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维持性血液透析和持续性非卧床腹膜透析中血钾异常的发病机制与治疗

Pathogenesis and treatment of dyskalemia in maintenance hemodialysis and CAPD.

作者信息

Kim Ho-Jung

机构信息

Department of Internal Medicine, College of Medicine, Hanyang University, Guri, Korea.

出版信息

Electrolyte Blood Press. 2006 Mar;4(1):47-52. doi: 10.5049/EBP.2006.4.1.47.

Abstract

In end-stage renal disease (ESRD) patients regardless of dialysis modes, i.e. maintenance hemodialysis (HD) and continuous ambulatory peritoneal dialysis (CAPD), potassium (K) homeostasis is regulated primarily via dialysis and extrarenal K regulation in the diverse daily K intake. However, K metabolism has been known to differ greatly between the two main methods of dialysis. Hyperkalemia is a common complication (10-24%) and the most common cause of the death (3-5%) among electrolyte disorders in patients on maintenance HD. On the contrary, hypokalemia (10-36%) is responsible for a rather common complication and independent prognostic factor on CAPD. Although excessive K intake or inadequate dialysis on maintenance HD and poor nutritional K intake on CAPD are accused without doubts upto 50% of ESRD patients as a primary cause of the K-imbalance, i.e. hyperkalemia on HD and hypokalemia on CAPD, other contributory factors including certain medications and unknown causes remain still to be resolved. Accordingly, the effects of medications as another source of K-imbalance on HD with RAS blockades and beta blockers as well as those of conventional and glucose-free dialysates (Icodextrin) for internal K-redistribution on CAPD were evaluated with reviewing the literatures and our data. Furthermore, new developments in the clinical managements of hyperkalemia on HD following the exclusion of pseudohyperkalemia before the initiation of dialysis were suggested, especially, by the comparison of the effects between mono- and dual-therapy with medications for transcellular K shifting in the emergent situation. Also, the intraperitoneal K administration via conventional glucose-containing (2.5%) and glucose-free dialysates (Icodextrin) as a specific route of K-supplementation for hypokalemia on CAPD was examined for its efficiency and the degree of intracellular K shift between these two different types of dialysates.

摘要

在终末期肾病(ESRD)患者中,无论采用何种透析方式,即维持性血液透析(HD)和持续性非卧床腹膜透析(CAPD),在每日不同的钾摄入量情况下,钾(K)稳态主要通过透析和肾外钾调节来维持。然而,已知两种主要透析方法之间的钾代谢差异很大。高钾血症是维持性HD患者电解质紊乱中常见的并发症(10 - 24%),也是最常见的死亡原因(3 - 5%)。相反,低钾血症(10 - 36%)是CAPD中较为常见的并发症和独立的预后因素。尽管毫无疑问,高达50%的ESRD患者中,维持性HD时钾摄入过多或透析不足以及CAPD时营养性钾摄入不足被认为是钾失衡的主要原因,即HD时的高钾血症和CAPD时的低钾血症,但包括某些药物和不明原因在内的其他促成因素仍有待解决。因此,通过回顾文献和我们的数据,评估了作为钾失衡另一个来源的药物对HD联合使用肾素 - 血管紧张素系统(RAS)阻滞剂和β受体阻滞剂的影响,以及传统和无糖透析液(艾考糊精)对CAPD时体内钾再分布的影响。此外,特别是通过比较紧急情况下用于细胞内钾转移的药物单药治疗和联合治疗的效果,提出了在透析开始前排除假性高钾血症后HD时高钾血症临床管理的新进展。同时,还研究了通过传统含葡萄糖(2.5%)和无糖透析液(艾考糊精)进行腹膜内钾给药作为CAPD时低钾血症的一种特定补钾途径的效率,以及这两种不同类型透析液之间细胞内钾转移的程度。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/599c/3894544/19113457d1e8/ebp-4-47-g001.jpg

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