYS, and was similar for 0.5 kDa. Our analyses indicated that the peritoneal membrane exhibited more tolerance to the HPG solutions compared to PYS, evidenced by less submesothelial injury and neutrophil infiltration in vivo, and less cell death in cultured human peritoneal mesothelial cells. Free water transport analysis of HPG indicated that these molecules function as colloids and induce osmosis mainly through capillary small pores. We attribute the differences in the biocompatibility and osmotic activity of different sized HPGs to the differences in the polymer bound water measured by differential scanning calorimetry. These preclinical data indicate that compared to PYS, low MW HPGs (0.5-3 kDa) produces superior fluid and waste removal with better biocompatibility profile, suggesting that they are promising osmotic agents for PD.

摘要

葡萄糖是腹膜透析(PD)常用的渗透剂,但对终末期肾病患者有许多不良反应。最近,超支化聚甘油(HPG)已被测试为 PD 的替代渗透剂。本研究旨在进一步研究不同分子量的 HPG 的疗效和生物相容性。在 PD 的临床前啮齿动物模型中评估了不同分子量(0.5 kDa、1 kDa、3 kDa)的 HPG。HPG PD 溶液的渗透压标准化,并与传统的基于葡萄糖的 Physioneal™ PD 溶液(PYS)直接比较。HPG 溶液的功效通过其超滤(UF)能力、溶质去除和游离水转运来衡量;生物相容性通过腹膜膜的组织学分析和分离的腹膜间皮细胞(PMCs)和中性粒细胞的细胞计数以及对培养的人 PMCs 的体外细胞毒性来确定。与 PYS 相比,所有不同大小的 HPG 在较长时间(长达 8 小时)内都能引起更高的 UF 和钠去除。1-3 kDa 的尿素去除率明显高于 PYS,而 0.5 kDa 的尿素去除率与 PYS 相似。我们的分析表明,与 PYS 相比,HPG 溶液对腹膜膜的耐受性更高,这表现在体内 Submesothelial 损伤和中性粒细胞浸润较少,以及培养的人腹膜间皮细胞中细胞死亡较少。HPG 的游离水转运分析表明,这些分子作为胶体起作用,主要通过毛细血管小孔诱导渗透。我们将不同大小的 HPG 的生物相容性和渗透活性的差异归因于差示扫描量热法测量的聚合物结合水的差异。这些临床前数据表明,与 PYS 相比,低 MW HPG(0.5-3 kDa)具有更好的生物相容性和更好的流体和废物去除效果,这表明它们是有前途的 PD 渗透剂。

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