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腹膜透析:从实验室到临床,再从临床到实验室。

Peritoneal dialysis: from bench to bedside and bedside to bench.

作者信息

Perl Jeffrey, Bargman Joanne M

机构信息

Division of Nephrology, St. Michael's Hospital, University of Toronto, and The Keenan Research Centre in the Li Ka Shing Knowledge Institute, St. Michael's Hospital, Toronto, Ontario, Canada;

Division of Nephrology, Department of Medicine, University of Toronto, Toronto, Ontario, Canada; and.

出版信息

Am J Physiol Renal Physiol. 2016 Nov 1;311(5):F999-F1004. doi: 10.1152/ajprenal.00012.2016. Epub 2016 Mar 23.

DOI:10.1152/ajprenal.00012.2016
PMID:27009336
Abstract

For patients with end-stage kidney disease unable to receive a kidney transplant, replacement of kidney function with dialysis is necessary to extend life. Peritoneal dialysis (PD) and hemodialysis (HD) are the two major forms of dialysis therapy. HD involves the passage of blood via an extracorporeal circuit whereby removal of small solutes, toxins, and water is achieved across a synthetic, semipermeable dialysis membrane. In contrast, in PD, the dialysis membrane is the highly vascularized internal lining of the peritoneal cavity. Intraperitoneal installation of hypertonic high glucose PD solution creates a transmembrane osmotic and diffusive gradient that facilitates water removal [ultrafiltration (UF)], convection, and diffusion of uremic toxins. Insight into the physiology of solute and water transport across the peritoneal membrane has been enhanced by the proposal of the ''three-pore model'' of peritoneal membrane transport. Transport characteristics and UF capacity of the peritoneal membrane vary among individuals, and deleterious changes in the membrane may ensue over time. The degree to which these changes are a direct consequence of the type and composition of currently available PD solutions, recurrent infectious episodes, genetic differences among individuals, or a combination thereof is the subject of intense study. Adverse consequences resulting from the systemic and local metabolic effects of intraperitoneal glucose exposure, infection of the PD fluid, PD catheter dysfunction, and patient burnout from self-care often limit the long-term success of the therapy. Research aimed at addressing these challenges will examine the use of more biocompatible PD solutions and strategies aimed at attenuating progressive peritoneal membrane injury.

摘要

对于无法接受肾移植的终末期肾病患者,采用透析替代肾功能以延长生命是必要的。腹膜透析(PD)和血液透析(HD)是透析治疗的两种主要形式。血液透析是使血液通过体外循环,通过合成的半透性透析膜来清除小分子溶质、毒素和水分。相比之下,在腹膜透析中,透析膜是腹膜腔高度血管化的内衬。腹腔内注入高渗高糖腹膜透析液会产生跨膜渗透和扩散梯度,从而促进水分清除(超滤)、对流以及尿毒症毒素的扩散。腹膜转运的“三孔模型”的提出,加深了人们对溶质和水分跨腹膜转运生理机制的理解。腹膜的转运特性和超滤能力因人而异,随着时间推移,腹膜可能会发生有害变化。这些变化在多大程度上是目前可用腹膜透析液的类型和成分、反复感染发作、个体基因差异或它们共同作用的直接结果,是深入研究的课题。腹膜内葡萄糖暴露的全身和局部代谢影响、腹膜透析液感染、腹膜透析导管功能障碍以及自我护理导致的患者倦怠所产生的不良后果,常常限制了该治疗方法的长期成功。旨在应对这些挑战的研究将考察使用生物相容性更好的腹膜透析液以及旨在减轻腹膜渐进性损伤的策略。

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